Outsmart Your Cancer
Outsmart Your Cancer
Outsmart Your Cancer
your cancer
sicoxo ioiriox
Tax\a Hairii Piiici, x.a., xicc
ruoucuroixs iuniisuixc
Stateline, Nevada 2009
Outsmart
your cancer
Alternative Non-Toxic Treatments That Work
Copyright 2009 Tanya Harter Pierce.
Printed and bound in the United States of America.
All rights reserved. No part of this book may be reproduced or transmitted in any
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ing, or by an information storage and retrieval systemexcept by a reviewer who
may quote brief passages in a review to be printed in a magazine, newspaper, or
on the Webwithout permission in writing from the publisher. For informa tion,
please contact Toughtworks Publishing, P.O. Box 4949, Stateline, NV 89449;
(888) 679-2669.
Although the author and publisher have made every eort to ensure the accuracy
and completeness of information contained in this book, we assume no responsi-
bility for errors, inaccuracies, omissions, or any inconsistency herein. Any slights
of people, places, or organizations are uninten tional.
First Edition: September 2004 (448 pp.)
Second Edition: August 2009 (528 pp. plus Audio CD)
Typesetting by www.FionaRaven.com
ISBN-I3: 978-0-9728867-8-9
ISBN 0-9728867-8-8
LCCN 2003I04206
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Disclaimer
Tanya Harter Pierce is not a physician and none of the information in
this book should be construed as medical advice. Te author is merely
presenting her ndings, as would an investigative journalist. Tus, the
material in this book should be used for educational and informational
purposes only. Each person must make his or her own decisions about treat-
ment. Prior to making those decisions, anyone who has cancer or suspects
he or she may have cancer, should consult with a qualied physician.
A conscientious eort has been made to only present information that
is accurate and truthful in this book. However, the author cannot be
held responsible for inaccuracies that may be found in her source mate-
rial. She is also not responsible for any changes in ingredients or reduc-
tion in quality of any of the products mentioned in this book, should
that occur. Moreover, this is not a comprehensive survey of all non-toxic
cancer treatments available.
Note: Te alternative non-toxic approaches presented in this book are
not approved by the FDA as treatments for cancer.
vii
Acknowledgments
My most abundant and never-ending gratitude goes to my husband,
David Pierce. Without his total support and belief in me, I would not
have been able to write this book. He not only supported me in a myriad
of ways, but also gave me excellent editorial input on every chapter. Next,
I send my love to Yahtzee, my devoted dog who gave me joyful compan-
ionship through all aspects of this work until she passed just before the
2nd Edition went to print. Her sweetness and special personality kept
me going and grounded me in the important things of life.
I also want to thank my brother, Craig, who introduced me to some
important sources of alternative cancer treatment information, and to
express warm gratitude to my sisters, Margo and Kathy, and my mother,
Bonnie, for their enthusiasm and encouragement about my project. And
I sincerely thank the many medical professionals and other experts who
graciously reviewed or provided important input to specic sections of
this book.
Finally, I deeply appreciate and applaud the eorts of all the pioneering
physicians, scientists, medical researchers and authors who went before me
and wrote books, articles, and Internet postings to share their knowledge
of alternative cancer therapies. To all of them I say, Your commitment
and courage will never be forgotten!
ix
Table of Contents
Acknowledgments, vii
Introduction, xi
Section One: Understanding Cancer, 1
1 Te Cancer Reality Today, 3
2 Why So Much Cancer and What Causes It? 17
Section Two: Alternative Non-Toxic Treatments, 41
3 Te Hoxsey Terapy, 43
4 Essiac Tea, 55
5 Te Gerson Terapy, 63
6 Laetrile, 71
7 Dr. Kelleys Enzyme Terapy, 85
8 Burzynskis Antineoplastons, 101
9 Protocel
for best
results. On top of all of that, a new audio CD has been inserted into
the back of the book that contains helpful information about alternative
versus conventional methods and presents testimonials from people who
courageously used non-toxic approaches to cure their own cancer. I hope
readers will be inspired listening to these testimonials. Tere is nothing
so convincing as hearing these types of stories from everyday people in
their own words!
Tough I cannot counsel you on the decision you should make for your
own particular medical situation, my hope is that this book will save you
valuable time in your own search for answers. And if you have been told
that conventional medicine cannot oer you a long-term cure, then this
book may provide you with much-needed hope.
I sincerely wish you the very best on your path to recovery!
Tanya Harter Pierce, M.A., MFCC
. . . Tat Wisdom may nish what Knowledge did start . . .
Astarius
From the invocation Let Tere Be on the CD Spirit Rap
2000 by Astarius Reiki-Om, www.astarius.com
Section One
Understanding Cancer
3
I
Te Cancer Reality Today
I
f you are facing a cancer diagnosis, the rst thing you should know is
that there is hope in the world of alternative, non-toxic treatments. And
I am referring to very real hopenot the false hope that is so often
oered in the guise of chemotherapy and radiation. Tens of thousands of
people have declined conventional medicine, either as soon as they were
diagnosed or after conventional methods failed, and used alternative
methods instead to overcome their cancer. Tese people have then gone
on to live normal, healthy lives!
Te second thing you should know is that you are far from alone. Right
now, one in every two to three Americans will develop life-threatening
cancer at some point in their lives. Tis estimate comes primarily from
the ocial American Cancer Society gures of I996, which predicted
that 40 percent of all Americans will develop life-threatening cancer.
Tis statistical estimate has been conrmed by other researchers as well,
many of whom believe the 40 percent gure to be conservative. Overall,
cancer rates have been rising at an alarming rate for the past I00 years.
In recent years, the rate of lung cancer incidence has been going down
due to fewer people smoking, but the rates of virtually all other types of
cancer are still increasing.
Whenever a person nds themselves facing a cancer diagnosis, time
is of the essence. Tere are urgent decisions to make, and you need treat-
ment information fast. You may have various doctors, relatives, or friends
4 oursxair \oui caxcii
pushing you to quickly get your surgery, chemotherapy, and/or radiation.
Tey may even say things like, If you dont do this now, you will die! If
this is happening to you, try to remember that these people are pushing
you because they care about you and are, themselves, scared. And they
are right when they say that you need to take action very soon.
But you deserve to know that everyone in America is strongly inu-
encedeven brought up all their livesto think that conventional
treatments are the only answers to cancer. Surgery, chemotherapy, and
radiation are commonly called Te Big Tree of mainstream cancer
treatment, and most doctors think these are the only answers.
Unfortunately, there are serious problems with these conventional
treatment approaches. Of the three, surgery is denitely the most eec-
tive. Surgery can sometimes bring about long-term recovery when cancer
is caught early and is in an area where the entire cancerous area can be
cut out. Tis is particularly true for early cancers where an entire organ
or body part can be removed, such as a kidney, thyroid gland, testicle, or
uterus. But for the majority of cases, the cancer has already metastasized
(spread to other areas of the body) by the time a person is diagnosed. And,
for those cases, surgery cannot get all of the cancer cells. Many researchers
believe that surgery can even promote metastasis in some cases.
Chemotherapy and radiation have even worse long-term recovery
rates than surgery. Tis is largely because they resort to toxic methods of
bludgeoning a persons cancer to death. Tese toxic treatments harm
healthy parts of a persons body along with the cancer, thereby making
long-term recovery dicult.
Te good news is that, even if you have been diagnosed with cancer
that has already metastasized, there are alternative options to conven-
tional treatments. And they often have better track records, in general,
than what mainstream medicine is oering. I know many people who
were told by their doctor that their late-stage or metastasized cancer was
incurable, only to completely recover later by using a non-toxic, alterna-
tive approach! In fact, you may nd after reading this book that your
biggest diculty is not in nding a good alternative treatment approach
to cancer, but in deciding which one to use because there are so many
to choose from.
Tere are very important reasons why alternative treatments for can-
cer often have better track records than conventional ones. Most impor-
tantly, alternative, non-toxic approaches work in ways that do not harm
normal, healthy cells of the body. Tey do this by focusing on those
5 The Cancer Reality Today
aspects of cancer cells that are signicantly dierent from healthy cells.
Tese approaches treat cancer as a whole-body disease and work with a
persons immune system to attack the cancer cells everywhere, even the
free-oating individual cells. Tis is dierent from mainstream practices,
which focus primarily on just treating tumors (which may represent most
of the cancer cells in a persons body, but not all), and use toxic treatments
that can seriously damage the bodys immune system and vital organs.
In other words, conventional medicine tries to bludgeon your cancer
to death with toxic treatments that can be extremely harmful to your
body, while alternative methods use non-toxic approaches to Outsmart
Your Cancer !
Benets of Non-Toxic Approaches
Te most obvious benet of using a non-toxic approach to cancer is
that, by doing so, a person does not damage healthy parts of his or her
body while trying to recover from their illness. Chemotherapy and radia-
tion can damage virtually any cells they come in contact with and may
have extremely serious long-term side eects such as liver, kidney, nerve,
and heart damage. Tese side eects can often be life-threatening in and
of themselves. Other side eects, such as chronic weakness, may result
from damaged adrenals and/or thyroid glands, and this can reduce a
persons quality of life.
Besides general bodily damage that can be caused, many cancer patients
are not even told by their doctors that some common conventional treat-
ments for cancer are themselves carcinogenic. Te fact is that some chemo-
therapy agents are known carcinogens, and the chemotherapy treatment
given to many patients to put their cancer into remission may directly
cause a secondary cancer to develop in that person a few years later. Radia-
tion can also cause cancer, which has been well-known since radiation
techniques were rst developed. Tough surgery is not considered carci-
nogenic, it may cause the spread of cancer to other parts of the body.
Moreover, at some point, the use of a toxic treatment for cancer may
enable the cancer to spread even faster in a persons body. Tis is because
that persons immune system and other natural defense mechanisms
have been so weakened by the treatment itself, the body can no longer
ght o the cancer. So it only makes sense that using a toxic treatment
for cancer can work against long-term recovery by giving the body more
damage to recover from.
6 oursxair \oui caxcii
But there is another benet of non-toxic approaches that is critical to
long-term recovery from cancer, yet is little understood. Tis is the benet
that comes from continual use of a treatment. Te importance of this par-
ticular benet cannot be overstated. Conventional toxic approaches, such
as chemotherapy and radiation, do not allow for continual use because
they are so toxic, continual use would kill the patient before the cancer
could! For this reason, toxic treatments are always administered with
doses spaced out. Tis necessity to space out the administration of a toxic
treatment is not optimally eective since one of cancers best abilities is
to grow new cells fast. Tus, in-between toxic treatment administrations,
while the patients body is recovering from the treatment, the cancer cells
are recovering too. And those cancer cells that grow back the fastest are
those cells that have some amount of resistance to the treatment. In
other words, the treatment itself selects for the proliferation of resistant
cancer cells in a persons body. Tis type of resistance has become more
and more evident with the use of antibiotics causing antibiotic-resistant
bacteria. In the case of chemotherapy use, this type of dynamic may result
in what are called multi-drug-resistant cancer cells, or MDR cells.
With non-toxic treatments, however, these vicious dynamics are avoided.
Non-toxic approaches do not harm the body and therefore allow for con-
tinual use. When a cancer treatment is non-toxic and can be administered
continually every day, resistant cells are not promoted. In fact, a non-toxic
approach can be done every single day for months or years. Tis allows
the treatment approach to work in the body 24/7 and never gives the
cancer cells a chance to grow back in ever more virulent forms.
Also, non-toxic approaches can often be continued for years after one
has achieved remission, if a person chooses to. Tis gives people a way to
help ensure that their cancer does not come back!
Te Bigger Picture
To sum up the bigger picture of conventional versus alternative can-
cer treatments today, I have come up with what I call the three basic
truths. Tey are:
I. Conventional treatments have failed
2. Successful alternative treatments abound
3. Te disbelief factor is alive and well
7 The Cancer Reality Today
First Basic TruthConventional Treatments Have Failed
It is commonly accepted by many reputable cancer researchers that the
conventional war on cancer has failed. In fact, it has failed so miserably
that the conventional cancer industry has had to resort to fudging their
cure-rate statistics so the public will continue to think they are doing a
good job! (By cancer industry, I mean the part of organized medicine
devoted to cancer research, treatment, and education, which is led pri-
marily by the National Cancer Institute [NCI], the American Cancer
Society [ACS], the Food and Drug Administration [FDA], the American
Medical Association [AMA], a few large centers throughout the country
such as Memorial Sloan-Kettering Cancer Center in New York, and vari-
ous pharmaceutical companies that produce cancer drugs.)
Once we clear away the fudged statistics and get down to the true
reality, however, we nd that current conventional medical treatments
for cancer can only bring about real cures (long-term survival) for a very
small percentage of cancer patients. People with primary cancer (cancer
that has not yet metastasized) have the best chance of survival with con-
ventional treatments, where they may have about a I0 to I5 percent chance
of long-term recovery if the cancer is caught early and is in an area of the
body that allows for total surgical removal. But most cancer patients are
not lucky enough to be diagnosed with primary cancer. In the United
States, between two-thirds and three-fourths of all cancer patients have
cancer that had already metastasized by the time they were rst diagnosed.
And when it comes to conventional medical treatments for metastasized
cancer, many researchers agree that the long-term survival rate for these
patients is less than I percent. (In some cases, it is as low as one-tenth of
a percent.) When it comes to the long-term eectiveness of chemotherapy
in general, some highly respected cancer researchers believe it is eective
in only 2 to 3 percent of all cancers.
You might say, Wait a minute; I heard that 40 to 50 percent of all
cancer cases today are being cured by mainstream medicine. I also heard
that most cancers, when caught early enough, are curable. Well, I believe
that you heard that because these are the typical types of gures the cancer
industry likes to advertise. But the truth is that when you hear a statistic
like 40 to 50 percent cure rate or most cancers are curable if caught
early, you are being presented statistics that have been incredibly fudged
and manipulated. I learned about the ocial fudging tactics from a variety
of sources, but primarily from the in-depth work done by two prominent
cancer researchers: Ralph W. Moss, Ph.D., and Lorraine Day, M.D.
8 oursxair \oui caxcii
Ralph Moss is a highly renowned cancer researcher who has written
numerous books including Te Cancer Industry, Questioning Chemotherapy,
and Cancer Terapy: Te Independent Consumers Guide to Non-Toxic
Treatment and Prevention. Moss began his cancer research when he was
hired as a science writer at New Yorks Memorial Sloan-Kettering Cancer
Center in I974. Tere, he was able to observe the workings of the can-
cer industry from the inside. But according to Moss, his employment at
Memorial Sloan-Kettering ended when he would not go along with the
advertising of misleading information to the public. Over the years since
then, he has diligently researched the real truth for the public, which he
has carefully quoted and documented in his books. In an ever-growing
circle of people researching the truth about cancer treatments, Ralph
Moss is considered to be a leading authority.
Dr. Lorraine Day is an orthopedic trauma surgeon who rose to the
position of chief of orthopedic surgery at San Francisco General Hospital.
In I992, Dr. Days life changed dramatically when she was diagnosed with
breast cancer that had already metastasized. Tough she was pressured
by specialists to undergo a mastectomy followed by chemotherapy and
radiation, she chose not to receive those treatments because she knew so
much about the severe damage to her body they could cause. Instead, she
immediately started looking into other ways to treat herself, and eventu-
ally was able to completely heal and overcome her advanced cancer by
drastically changing her diet and through other natural steps.
Dr. Day details her amazing story and reveals the results of her own in-
depth research into cancer treatments in her numerous videos which can
all be purchased from her website (www.DrDay.com). One of Dr. Days
videos reveals the stark truth about conventional cancer treatments and
their side eects and real cure rates. It is called Cancer Doesnt Scare Me
Anymore, and I highly recommend it. (See ordering instructions at the
end of this chapter.)
Taken primarily from research done by both Dr. Moss and Dr. Day,
the six big ways ocial cancer cure rates and statistics have been fudged
are the following:
I. By the way cure is dened. Te current cancer authorities, such as
the ACS, NCI, and FDA, have all chosen to dene cure as alive ve
years after diagnosis. Tis ocial denition does not mean cancer
free, nor does it mean healed of your disease, which is what most
people think the word cure means.
9 The Cancer Reality Today
To give you a better idea of what I am talking about, we can look
at the true story of one female cancer patient. In this womans battle
against breast cancer, she did all the conventional approachessur-
gery, radiation, and chemotherapy. Unfortunately, the woman did not
survive. She died, full of cancer, ve years and two weeks after her
diagnosis. To add insult to injury, her husband found out later that
his beloved wife was listed as a cure on the ocial ledgers, because
she had died two weeks after the ve-year mark. Tus, because of the
American Cancer Societys denition of cure, many patients who
live ve years after their cancer diagnoses are listed as curedeven
though they still show evidence of having cancer, or even though they die
from their cancer. Tus, the denition of cure is the rst big fallacy
of ocial cancer cure-rate statistics, and may be the biggest ocial
fudging tactic used.
2. By simply not including certain groups of people, or certain types of
cancer. Tis is one of the hardest fudging tactics to believe. It means
that, at times, the ocial cancer authorities have been able to make
their statistics look better than they really are by simply not includ-
ing certain groups of people in their statistics who tend to show lower
recovery rates than other groups. Tese groups might be less likely to
recover for socio-economic or other reasons.
I was shocked when I discovered this could include all non-white
Americans. According to Ralph Moss, two prominent medical research-
ers who published their ndings in the New England Journal of Medicine
stated that the NCI generally reports whites-only gures. Nonwhites
. . . are kept in a separate category, untallied with the main group.
Moss states that NCIs solution is to list them in separate (but equal)
charts, and then to present the white charts as the norm. Moreover,
the NCI has also been known to greatly improve its advertised can-
cer cure rates by simply omitting all lung cancer patients from their
statistics! (It seems that the NCI sees lung cancer as dierent from
other cancers because of its connection to cigarette smoking.) Yet,
according to the American Cancer Society, lung cancer is the lead-
ing cause of cancer death for both men and women. Tus, in some
statistics, the National Cancer Institute simply does not include the
type of cancer that causes more deaths than any other type. Both of
the above tactics of omission can only be called biased selection, and
yet these statistics are presented as representative of all patients and
all life-threatening cancers.
10 oursxair \oui caxcii
3. By including types of cancer that are not life-threatening. Te can-
cer authorities were able to improve their publicized cure rates even
more when they took this brilliant step years ago. Tis tactic involves
including cancers in their statistics that are easily treatable and not
life-threatening, such as simple skin cancers. According to Dr. Douglas
Brodie, Five-year survivals of non-melanoma skin cancers, localized
cancers of the cervix, and some other non-spreading (metastasizing)
cancers detected early in specic sites, have been curable (that is, ame-
nable to ve-year absences of symptoms) since the days of Ptolemy.
As will be covered in Chapter I9, ductal carcinoma in situ (DCIS)
is now included in breast cancer statistics. DCIS is really more of a
pre-cancerous state that many experts believe should not even be clas-
sied as cancer, and is 99 percent curable. Yet, DCIS now comprises
about 30 percent of all breast cancer diagnoses in the United States
and is included in the cure-rate statistics for life-threatening breast
cancer as well. Tus, easily treatable skin cancers and DCIS are types
of non-life-threatening cancers that are included in statistics used to
imply what a patients chances of recovering from life-threatening can-
cers are. Tis tactic is like adding the risk of being killed by a bicycle
or someone on a skateboard when compiling the statistical likelihood
of being killed in a car crash!
4. By allowing earlier detection to imply longer survival. Tis tactic is
subtle but important. Over the decades, one of the aspects of cancer
medicine that has improved because of improved technology is that
of earlier detection. Advances in technology have allowed doctors and
researchers to detect cancer on average about six months earlier than
they used to be able to detect it. With the denition of cure being
alive ve years after diagnosis, earlier detection has, by itself, added
many new patients to the conventional cure list.
What is not accurate, however, is to claim that these improved
statistics reect improved life expectancy because of better treatment
methods. In other words, because tumors are getting diagnosed at
earlier stages than before, and because of the way cure is ocially
dened as a time deadline following diagnosis, long-term survival rates
may look better now than they did years ago. But the reality is that no
improvement in long-term survival has occurred at all.
5. By deleting patients from studies who die too soon. Tis is a par-
ticularly treacherous way the cancer industry manipulates statistics.
11 The Cancer Reality Today
What this means is that it has become an acceptable practice in ocial
cancer studies with human patients to simply drop a patient from the
records if he or she dies from cancer before the treatment protocol is
considered to have been completed. According to Dr. Lorraine Day, this
means that if a cancer patient dies on day 89 of a prescribed 90-day
course of chemotherapy, he or she would just disappear from the list of
treated patients and would not be listed as a failure. Yet, if a patient
in the control group (those not getting the specied treatment) dies
at any time, that patient is listed in the study as a death from cancer.
Tis is a double standard that shows an institutional lack of integrity
and is denitely not consistent with true scientic method.
6. By using an adjustment called relative survival rate. Tis was a vari-
ant on the ve-year survival statistic that the ocial cancer industry
created and adopted in the I980s to help them claim that the war on
cancer was being won. According to Ralph Moss, Relative survival
rates take into account the expected mortality gures. Put simply,
this means that if a person hadnt died of cancer he might have been
run over by a truck, and that must be factored into the equation.
Tese adjusted rates are used in a very misleading way because they
are presented to the public as representative of mainstream medicines
ability to help a cancer patient recover from their life-threatening cancer.
But, in truth, the relative survival rate adjustment is just one more way
that cancer cure-rate statistics are manipulated to make conventional
treatments look better than they really are.
Te above six major fudging tactics are the real back story behind the
ocial cancer cure-rate claims currently being advertised to the public.
It is only by using these types of extreme statistical manipulations and a
totally misleading denition of cure that the cancer industry can make
bogus statements like 40 to 50 percent of all cancers are curable. It takes
very little research to see that these statistics are not real, and that con-
ventional medicine has failed in the arena of cancer treatment.
Because these tactics are now institutionally ingrained in mainstream
cancer treatment and research, the conventional data available start out
distorted from the get-go. Terefore, the real data needed to gure out
the true conventional cure-rate statistics for cancer just arent available.
However, we dont need those data to know that we are in the midst of a
very serious problem. All we need to know is that in just one year (I996),
12 oursxair \oui caxcii
more people in the United States died of cancer than the number of U.S.
soldiers who died in all of World War II, the Korean War, and the entire
Vietnam War combined! Tis is quite a sobering thought. Another is
that Americans are dying of cancer at a rate approximately equivalent to
ten September II' terrorist attacks every month!
So, in the bigger picture, the rst basic truth is conventional cancer
treatments have failed.
Second Basic TruthSuccessful Alternative Treatments
Abound
How many times have we heard television commercials that imply
the pharmaceutical companies are working very hard to nd a cure for
cancer? Yet, you will discover in the following pages that many success-
ful treatments for cancer have already been developed. Tey just dont
get publicity since they are labeled alternative. To put it briey, the
cancer treatments that have been relegated to the alternative world have
generally involved natural forms of treatment that could not be patented
or otherwise controlled by the big multi-billion-dollar cancer industry.
Tis huge industry is run by powerful pharmaceutical companies and
even bigger corporate cartels. Its prots are threatened by any natural or
individually owned treatment that cant be patented or controlled by big
business for prot.
Te truth is that there have been many highly successful cancer treat-
ments developed over the past century that should have been incorporated
into mainstream medicine. Most of them were developed and pioneered
by highly respectable physicians or scientistsnot quacks or con artists.
Te best of the alternative, non-toxic treatments for cancer have had bla-
tantly higher success rates than conventional treatments, and these success
rates reect real cures, not phony redened cures! But these successful
cancer treatments have been suppressed to one degree or another, and
many misconceptions about alternative cancer treatments have ourished
as a result.
One misconception is that, in order for treatments to be suppressed,
there must be some kind of centrally located, conspiracy going on with
little evil men in dark clothes wringing their hands and tittering hee-hee
while eagerly anticipating peoples deaths. Tis is not at all how it works.
Te suppression has been carried out in many dierent ways by many
dierent organizations and is simply the result of business economics and
13 The Cancer Reality Today
common unethical tactics that tend to occur when large money interests
are involved in any eld.
Surgery, chemotherapy, and radiation involve billions of dollars of
prot for the industries that supply them. Moreover, the current system
for new drug development and approval by the FDA is set up such that
the cost of developing and bringing a new cancer drug to market is close
to a billion dollars. (Common costs are 700 to 800 million dollars in
the United States.) Without a patent, this type of cost investment is not
economically feasible for a pharmaceutical company. Tis means that,
since any treatment made up of natural ingredients is not patentable, a
natural form of treating cancer will never be pursued by a drug company.
Unfortunately for the public, the most successful treatments for cancer
either involve natural substances or are privately owned and patented by
creative individuals who were willing to think out of the box to develop
something totally new. What they have to oer is always going to be an
economic threat to the multi-billion-dollar cancer establishment.
Tus, to say that there is a conspiracy to suppress alternative cancer
treatments is like referring to industries that pollute the environment as
joining in a conspiracy to sacrice the well-being of our natural ecology.
Tat would be ludicrous and would show a total lack of understanding
that the way big businesses get where they are is by being prot-motivated.
When it comes to the environment, it is true that some of the tactics used
by industries to circumvent environmental protection laws or public safety
may seem conspiratorial, especially if they involve falsifying paperwork,
paying o Congress, or illegally dumping waste under the cover of dark-
ness. But that does not mean there is a broad conspiracy by big business
to pollute the environment. In the same way, there is no broad conspiracy
by big business to suppress alternative cancer treatments. In both cases,
big businesses are just doing what they do bestprotecting their prots.
Another misconception about alternative treatments for cancer in
general is that they simply involve going to the nearest health food store
and buying everyday types of supplements. If you nd it hard to believe
that doing this would be a successful way to overcome such a powerful
health challenge as cancer, your instincts are right. Tis is rarely how it
is done. Most of the successful alternative approaches involve much more
powerful treatments than that, and often revolve around very innovative
methods that require the help of an experienced alternative practitioner
or a knowledgeable support group to be done properly.
Tere is actually an amazing human story going on in the world of
14 oursxair \oui caxcii
alternative cancer treatment these days. With conventional medicine fail-
ing most cancer patients, more and more people are turning to alternative
medicine every year to save themselves. And large numbers of them are
winning! Tey are beating their cancer even though conventional medi-
cal experts are claiming that what they are doing cannot be done. Tey
are beating their cancer even though the big insurance companies are not
recognizing or paying for the treatments they are using. Tey are beating
their cancer because they are outsmarting their cancer with alternative,
non-toxic treatments that work. Tus, the second basic truth of the cancer
reality today is that successful alternative treatments abound.
Tird Basic TruthTe Disbelief Factor Is Alive and Well
Another widely held misconception about alternative cancer approaches
is that, if they really worked better than the current conventional approaches,
doctors and clinics everywhere would be using them. Tis misconception
is at the heart of what I call the disbelief factor. Te disbelief factor is
a dynamic that occurs in peoples minds when they say, If there really
are natural, non-toxic treatments for cancer that can bring about real,
long-term cures, even in cases of late-stage metastasized cancers, then
why arent all doctors using these treatments?
Finding it hard to understand why all doctors are not using the most
eective and least toxic treatments for cancer is not the problem. Te
real problem arises when a person nds this so hard to believe that he
or she simply cant accept the possibility that there could be alternative
approaches out there that really work. And when they are told there are,
they often dont listen at all because it is just too preposterous to believe.
Tis is the disbelief factor at work.
For those people with cancer who let the disbelief factor win, it is
a tragic situation. Teir disbelief keeps them from doing any further
research on their own. Tey trust their doctors, not knowing that their
doctors have only been taught the mainstream treatments and usually
know nothing of the alternative ones. What these people dont realize
is that most doctors are just people who also have a hard time believing
in alternative treatments, and who ask, If these treatments really work,
why wasnt I taught them in medical school?
And patients usually do not realize that, even if their doctor did think
an alternative treatment for cancer would help them, in most U.S. states
that doctor is not legally allowed to prescribe or even recommend anything
15 The Cancer Reality Today
other than the big three of surgery, chemotherapy, and radiation. Tat
is why cancer patients who are doing alternative treatments will so often
hear from their conventional doctor monitoring them, Just keep doing
whatever it is you are doing! Tese oncologists often dont even want to
know what the patient is doing that is working because they know they
cant prescribe it anyway. Unfortunately, the legal straightjacket that
conventional oncologists are in only contributes to the prevalence of the
disbelief factor. Te fact that the disbelief factor is alive and well is the
third basic truth of the cancer reality today.
As you can see, the bigger picture of cancer treatment in modern
countries such as the United States puts cancer patients at a disadvantage.
Te almost total separation between conventional and alternative thera-
pies requires patients to do their own homework if they are to make a
fully informed decision about their treatment. Te good news, however,
is that there are excellent alternative approaches available. But before we
delve into those approaches, there are two basic questions to answer rst:
Why so much cancer? and What causes it?
Resources:
Book
Ralph W. Moss, Ph.D. Te Cancer Industry. New York: Equinox Press,
1999.
Video
Lorraine Day, M.D. Cancer Doesnt Scare Me Anymore. To order, call (800)
574-2437, or visit Dr. Days website: www.drday.com.
17
2
Why So Much Cancer
and What Causes It?
M
ore and more people who have never smoked, who do not drink
heavily, and who have exercised and been health conscious all their
lives are being diagnosed with cancer. And they are wondering how this
could have happened to them. It is common for a persons rst question
after diagnosis to be, Why me? When they nd out that they are far
from alone, then the questions become, Why so much cancer? and
What causes it?
It seems that if we listen to doctors, pharmaceutical companies, or
advertisements on television about cancer clinics and treatments, we come
away with the idea that cancer is some sort of mysterious aiction that
no one completely understands. Other than knowing that too much sun
exposure can cause skin cancer, smoking too much can cause lung cancer,
and drinking too much can cause liver or kidney cancer, we somehow
get the idea that, for just about any other case, the medical profession
is stumped as to what causes cancer. What the public does not know,
however, is that it is only the conventional medical world that is stumped.
Researchers and practitioners who have been relegated to the alternative
no mans land have been putting important pieces of the cancer puzzle
together for decades and have already proven a number of key causes.
Understanding these causes is important for the cancer patient because it
18 oursxair \oui caxcii
moves cancer out of the realm of something I cant ght into the realm
of something I have control over.
Is Cancer Genetically Caused?
What about cancer being genetically caused? We hear so much about
modern cancer research focusing on genes and how certain people are
predisposed to cancer because of their family history. In fact, looking
at cancer as a genetically inherited disease has become so common that
some women who have never been diagnosed with cancer are actually
considering having both of their breasts surgically removed because they
have a family history of breast cancer. Tis incredibly extreme preventive
measure exhibits a powerful belief that cancer is genetic!
Although it is certainly possible that a predisposition to a few can-
cers may be genetically inherited, I will go out on a limb here and say
that most cancers are not a result of genetic inheritance. In her video,
Cancer Doesnt Scare Me Anymore (mentioned in Chapter I), Dr. Lor-
raine Day presents two compelling reasons why we must assume that
most cancers are not genetically inherited. Her rst reason is based on
the incredible rate at which cancer incidence has risen over the past
century. As an example, she refers to how the incidence of breast cancer
has risen dramatically since the early I900s. Yet, those were the days
of our grandmothers. Since the women of today are so closely linked
genetically with their grandmothers, if breast cancer were a genetically
inherited disease, then the grandmothers would have about the same
basic rate of incidence as their granddaughters. But the grandmothers of
todays women had a much lower incidence of breast cancer than todays
women. As recently as the I960s, about I in every 20 American women
developed breast cancer. Now, just 45 years later, about I in every 8
American women are developing breast cancer. If breast cancer were a
genetically inherited disease, there would be no way of explaining this
dramatic increase in incidence over just 45 years, between one genera-
tion of mothers to their daughters.
Tere are many other examples of dramatic rises in cancer rates as well.
For instance, Dr. Sto and Dr. Clouatre wrote in their book, Te Prostate
Miracle, that between I985 and I996, prostate cancer diagnoses in this
country rose from about 85,000 cases per year to over 3I7,000 cases per
year. Tis huge increase was over a mere II-year period! And the inci-
dence rate of non-Hodgkins lymphoma has nearly doubled since the early
19 Why So Much Cancer and What Causes It?
I970s. Both breast cancer and prostate cancer have been strongly linked
to pesticide exposure, and non-Hodgkins lymphoma has been strongly
linked to herbicide exposure. Tus, it would seem much more likely that
pesticides and herbicides are bigger contributors to these types of cancers
than genetic inheritance. Moreover, all cancer incidence rates have risen
over just a few generations. Tis sort of rise in all types of cancer would
not be happening if cancer were primarily genetically caused.
Dr. Days second reason to not assume that cancer is primarily an
inherited disease is based on the reality that dierent groups of people
around the world show dierent incidences of various types of cancers
depending on what lifestyle or diet they are engaged in. In countries
where certain types of cancer are particularly rare, the incidence of these
cancers increases when people from those countries adopt a Western diet.
But attributing cancer to dietary factors alone is misleading. As you will
see, there are many environmental and common lifestyle factors that can
contribute to the development of cancer. For example, cigarette smoking
may be the single biggest causal factor to cancer in our modern world today.
It has been estimated that a whopping 30 percent of all cancer deaths
in the United States are attributable to tobacco smoke. Tis means that
if everyone were to suddenly stop smoking, deaths from cancer would
reduce by about one-third!
Te confusing issue is that cancer does, to a certain extent, involve the
genes in cells. But that does not mean it is an inherited condition. For
instance, genes in cells can mutate as a result of being hit by radiation or
because of damage caused by some sort of toxin. Nutritional deciencies
can also contribute to gene damage. Robert Barefoot and Carl Reich,
M.D., make the point in their book Te Calcium Factor that chronic
calcium deciency in a persons diet can precipitate a condition around
cells whereby carcinogens are more able to penetrate the cell walls and
thereby gain access to and cause mutations of genes.
Moreover, researchers have proven that there are certain genes that
can promote the growth of cancer (oncogenes) and certain genes that
can inhibit the growth of cancer (tumor suppressor genes), and that the
activity of these oncogenes and tumor suppressor genes can be turned on or
o by various physiological factors. Tis is critical for people to understand.
Tere are many things in our inner physiological environment that can
either promote or suppress the actions of certain genes within cells. So, yes,
cancer does involve genes, but that does not mean that cancer is geneti-
cally inherited. When it comes to cancer, gene activity simply reects the
20 oursxair \oui caxcii
dynamic state of genes in their interrelationship with the bodys inner
environment.
Tis is not to say that a predisposition to cancer is never inherited.
Tere may be a very small percentage of cases involving some inherited
factor. But very little has been proven about this to date, and what the
evidence proves much more powerfully is that genetic inheritance is not
a signicant cause of cancer. When cancer appears to run in families, it
is more likely that there are other factors, such as diet, lifestyle, ways of
dealing with emotional stress, and so forth, that family members have in
common which are contributing to the development of cancer.
In general, the approach in modern medical science today is to look for
just one thing that causes a particular illness. Tis may be partly why
the search for an inherited genetic cause of cancer is so popular. However,
a great deal of evidence points to cancer as a multi-factorial disease.
Tis means that many factors usually go into the development of cancer
for any particular person. I have come to look at these multiple factors
as falling into two general categories: (I) triggers, and (2) decient
control mechanisms.
Triggers and Decient Control Mechanisms
To understand how triggers and decient control mechanisms con-
tribute to the development of cancer, Id like to use the analogy of a for-
est re. What if someone were to ask the question: What causes forest
res? Looking for just one answer would be silly. We all know there
are many things that can trigger a forest rea commuter throwing a
lit cigarette out the car window into roadside brush; a camper allowing
embers from a camp re to blow up into the limbs of an overhanging tree;
a bolt of lightning during a storm that hits a tree and causes it to ignite;
or sunlight shining through a discarded piece of glass just the right way,
causing some pine needles to ignite. Tese are all examples of factors that
can trigger a forest re.
But does a forest re occur every time one of these triggers happens?
No. Tis is because there are also many factors that will determine whether
or not the initial spark will turn into a raging forest re or not. I refer to
these factors as control mechanisms.
Some of the control mechanisms in the forest re analogy may involve
humans actively putting the re out before it becomes big enough to
be classied as a forest re. But many of the control factors can happen
21 Why So Much Cancer and What Causes It?
without human involvement at all, and these would be factors in the
environment around where the initial trigger, or spark of re, occurred.
For instance, environmental control mechanisms for the above examples
might be: not enough brush and wind occurs along the roadside to fan a
re, so the commuters cigarette spark is short-lived and burns itself out;
the embers from the campers re have blown into the tree leaves of a very
healthy, moist tree, so the re never gets started in the rst place; the bolt
of lightning during the storm starts a tree blazing, but the accompany-
ing rain drenches the tree and puts the re out; or the sunlight shining
through the glass starts a wisp of smoke in some pine needles, but the area
is damp and surrounded by large rocks so the small re has no where to
spread and dies out quickly.
In this way, we can see that there are many triggers that can cause
a spark that could result in a forest re, but there are also many environ-
mental control mechanisms that could stop that spark from turning
into something that rages out of control and causes great destruction. So
too with cancer. Tere are many common triggers, such as random errors
in cell replication, or too much exposure to ultraviolet radiation, radio-
active fallout, pesticides, and other environmental toxins. But there are
also many natural control mechanisms within our bodies to keep these
sparks from turning into raging forest res of cancer.
Most medical practitioners and researchers agree that, in fact, we all
probably have cancer cells developing in each of us all the time, but our
bodies are able to dispose of them before they rage out of control. In other
words, a healthy body can normally defend itself quite well against the
development of cancer because it knows how to deal with these natural
occurrences.
But life in the modern world has skewed the balance between triggers
and control mechanisms for cancer. On the one hand, modern industrialized
societies have introduced countless potent carcinogens and other toxins
into our air, food and water, so that our bodies now have to deal with
many more triggers to cancer than ever before. And on the other hand,
modern industrialized societies have created highly processed, less than
optimum foods and, through advertising, have promoted eating habits
that result in poor nutritional support to our bodies. Tis lack of vital
nutritional support can cause our own natural control mechanisms to
become compromised and decient.
Te sad reality is that there are many more triggers to the development
of cancer in humans than ever before in history, and peoples control
22 oursxair \oui caxcii
mechanisms are generally more decient than ever before as well. Tere
is just no getting around it. When we ask the questionWhy so much
cancer and what causes it?the simplest answer is modern living.
A Disease of Modern Living
Modern living is obviously a broad reference, but it can be easily
broken down into the categories of diet, environment, and lifestyle. For
each of these categories, there are numerous factors that can contribute
to cancer. Some are cancer-causing triggers, others are decient control
mechanisms. Briey listed, some of the most important cancer-contributing
factors of modern living are the following:
Modern Diet
Not enough fresh fruits and vegetables
Too many cooked and processed foods
Foods grown in depleted soils
Not enough essential fatty acids
Too much rened sugar and rened our
Articial sweeteners
Excessive soda, coee, or tea consumption
Chronic dehydration (not enough water)
Modern Environment
Pesticides
Herbicides
Chlorine byproducts (from chlorinated water and other sources)
Fluoride
Asbestos
Fiberglass
Nuclear radiation (from nuclear tests done decades ago)
Modern Lifestyle Choices and Treatments
Cigarette smoking
Birth control pills
Hormone replacement therapy for menopause
Common medical and dental X-rays
23 Why So Much Cancer and What Causes It?
Toxic teeth (from dangerous dental practices)
Childhood vaccines
Chronic stress
Prescription drug use
Tis is not a comprehensive list by any means, but it is enough to give
you an idea of the types of factors today that can contribute to cancer.
Now, lets look in a little more detail at these factors. (Each item above is
listed in bold where it rst appears in the following text.)
Diet
One of the biggest problems with the modern American diet today is
that it typically involves a huge deciency of fresh fruits and vegetables.
Our modern diet has unfortunately developed around speed, ease, and
the protability of the foods being sold. People living fast and on-the-go
lifestyles dont generally have a chance to carry fresh fruits and vegetables
around wherever they go, so they must rely on cooked and processed foods,
which are easier to carry around or prepare quickly. Cooking destroys
important natural enzymes that aid the body in assimilating nutrients,
and highly processed foods are practically devoid of much-needed vita-
mins, minerals, ber, and phytochemicals. Fresh fruits and vegetables, on
the other hand, provide us with many dierent nutrients that help our
bodies defend against the development of cancer.
When we, in modern industrialized countries, do eat fresh fruits and
vegetables, we are often eating produce that was grown in depleted soils.
Te more and more commonly occurring soil depletion results from over-
cropping and the use of chemical fertilizers that do not maintain a proper
balance of minerals in the soil. Tis means that even our fresh fruits and
vegetables may be decient and imbalanced in their mineral content.
Essential fatty acids are another nutritional category critical to the
healthy functioning of the body yet very decient in the common modern
diet. Two of the most important are the omega-3 and omega-6 fatty acids.
Tese are called essential because the human body cannot biosynthesize
them; therefore, they must be obtained through diet. Te omega-6 fatty
acids are primarily found in nuts and seeds, and the omega-3 fatty acids
are primarily found in sh. When you think about it, seeds, nuts, and
sh have been common dietary staples for humans for eons. Yet they are
not abundant in the modern Western diet.
24 oursxair \oui caxcii
When we dont get enough vital nutrients, the cancer control mecha-
nisms in our bodies cannot function optimally. But problems with the
modern diet are not only dened by deciencies. For instance, there is
an overabundance of certain foods such as rened sugar. Rened sugars
and rened ours (which are metabolized like sugar in the body) are
hundreds of times more prevalent in the common modern diet than in
the natural diets humans thrived on for millennia. Tis overabundance
of rened sugars and ours contributes to all kinds of physical problems.
One problem is that, if cancer does get started, lots of sugar in the diet
may help the cancer to thrive because cancer loves sugar.
If a person tries to reduce his or her sugar intake, however, he or she
often does this by replacing white sugar with articial sweeteners such
as aspartame (the sweetener used in NutraSweet, Equal, and Spoonful).
Aspartame is one of the most common articial sweeteners used today,
and yet it was found to cause various types of primary brain tumors in
rats when studies were done in the I970s. Even though these studies
showed a very clear connection between aspartame and brain cancer,
the FDA approved its use as a tabletop sweetener in July I98I. Two
years later, in July I983, aspartame was approved for widespread use in
diet beverages as well. One year after that, the number of human brain
tumors in the United States suddenly increased by I0 percent! Tere are
currently more than 5,000 aspartame-containing products on the mar-
ket today, and it is estimated that over 200 million people in the United
States consume it.
Aspartame is comprised of I0 percent methanol, 40 percent aspartic
acid, and 50 percent phenylalanine. Methanol has been proven to cause
damage to the optic nerve which can cause blindness, and aspartic acid
has been proven to create holes in the brains of mice. Phenylalanine breaks
down into diketopiperazine (DKP), a tumor-causing agent.
Te creation of DKP in the body is one way aspartame can trigger
cancer. Another way is partly related to what happens to aspartame when
it exceeds 86 degrees Fahrenheit, as it often does when, for instance, diet
drinks are being shipped in hot trucks or stored in hot warehouses. At
higher than 86 degrees, the methanol (wood alcohol) in aspartame con-
verts to formaldehyde and then to formic acid. Both formaldehyde and
formic acid are potent carcinogens. In fact, formaldehyde is categorized
in the same class of deadly poisons as cyanide and arsenic. On the other
hand, when methanol occurs naturally, as it does in fruits, it is always in
the presence of ethanol. Ethanol keeps methanol stable and prevents it
25 Why So Much Cancer and What Causes It?
from breaking down into formaldehyde and formic acid. But the metha-
nol in aspartame is free methanol, and thus unstable.
Terefore, not only does the methanol break down into carcinogenic
agents, but the ingredient found in largest quantity, phenylalanine, also
breaks down into a direct tumor-initiating substance. Te brain seems
to be particularly susceptible to these types of damaging substances and
some neurosurgeons have found high levels of aspartame in brain tumors after
the tumors were surgically removed and examined.
But brain cancer is not the only type of cancer aspartame has been
linked to. Animal tests performed between I97I and I974 proved that
aspartame caused mammary tumors (breast cancer) in rats. Nutritionist
Janet Starr Hull, Ph.D., wrote a revealing book on the dangers of aspar-
tame called Sweet Poison. In it, she lists the names of researchers and
their universities who have published studies on aspartame. According
to Dr. Hull, testicular cancer and endometrial (uterine) cancer have also
been associated with aspartame. And in 2005 and 2007 the Ramazzini
Foundation in Bologna, Italy completed animal studies that indicated a
link between aspartame and the development of leukemia and lymphoma
in both male and female rats and mammary gland tumors (breast cancer)
in female rats. (Te link to breast cancer, of course, had already been
found in the earlier I970s studies.)
Tus, it appears that staying away from aspartame is one way to help
oneself avoid cancer. And parents may want to be extra diligent about
checking the ingredients list of anything sweet they give their children.
For instance, aspartame is commonly used now to sweeten childrens
syrups, antibiotics, and vitamins. Given the high rate of brain cancers
and leukemias in children these days, aspartame could certainly be a
contributing factor that needs to be avoided.
Besides cancer, aspartame causes over 90 dierent documented adverse
side eects. Tese side eects include debilitating MS type symptoms,
seizures, coma, blindness, birth defects, and death. Some experts believe
that aspartame was the primary cause of the Gulf War Syndrome suf-
fered by so many American troops. Tis is because thousands of pallets
of diet drinks were shipped to Desert Storm troops where they were left
to sit for weeks at a time in I20-degree Fahrenheit heat. Dr. Hull states
that out of 90 independently-funded studies, 83 of them found one or
more problems caused by aspartame. But out of the 74 studies funded by
the aspartame industry (e.g., Monsanto, G.D. Searle, and ILSI), every
single one of them claimed that no problems were found.
26 oursxair \oui caxcii
Sodas are now one of the most common beverage alternatives to water.
But they are either high in sugar or high in aspartame or some other arti-
cial sweetener. Tey are also high in phosphorus, which can disrupt the
mineral balance of the body. And many sodas contain caeine, which
is a diuretic. All caeinated drinks, whether they are sodas or coee or
tea, can actually contribute to chronic dehydration. Good, clean water
is much more important to drink than many people realize. None of
the cells of the body can work at optimum functioning levels if they are
chronically dehydrated, and many experts believe chronic dehydration
can contribute to cancer by causing cell damage.
So, the common modern way of eating and drinking in the Western
world is full of nutritional deciencies and, at the same time, complicated
with an overabundance of harmful substances. Tis type of diet contrib-
utes to decient control mechanisms. And when an overload of toxins
barrages the body on a daily basis for year after year, there are going to
be problems. Unfortunately, most of these toxins come from our environ-
ment, which includes our air, water, and foods we eat. And more of these
toxins are directly carcinogenic than most people realize.
Environment
Tis category of cancer-causing factors is probably the worst oender.
In our modern world, we are surrounded by toxins in our air, water, and
soil. We eat, drink, and breathe them on a regular basis. For instance, we
breathe in countless petrochemical molecules every day from smog if we
live in a normal industrialized city. But some of the worst chemicals, and
most carcinogenic, are often the ones we dont ever see, feel, or taste.
One primary source of these invisible chemicals is pesticides. Pesticides
are amply sprayed onto our food crops and are also used for household or
garden insect control. I, like many others, used to have the misconcep-
tion that pesticides can be removed from our produce once we get the
produce home from the grocery store and thoroughly wash it. Tis is not
true. Te pesticides sprayed onto crops get into our foods. Tese danger-
ous substances cannot be completely removed by washing the fruit or
vegetable before eating it because they are absorbed into the fruit or veg-
etable as it grows. Tis happens in large part as a result of the pesticides
being washed into the soil around the crops and then being absorbed by
the plants as they take up water and nutrients from the soil.
Tus, no matter how much we wash our fruits and vegetables, we will
27 Why So Much Cancer and What Causes It?
be eating pesticides unless we buy only organic produce from reputable
sources. But even those people who are conscientious about buying only
organic foods will probably also be ingesting at least some pesticides. Tis
is because, through rain and irrigation runo, pesticides have contami-
nated virtually all of our surface and ground water.
Pesticides are similar to articial sweeteners in that small exposures
to them may be considered harmless, but daily exposure over many years
is a very dierent story. Many of the carcinogenic compounds in pesti-
cides do not easily break down over time, and tend to build up in the
body, where they are stored in the fat cells. Tis can cause a cumulative
buildup over the years. Many pesticides produce a potent estrogenic eect,
which means they mimic estrogen in our bodies. (More details on their
relationship to cancer are covered in Chapter I9.) Because so many of the
pesticide chemicals have estrogenic properties, they can be a big factor in
numerous cancers of the body where sex hormones play a rolesuch as
cancers of the breast, uterus, ovaries, and prostate.
In I978, Israel enacted a strict ban of certain pesticides that had been
linked to breast cancer. Previous to this, the occurrence of breast cancer
in Israel had been steadily rising. Over the next I0 years, after banning
these pesticides, breast cancer incidence in Israeli women dropped sharply.
(Tere was an 8 percent overall decline, and a 30 percent drop in breast
cancer deaths for women under age 44.) And this decline in breast can-
cer incidence and mortality occurred while these same rates in the rest of
the world were climbing, and while other negative factors in Israel, such
as alcohol consumption, fat intake, and insucient dietary amounts of
fruits and vegetables, were increasing.
Te I976 Israeli study that had identied these pesticides found them
to occur at much higher concentrations in the malignant tissues of women
with breast cancer when compared to normal breast tissues. Over the
years following the ban, there was a corresponding noticeable drop of
these same pesticides in Israeli cows milk and Israeli womens breast milk.
Tus, these carcinogenic pesticide chemicals were clearly associated with
breast cancer. Te fact that these chemicals have been found in mothers
milk also indicates they can be passed on to infants through breast feed-
ing. Tis scary possibility may be one explanation of why so many young
children these days are developing cancer.
One of the pesticide chemicals that Israel banned in I978 was DDT,
which has been linked to breast cancer by many dierent studies since
the I970s. Most people dont know, however, that DDT is still showing
28 oursxair \oui caxcii
up in our environment here in the United States. For instance, in I996,
80,000 tons of dirt containing DDT were dredged from Richmond Har-
bor in the San Francisco Bay at a site that had previously been a pesticide
packaging plant. Te plant had conveniently dumped much of its resi-
due into the bay. After dredging up this massive amount of dirt, the U.S.
government decided to get rid of it by having it moved and buried in a
landll in Arizona. At some point in the future, the DDT in this landll
is probably going to leach into the surrounding Arizona groundwater and
become a toxic contaminant to humans and animals once again.
But the use of pesticides on crops is not the only way we are exposed
to pesticide carcinogens. A recent Science News article highlighted a
study that showed a link between household pesticide use and child-
hood leukemia. According to the article, written by J. Pickrell, a team
of researchers from the University of California at Berkeley interviewed
families in Northern California over a four-year period (I995I999).
Among these families were 324 children age I4 years or younger. Half
of these children were already diagnosed with leukemia (mostly acute
lymphoblastic leukemia), and the other half were free of cancer. What
these researchers found was that:
Families of the children who had developed leukemia were about three
times as likely to have employed the use of a professional exterminator in
their home than the families who did not have a child with cancer.
Te highest risk to children appeared to occur when a professional
exterminator was employed while the child was two years old.
Whenever a mother was exposed during pregnancy to any kind of
household pesticide, the risk of her unborn child later developing
leukemia was twice as high as for mothers who were not exposed to
household pesticide use during pregnancy.
Tus, regularly spraying our homes for cockroaches, ants, eas, or
other pests may put us in danger of developing cancer in a similar way
that large-scale spraying of food crops can.
Herbicides that are sprayed on lawns and crops to kill weeds also can
contribute to cancer. For example, one of the most widely used herbi-
cides in the world, a chemical called 2,4-D has undergone scrutiny as
a contributor to cancer in humans. Used in lawn products since I944,
2,4-D is particularly good at killing dandelion weeds, which plague parks,
29 Why So Much Cancer and What Causes It?
residential lawns, and golf courses, but it has also been heavily used on
commercial crops.
A revealing Los Angeles Times newspaper article from June I, 2002,
written by Emily Green, stated that Kansas crop workers who had been
working with 2,4-D had a higher than normal rate of non-Hodgkins
lymphoma. Tis article also reported that the overall incidence of non-
Hodgkins lymphoma had increased in farm workers by 75 percent over
the previous 20 years and that some statisticians have now linked heavy
wheat growing regions of the United States (which are notable for their
use of 2,4-D) to higher incidences of cancers of the esophagus, stomach,
rectum, throat, pancreas, larynx, prostate, kidney, and brain.
According to the Times article, one reason the carcinogenic eect of
this herbicide may have gone unnoticed for about 50 years is that the
eect only surfaces as a result of combining dierent ingredients together.
In other words, by itself, 2,4-D is virtually biologically inert, but when
it is mixed with other common ingredients in weed killer products it can
combine with other chemicals to become deadly. Yet, this weed killer is
still commonly sold for residential lawns and gardens and used by many
people who have no idea how cancer-causing it may be.
Smog, pesticides, and herbicides are all sources of environmental tox-
ins that most of us are aware of to at least some degree. But many of the
most carcinogenic environmental pollutants we are exposed to on a daily
basis are ones that most of us are not at all aware of. Te biggest invisible
culprits may be chlorine byproducts, uoride, asbestos, berglass, and
nuclear radiation. In the following paragraphs, these carcinogens will be
introduced briey. But since they are such important issues, they will be
discussed in more detail in the Appendix of this book as well.
Chlorine byproducts, also called organochlorines, are unnatu-
ral compounds that are created as a result of the chemical interaction
between chlorine and organic material. Tey occur largely as a result of
chlorinating public water supplies, but they also occur in our daily lives
from other chlorine sources. According to a joint study conducted by
Harvard University and the Medical College of Wisconsin, the simple
act of drinking chlorinated water accounts for about I5 percent of all
rectal cancers and about 9 percent of all bladder cancers. Tese add up
to about I0,700 cases of cancer every year in the United States that are
suspected to be due to drinking chlorinated water alone.
More details about chlorination are discussed in the Appendix, but
it is worth noting here that one category of chlorine byproduct, called
30 oursxair \oui caxcii
dioxins, has been referred to by scientic experts as the single most car-
cinogenic type of manmade chemical known to science. Read the Appendix
to see how you may be ingesting dioxins every time you eat beef or dairy
products, or even every time you drink a cup of coee.
Fluoride is currently a controversial issue. But it appears to be contro-
versial only on the political level, not the scientic level. To researchers who
have studied it, there is no doubt that uoride is an extremely hazardous
substance to everyones health in many ways.
Besides many other serious health problems, uoride has now been
linked to human cancers of the bone, bladder, liver, mouth, and lung,
and it may contribute to other cancers as well. Dean Burk, Ph.D., former
chief chemist of the National Cancer Institute, has been quoted as saying,
In point of fact, uoride causes more human cancer deaths, and causes
them faster, than any other chemical. Even Proctor and Gamble (the
makers of Crest toothpaste) presented studies to the U.S. Public Health
Service that showed uoride to be a cancer-causing agent at the lowest
concentrations used.
Te public was fooled into accepting water uoridation because the
original tooth-decay prevention tests were done using calcium uoride,
or CaF. Calcium uoride is the type of uoride found naturally in water
and plants. Yet, the type of uoride that got added to public water sup-
plies and toothpaste was sodium uoride, or NaF. As opposed to calcium
uoride, sodium uoride is highly toxic, but it is still the type of uoride
added to many public water sources and common dental products.
Unfortunately, even if you dont drink uoridated water or use uori-
dated toothpaste, that does not mean you are not being exposed to toxic
sodium uoride. Trough water sources, it has now contaminated many of
our foods and numerous commercial beverages such as sodas, juices, teas,
beer, and wine. Exposure to uoride contamination in modern countries
is virtually inescapable. (See the Appendix for more information on the
history of uoridation and studies that link it to cancer.)
Another environmental cancer-triggering substance most people rarely
think about is asbestos. We have heard bad things about it and have
also heard that it has been largely banned and regulated. However, what
we dont know is that a great deal of asbestos is still in our environment.
Countless buildings all over the United States still contain asbestos insu-
lation that releases microscopic bers into the air. Tis includes count-
less modern skyscrapers and tens of thousands of childrens schools. Te
microscopically small bers from asbestos get into the air we breathe and
31 Why So Much Cancer and What Causes It?
take an incredibly long time to settle out of the air. Tey are also virtually
indestructible. Once breathed into the body or ingested into the intestinal
tract, these bers can irritate cells and eventually cause cancer.
Virtually every man, woman, and child in industrialized countries has
now been exposed to asbestos-contaminated air, no matter where they live
or work. It has been estimated that in the 20th century asbestos killed
something like 300,000 asbestos workers, and countless other people
whose cancers and other illnesses are suspected to have been asbestos
related. According to cancer researcher Ralph W. Moss, Ph.D., some
ocials in our government have estimated that possibly I0 to I5 percent
of all cancer deaths in this country are due to asbestos! (For more details
on asbestos and cancer, please refer to the Appendix.)
It took many years before the use of asbestos was regulated in the
United States, but as it was phased out, many manufacturers turned to
the use of berglass instead. Fiberglass has not been studied as much as
asbestos, but many researchers believe it may be just as cancer-causing.
Tis is a controversial subject as well, but if berglass is as carcinogenic as
asbestos, then we are in big trouble because approximately 90 percent of
all the homes in America use berglass insulation. Air circulating through
air condition and heating vents can pick up and circulate microscopic
pieces of this material from the insulation packing. It is as yet unknown
as to how much berglass pollution is in the air we breathe. (For more
details on berglass and cancer, please refer to the Appendix.)
Last but not least, in our look at major environmental cancer-causing
factors we rarely think about, we come to nuclear radiation. Back in I954,
a Hollywood movie called Te Conqueror was lmed on sand dunes out-
side of St. George, Utah. Tis location was about I50 miles downwind
from atomic bomb testing sites. For three months, crew members and
stars including John Wayne, Susan Hayward, Agnes Moorehead, and
producer Dick Powell breathed in dust that was laced with radioactive
fallout. Of the total 220 people involved with that lms production,
9I had contracted cancer by I980 and half of them died of the disease.
Tose who died of cancer included John Wayne, Susan Hayward, Agnes
Moorehead, and Dick Powell.
We cannot be sure that radiation from nuclear fallout was the only
cause of these actors deaths, but the rates of cancer incidence in some areas
of Utah have been so high that, in I990, Congress ocially apologized
to the citizens of Utah and other areas downwind from nuclear testing.
(See the Appendix for more details.)
32 oursxair \oui caxcii
Of course, you may be thinking, Why would nuclear radiation be a
factor in cancer today? After all, were not testing nuclear bombs anymore,
and were not in a war involving nuclear weapons. Te answer is that,
during the I950s and I960s about a thousand nuclear devices were test-
detonated in the Nevada desert as well as in a few other places around the
United States, and the nuclear fallout from those tests is still aecting us
today. Many of the detonations were carried out underground, but I84
were atmospheric, above-ground tests. Radioactive nuclear fallout was
then wind-blown over just about every part of the United States. More-
over, the tests in the United States were not the only sources of nuclear
fallout exposure. It is probable that Americans were also exposed to fallout
blown over the Pacic from the World War II detonations at Hiroshima
and Nagasaki, test detonations carried out in the Pacic, test detonations
carried out in the Soviet Union, and from nuclear power plant disasters
such as Chernobyl and Tree-Mile Island.
Tis wind-blown fallout from domestic tests, as well as from sources
abroad, resulted in a great deal of direct radiation exposure to many
people who later developed cancer. But it also settled onto our crops and
into our soil and water. Since many of the damaging radioactive sub-
stances that settled into our water and soil have a very long half-life, they
are still aecting us today. We still breathe them into our bodies when
dust blows through the air, and we still ingest them through our crops
and drink them in through our water.
Te important thing to remember about nuclear fallout is that some
of the radioactive substances take only about 30 years to deteriorate, but
other radioactive substances take thousands of years to deteriorate. Tis
means that they keep on emitting radioactivity for a very long time. In
other words, the fact that test detonations have stopped does not mean
radiation exposure has stopped.
Once ingested, these radioactive compounds can get stored in various
places in our bodies and keep on radiating. Tat is why nuclear fallout
is capable of causing so many dierent types of cancers over a very long
period of time. Even the National Cancer Institute nally admitted in
a government report in I997 that fallout from bomb tests carried out
in the I950s could have caused up to 75,000 cases of cancer. And since
the NCI was only looking at the eects of one of the many radioactive
isotopes generated, nuclear fallout has probably caused more like hun-
dreds of thousands of cancers in humans. (For more details on nuclear
radiation and cancer, please refer to the Appendix.)
33 Why So Much Cancer and What Causes It?
Modern Lifestyle Choices and Treatments
Tis is a very important category of modern living because it involves
cancer-causing factors we have control over. It is also a very disturbing
category, since it highlights some big cancer-causing triggers that we may
unwittingly choose to subject ourselves to without realizing that we are
greatly increasing our chances of developing cancer by doing so.
Without a doubt, the rst of these factors to look at is cigarette smok-
ing. Te director of the Harvard Center for Cancer Prevention has esti-
mated that tobacco smoke alone accounts for about 30 percent of all cancer
deaths in the United States. Only about one-third of these cancer deaths
involve tobacco-related lung cancer. Tis is because cigarette smoking
has also been linked to cancers of the head, neck, mouth, throat, vocal
cords, bladder, kidney, stomach, cervix, pancreas, and even to leukemia.
Of the lung cancer cases that are tobacco-related, an estimated 20 percent
of them are due to passive exposure. In other words, about 3,000 lung
cancer deaths occur each year in the United States among non-smokers
who have been passively exposed to tobacco smoke.
According to W. John Diamond, M.D., and his co-authors of the book
An Alternative Medicine Denitive Guide to Cancer, the cancer-causing
ability of cigarette smoking was known to the tobacco industry back
around I950. Among a number of studies linking cigarette smoke to
cancer incidence, in December I953, researchers at the Sloan-Kettering
Institute in New York published the alarming results of one scientic
study involving laboratory animals. Tis study showed that when ciga-
rette smoke condensate was simply painted onto the skin of mice, 44
percent of the mice developed cancer.
It is a sobering thought that the number of cancer deaths in the
United States could be cut by one-third if people just stopped smoking
cigarettes.
One of the next biggest cancer-triggering modern lifestyle choices has to
do with the use of synthetic hormones by women. Many modern women
have chosen to use birth control pills or to take synthetic hormones for
relief from menopause symptoms. Whether or not long-term use of birth
control pills can cause cancer is still a controversial subject, but there is a
great deal of research indicating it can be a contributorat least for young
women who start their use of the pill before age 20. On the other hand,
the cancer-causing ability of synthetic hormone replacement therapy
(HRT) for women dealing with menopause has been well established.
34 oursxair \oui caxcii
Te following is a quote from Dr. Walter Willett, M.D., chairman of the
Department of Public Health at Harvard Medical School. He refers to
the current common HRT prescriptions of Premarin and Provera in the
following statements:
Te downplaying of the risk of using animal-derived and synthetic
HRT is even more despicable. Te spin doctors calmly stated that for
every I0,000 women on HRT during one year, only eight more will
have invasive breast cancer, only seven more will have a heart attack, only
eight more will have a stroke, and only I8 more will have blood clots.
Sounds benign, doesnt it? It does, until you do the math.
Tere are 8 toI0 million women currently using HRT. Using con-
servative numbers, that adds up to 6,400 cases of invasive breast cancer,
5,600 heart attacks, 6,400 strokes, and I4,400 cases of blood clots to
organs such as the lungs. Tat adds up to 32,800 cases of drug-induced
morbidity each year !
And the above quote only refers to conservative estimates for HRT-
induced breast cancers, though HRT-induced uterine cancer has also been
well-established. (Tis will be discussed in more detail in Chapter I9.)
Another choice common to modern living is the use of X-rays. It has
been estimated that approximately 78,000 people every year develop
cancer as a direct result of having been given medical and dental X-rays.
Some researchers believe that a majority of breast cancer occurrences may
be caused by medical X-rays given for diagnosing chest and lung problems,
or spinal-related back and neck problems.
One of the most insidious sources of contributing factors to cancer,
unfortunately, may be the eld of modern dental practices. Te subject of
toxic teeth is still controversial, but evidence linking cancer with danger-
ous dental practices exists. Te most common dental practices that have
been linked to cancer are: (I) silver/mercury llings, (2) nickel-alloyed
stainless steel used in certain types of crowns, and (3) root canal proce-
dures. Many alternative practitioners who specialize in treating cancer
agree that it can be important to deal with ones toxic teeth for a better
chance of recovery from cancer. Not everyone has toxic teeth, but those
who do may not know it. Tis is because toxic teeth dont always display
clear warning signs, such as pain in the mouth or abnormal shading on
X-rays. (Chapter 2I presents more details on toxic teeth and what you
can do about them.)
Possibly one of the saddest realities today is that the common practice
35 Why So Much Cancer and What Causes It?
of administering childhood vaccines may be introducing carcinogenic
substances into millions of children and contributing to pediatric cancers.
Tis subject is also very controversial, but some researchers have come up
with information that is quite alarming.
One couple whose two-year-old son was diagnosed with the most
common type of pediatric brain cancermedulloblastomadid their
own informal research, which they posted on the Internet at www.our
alexander.org/burton.htm. Tese parents went through agony when their
small son was diagnosed and suered through two brain operations and
then chemotherapy. After their little boy Alexander died, these parents
tried to gure out why he might have gotten cancer. He had been a strong
child, and no one in his family, going back three generations on both his
parents sides, had ever developed cancer.
Alexanders parents researched how long medulloblastoma tumors gen-
erally take to grow, then looked into what had happened in the months
just before that time. From their sons medical les, Alexanders parents
discovered that just before this tumor had most likely started growing,
Alexander had gotten numerous pediatric vaccines. Ten his parents
researched the available material on these vaccines, particularly on the
DPT, IPV, OPV, and Hepatitis B vaccines. What they found out was
horrifying.
Taken from www.ouralexander.org/burton.htm, here are some of the
facts Alexanders parents discovered:
Tere are six ways that vaccinations may cause cancer, directly or
indirectly.
Standard medicine really doesnt know if vaccines are carcinogenic or
not, because no ocial studies have ever been done on this. In fact,
according to Alexanders parents, None of the vaccines injected into
children have ever been tested for their carcinogenic (cancer causing),
mutagenic (mutation causing), or teratogenic (developmental malfor-
mation causing) potential.
Most vaccines contain carcinogenic chemicals in them, usually in the
form of mercury derivatives, aluminum, and/or formaldehyde. If a
parent were found injecting any of these substances into a child, they
would be charged with child abuse. Yet these potent carcinogens are
in most childhood vaccines.
36 oursxair \oui caxcii
Vaccines sometimes contain viruses, or bacteria that contain viruses,
and some viruses have been associated with certain cancers. Also, vac-
cinations for one type of virus can carry unexpected viruses in them that
may come from the animals used to create the vaccine. For example,
the polio vaccine of the I950s and I960s that was injected into mil-
lions of children was found to carry an unexpected virus from the
monkey kidney cells that were used to culture the polio vaccine. Tis
monkey virus, called SV40, was found to denitively cause cancer. In
fact, in studies with young hamsters that were injected with SV40, 80
percent of them developed brain cancer! When this was discovered,
polio vaccine manufacturers switched to a dierent type of monkey to
avoid the SV40 virus, but in the meantime, millions of young people
had already been injected with it. In I995, the authors of one study on
human brain tumors who published their results in the Journal of the
National Cancer Institute, stated, . . . we found SV40 DNA sequences
in ve of six choroid plexus papillomas, eight of eleven ependymomas,
three of seven astrocytomas . . . None of the I3 normal brain tissues
were positive for SV40 DNA.
Te possibility that many children may be developing cancer as a result
of vaccines given to them to avoid illnesses that are less critical than can-
cer is simply horrifying and is an issue that desperately needs to be more
prevalent in the publics awareness.
Another common aspect of modern life that is connected to lifestyle
choices is stress. Chronic stress is probably the most common type of
modern stress, as opposed to the type of stress generated by a single,
temporary crisis. Chronic stress can result from a lifestyle that creates
daily situations where a person is constantly feeling as though he or she
is racing against the clock or on the edge of a crisis. Mothers and fathers
who try to juggle full-time jobs while raising children and dealing with
extracurricular school activities, busy freeway driving, and so forth, are
prime targets of chronic stress.
But even without fast-paced lifestyles, certain personality traits alone
can sometimes generate chronic stress. Tese tend to be the personality
traits, or learned behavioral patterns, involving how we communicate with
other people and deal with our emotions. People who chronically stu
their anger, frustration, or fear and dont know how to get their emotional
needs met are often suering on a physiological level from chronic stress.
High levels of chronic stress can negatively aect the bodys defenses
37 Why So Much Cancer and What Causes It?
in many ways. It can cause higher than optimum stress hormones to be
produced by the body on a daily basis, which can create an imbalance
in other hormones. Te adrenals are the glands that respond to stress
the most and they release stress-related hormones. If they are chronically
stressed over time, they can eventually become fatigued or even burn
out to a point where they are no longer able to produce their hormones
in optimum levels. Tis can then lead to pH imbalance, poor digestion,
and reduced eectiveness of the thyroid gland, among other problems.
Chronic stress can even deplete the bodys stores of vitamin C, because
this vitamin is used up to create some of the stress hormones that the body
generates. Along with other weakening eects of environmental triggers
and decient control mechanisms in the body, many cancer researchers
believe that chronic stress can actually be a powerful factor in contribut-
ing to the development of cancer.
Finally, one fast-growing area of lifestyle choices that can trigger can-
cer is that of common prescription drug use. Some types of commonly
prescribed drugs such as cholesterol-lowering medications are now being
linked to an increased risk of cancer. It is not always easy to prove whether
a prescription drug can cause cancer or not, but all you have to do is listen
carefully to the many pharmaceutical ads on television in order to get
an idea of the magnitude of this issue. A large number of drugs that are
advertised for non-life threatening conditions actually have lymphoma
stated as one of the possible side eects in these commercials. What much
of the public doesnt know is that lymphoma is a life-threatening form of
cancer! For anyone diagnosed with lymphoma, a 50% chance of being
alive 5 years after diagnosis is a common prognosis, and there is little
assurance of being cured anytime after those 5 years. It is obvious that
Big Pharma is counting on people not understanding what lymphoma
is, and of course lymphoma is not the only type of cancer that many of
these drugs can cause.
Is It All Doom and Gloom?
It is clear that, although cancer has been around for thousands of years,
and has occurred in humans, animals, and even plants for millennia, the
frequency of cancer today has put cancer into the category of a disease of
modern living. After reading about so many possible cancer-promoting
factors in the modern world, it is no wonder that many people who have
eaten well, exercised, and otherwise lived conscientiously healthy lives are
38 oursxair \oui caxcii
developing cancer. But the purpose of this chapter is not to promote a
doom and gloom attitude. In fact, a doom and gloom feeling is already
alive and well with so many of us seeing our friends and loved ones suc-
cumbing to cancer at such a high rate.
On the contrary, the purpose of this chapter is just the opposite. Under-
standing something is the rst step toward releasing fear about that thing
and also toward conquering it. Too many people are being diagnosed with
cancer today and feeling totally confused as to why it happened. Tey
also may feel guilty or bad about themselves. Since there appears to be no
reason why they should have gotten cancer, they may even feel they are
being divinely punished in some way. Under these circumstances, they
may give up all hope of surviving the disease.
But, as we have seen, there are very clear reasons why so many people
are developing cancer today and there are very clear things each one of
us can do to help ourselves avoid a cancer diagnosis or cancer recurrence
(besides using a treatment approach.) We can stay away from toxic dental
practices, stop ingesting aspartame, avoid toxic household pesticide spray-
ing, and say no to non-bioidentical hormones, vaccines and prescription
drugs, to name a few. Tere are also things we can do collectively as a
public to help ensure better health for our children. We can stand up
for our rights not to have pesticides, dioxins, nuclear radiation, uoride,
asbestos, or ber glass in our environment, food, and water.
It is up to us to not fall prey to the two big conventional medicine
lies: I) that cancer is some sort of mysterious aiction that nobody really
understands, and 2) if you have a family history of cancer, that proves its
genetic and runs in your family. Tese two lies simply make people feel
they are powerless to do anything about cancer.
In actuality, cancer is really quite well understood, but you wont nd
this understanding in conventional medicineyoull nd it by looking
into alternative non-toxic treatments. And there is a very good reason
for this. Because alternative approaches are non-toxic, they cannot rely
on a toxic shotgun type of method. Tey have to outsmart cancer by
targeting common characteristics of all cancer cells. Tis brings up the
question, How dierent are dierent types of cancer?
How Dierent Are Dierent Cancers?
Is lung cancer a whole dierent disease from liver cancer or uterine
cancer or prostate cancer? Are leukemias, bone cancers, lymphomas,
39 Why So Much Cancer and What Causes It?
kidney cancer and bladder cancer all dierent diseases? Te simple answer
is that conventional medicine tends to look at cancers in dierent parts
of the body as dierent diseases. But in the alternative cancer treatment
eld, cancer is cancer no matter where it is.
What you will discover in the following pages is that, once cancer
develops in the body, it basically involves the same mechanics and cell
functioning wherever it occurs. Although there are some minor dier-
ences among dierently diagnosed cancers, these dierences are minimal
compared to the similarities that all cancers share. And the dierences
that do show up appear to result more from the fact that dierent types
of body cells and body locations are involved in dierent diagnoses of
cancer. Tus, rather than say there are dierent types of cancer, it would
be more accurate to say there are dierent manifestations of cancer.
One minor dierence the location of cancer can cause is the speed at
which the cancer cells grow. Tis dierence is linked to the type of cell
involved in that particular system of the body. For instance, cancers of
the blood, such as leukemia, replicate faster than many other cancers
simply because blood cells normally have the characteristic of replicating
more quickly than other cells. Another minor dierence is that cancers
in sexual organs are generally much more aected by the sex hormones
of the body than other cancers are. Tis is for the obvious reason that
normal cells of sexual organs tend to have more receptor sites for those
types of hormones, so when those cells become cancerous, they still have
receptor sites.
And yet another minor dierence that may be caused by the loca-
tion of cancer in the body is the circulatory system that is involved. For
instance, cancers of the lymph system and brain are in areas of the body
that have unique circulatory characteristics and this may aect how well,
or how quickly, medicines or nutrients from the blood can get to these
types of cancer.
However, if we look at the most important characteristics of cancer
on the basic level of cellular structure and functioning, dierent types of
cancer are not signicantly dierent. In other words, all malignant cancer
cells share important common characteristics no matter where they occur in
the body. Understanding these common characteristics can help take the
mystery out of cancerbut more importantly, understanding the com-
mon characteristics and mechanics of all cancer cells provides the keys to
understanding how to outsmart your cancer. Te nal key is provided by
the fact that non-toxic treatments can safely be administered over long
40 oursxair \oui caxcii
periods of time, 24 hours a day and 7 days a week. In this way, cancer
cells are never given the chance to grow back in between treatments as
they are with toxic chemotherapy or radiation.
Dierent non-toxic approaches may target dierent characteristics of
cancer, but the outcome is always the same. In other words, they out-
smart and defeat the cancer by either naturally blocking some aspect of
the cancer cells ability to function, by naturally strengthening the bodys
own ability to overcome the cancer, or both. In the next section, you will
read about 2I dierent strategies that others have used to outsmart their
cancer over the past I00 years. Tese are not all of the alternative strate-
gies that have ever been used, but they are approaches that have exhibited
some of the longest and most successful track records and are largely still
available to people within the United States.
To give the reader a historical sense of these remarkable approaches,
they are presented in a somewhat chronological order. Te rst two non-
toxic methods for cancer that were widely used in the U.S. were herbal
therapies in the early I900s. Tese herbal approaches were observed to work
and are still working for many people today, but they have not been well
understood as to their mechanism of action. Even without full scientic
understanding, however, the herbal therapies of the early I900s were work-
ing better than conventional treatments for cancer today. Later approaches
tended to be more completely understood and scientic explanations are
presented in those chapters along with studies and case stories.
If you are currently dealing with a cancer diagnosis, there is hope in
the world of alternative, non-toxic treatments.
Section Two
Alternative
Non-Toxic Treatments
43
3
Te Hoxsey Terapy
W
e begin our in-depth look at alternative, non-toxic cancer treat-
ments with an herbal approach called the Hoxsey therapy. Herbal
treatments are documented as the oldest type of approach to cancer and
have been used with success for thousands of years by indigenous people
all around the world.
In recent years, modern science has proven that many herbs do, in fact,
have cancer-ghting properties. Tey have been shown to support the
bodys immune system, improve blood circulation, strengthen the func-
tioning of major organs, and enhance the ecient elimination of toxins,
among other things. Tey can act very much like a potent drug as well.
For instance, some herbs have direct cytotoxic eects on the cancer cells
themselves, while not harming other cells of the body. Other herbs have
been shown to inhibit a tumors ability to produce new blood vessels to
feed itself, thereby strangling the tumors system of nourishment. And
still other herbs have anti-microbial properties. Tus, herbs are often
referred to as natures medicine and the Hoxsey therapy for cancer is a
wonderful example of this.
Te Hoxsey therapy was the rst widely used alternative non-toxic
treatment for cancer in the modern United States. Still obtainable today,
it is a treatment that consists of an herbal topical salve, an herbal topical
powder, and an herbal internal tonic. Tough many people have never
heard of it, this treatment approach was very successful and was actually
44 oursxair \oui caxcii
used by tens of thousands of Americans in the early to mid-I900s. Around
I953, at the height of the Hoxsey therapy, the main Hoxsey clinic in Dal-
las, Texas had I2,000 patients and was the largest private cancer center
in the world. Tere were also subsidiary clinics in I7 other states.
History
Te history of the Hoxsey therapy is a colorful one. Harry Hoxsey, an
American man born in I90I, was the person responsible for the wide-
spread use of the Hoxsey therapy for cancer. But the herbal remedy had
started farther back in time, and had been passed down to Harry by his
great-grandfather, John Hoxsey. It was John Hoxsey, a horse breeder in
Illinois, who developed the herbal remedy in the mid-I800s. According
to the story as Harry told it, in I840 his great-grandfather John had a
stallion that was expected to die as a result of having developed a cancer-
ous lesion on its leg. Tis horse had been one of Johns favorites, so when
the horse had to be put out to pasture, he kept an eye on it. He noticed
that the horse exhibited atypical behavior by grazing primarily on one
clump of shrubs and owering plants. He also noticed that the horses
cancer completely healed after a number of months and the stallion made
a full recovery.
Curious about his horses amazing return to health, John picked
samples from the plants on which the stallion had been grazing. Trough
experimentation, he developed an herbal tonic, salve, and powder from
them. Some think John Hoxsey may have also gotten input from some
of the local Native Americans about the use of these plants, but no one
knows for sure. He then started using these remedies to treat other horses
suering from external cancers or other types of lesions. Johns herbal
mixture proved to be quite successful, and word spread quickly until horse
breeders were bringing their horses to him from as far away as Indiana
and Kentucky.
John Hoxseys herbal mixtures were eventually passed down to Harrys
father, a veterinarian. Harrys father used the herbal remedies to treat
animals with cancer and other conditions. But he started to quietly use
the herbal treatments to help humans with cancer as well.
When Harry was eight years old, he began assisting his father in
administering these treatments to some of the local people. Tese were
generally people who had no other hope for recovery, and the Hoxsey
remedies were having success. Just before his fathers death, Harry, the
45 The Hoxsey Therapy
youngest in a family of I2 children, was entrusted with the secrets of how
to prepare the remedies and was given the responsibility to carry on the
familys healing tradition.
Harry wanted to do this and enjoyed helping people. He decided to
become trained as a doctor so he could legally administer the remedies to
cancer patients. But coming from a poor coal-mining family, he had to
work very hard to start saving money for medical school. Kenny Ausubel
wrote the most in-depth and well-documented book about the history of
the Hoxsey therapy, titled When Healing Becomes a Crime: Te Amazing
Story of the Hoxsey Cancer Clinics and the Return of Alternative Terapies.
According to Ausubel, Harry did not want to treat any person with cancer
until he had obtained his medical license. But while Harry was saving
up for his medical training, people with life-threatening cancer who had
heard about the success of his fathers remedies kept coming to him and
begging him to treat them. He tried to avoid doing this, but eventually
treated some of them out of the goodness of his heart.
Unfortunately, Harry later discovered that his eorts to get a medical
license would never be successful because, as a result of treating some of
these desperate cancer patients without a license, Harry was blackballed
from entry into medical schools.
Finally, one physician convinced Harry that he could legally administer
his remedies to cancer patients as long as he was working as a medical
technician under the supervision of a licensed physician. Since he couldnt
get a medical license, Harry agreed to do this and began helping people
with cancer under the ocial supervision of various dierent doctors. He
was just in his early twenties, but he was a bright and energetic young
man. Te Hoxsey remedies were very successful, which brought more
and more cancer suerers to his door. Ten, in I924, when Harry was
only 23 years old, he opened the rst ocial Hoxsey Cancer Clinic in
Dallas. It was operational into the I950s and eventually became the big-
gest private cancer center in the world.
Te Hoxsey therapy was mostly known for its success with external
tumors on the surface of the body. People with external cancers were treated
with an herbal paste applied directly onto the tumor and given a liquid herbal
tonic to drink as well. People with internal cancer that showed no external
signs were just given the tonic. Certain dietary changes were also recom-
mended to patients in general, along with a few nutritional supplements.
Te ingredients of Hoxseys internal tonic are well known, with most sources
saying it was made up of potassium iodide, licorice, red clover, burdock
46 oursxair \oui caxcii
root, stillingia root, berberis root, pokeroot, cascara, prickly ash bark, and
buckthorn bark. Tough it was not proven at the time, botanists have
since found all of the herbs in the Hoxsey tonic to have various anti-cancer
properties. And the external salve contains bloodroot, which has been
used by Native Americans to treat cancer for centuries.
But Harry Hoxsey was a renegade self-taught healer, and because he
was not a doctor of medicine, he was constantly being arrested for practic-
ing medicine without a license. Technically, he ran his treatment facilities
legally because he always maintained a supervising physician with a valid
license. But despite this fact, and maybe because established doctors felt
threatened by him, Harry Hoxsey is said to have been arrested more times
than any other person in medical history!
According to Ausubel and others, the biggest reason that Harry Hox-
sey kept getting arrested was because the powerful head of the American
Medical Association, Morris Fishbein, was out to get him. Tey claim that
Fishbein wanted to buy Hoxseys remedies from him, but Hoxsey refused.
Tereafter, it is well documented that the ruthless Fishbein conducted a
personal vendetta against Hoxsey.
Unfortunately for Hoxsey, the American Medical Association was just
coming into its own as a powerful organization, and Morris Fishbein was
not only the head of this organization, but also editor of the Journal of
the American Medical Association (JAMA). Tis journal was becoming a
powerful force, and Fishbein used it as his primary vehicle for discredit-
ing the Hoxsey therapy. In numerous articles over many years, Fishbein
pronounced Hoxseys cancer treatment as nothing but quackery. Jour-
nal articles also ridiculed and discredited any physician who chose to
endorse Hoxseys therapy. In this way, it soon became political suicide
for a doctor or other medical expert to even consider using the Hoxsey
treatment. Te AMAs adamant disapproval of Hoxsey also seemed to
be what prompted many of his arrests for practicing medicine without a
license even though Harry always worked legally under the supervision
of a licensed physician.
What kept saving Hoxsey was the success of his treatment as well as his
own tenacious character. Virtually every time Harry was arrested, groups
of his cancer patients would gather outside the jail as a show of support.
Te crowds got bigger and bigger, and people brought Hoxsey homemade
food and sang hymns outside the jailhouse all day long. Eventually, the
wardens would release him.
Te success of Hoxseys cancer treatment was also what kept getting
47 The Hoxsey Therapy
him acquitted in the many court trials he had to go through. Accord-
ing to Ausubel, in one case, a local deputy sheri refused to serve Hox-
sey with a subpoena, even though he was ordered to do so, because the
deputy sheri himself was undergoing treatment for cancer with Hoxsey.
In another case, Hoxsey was acquitted in a trial because I2 of the jury
members were either former patients of Hoxseys or had relatives or friends
who had been helped by him. In yet another court battle, the trial ended
favorably for Hoxsey because the presiding judge had been raised by a rela-
tive Hoxseys father had cured of cancer. Even several senators endorsed
Hoxseys cancer therapy. And over the many years he was charged with
practicing medicine without a license, not a single cancer patient ever
testied against him.
One of Harry Hoxseys vehement opponents in Texas was Al Templeton,
assistant district attorney. Over a two-year period, Templeton had Harry
arrested more than I00 times. But in an ironic twist of fate, the district
attorneys younger brother, Mike Templeton, came down with cancer of
the intestine. He went through conventional treatment and a colostomy.
But when his cancer was still there and began growing again after the
surgery, Mikes conventional doctors told him there was nothing more
they could do for him. At this point, Mike secretly went to the Hoxsey
clinic for treatment and ended up completely recovering from his cancer.
Upon hearing of his younger brothers unexpected cure, Al Templeton
reversed his attitude toward Harry. After years of continually arresting
him, Templeton became Harry Hoxseys lawyer and began legally defend-
ing him in court instead!
A Texas nurse named Mildred Nelson also believed Harry Hoxsey to
be a quack at rst. Mildred was trained in conventional medicine and
tried to talk her own mother out of receiving the Hoxsey therapy for
cancer in I946. Mildreds mother, Della Mae, was in a desperate situa-
tion. According to Ausubel,
Ranch wife Della Mae Nelson had uterine cancer that had been exten-
sively treated with twenty units of X-ray and thirty-six hours of radium.
She was so badly burned from the radiation that she couldnt even pull
a sheet over her body for a year after. Wasted to eighty-six pounds, she
was bleeding internally, so severely impaired that she had to learn to
walk all over again. Ten the cancer recurred.
When Della Maes cancer recurred, her conventional doctors told the
family there was nothing more they could do for her. Against her daughters
48 oursxair \oui caxcii
wishes, Della Mae then sought treatment at the Hoxsey clinic in Dallas.
She, too, completely recovered from her cancer as a result of the Hoxsey
therapy. (Della Mae Nelson died about 50 years later, in I997, at the age
of ninety-nine. She had outlived most of the conventional doctors and
nurses that had treated her). Needless to say, Mildred was nally con-
vinced that Hoxseys herbal treatment was eective and went to work for
Hoxseys Dallas clinic as a nurse. Mildreds father was subsequently also
treated for cancer by Hoxsey, and he completely recovered as well.
Mildred found Harry Hoxsey to be a compassionate, admirable man
with many talents. She recalled that he had a photographic memory and
never forgot a patients name or face. She also said, He had a sixth sense
if somebody was sick. He seemed to have almost a psychic thing of what
would work for this particular person. Hoxsey claimed to achieve about
an 85 percent success rate for cancers that were external and about an
80 percent cure rate for patients with internal cancer that had not been
already treated with prior surgery or radiation. Many of the bus and
taxi drivers in the local area were so used to transporting and talking to
people who were getting well at the Hoxsey clinic, they claimed it was
where they would go if they got cancer.
During the time that Hoxseys treatment was showing great success,
however, conventional treatments for cancer were beginning to become
a very big business. By the I950s, conventional cancer treatment had
already become focused on surgery, radiation, and the fast-growing eld
of chemotherapy. Some people believe that Morris Fishbein was not the
only obstacle to Hoxseys Terapy, but that the inexpensive and unpatent-
able Hoxsey therapy threatened the emerging cancer industrys big prots
and stimulated opposition from many sources. Te favorite approach
from the conventional medical establishment was to label Hoxsey a
quack or a hoaxer. Tese statements went completely against the facts,
which unequivocally showed that Hoxseys treatment not only worked
for a wide variety of cancer cases, but worked better than conventional
methods of the day.
Since most quacks are in it for the money, if Hoxsey was a quack, he
wasnt a very good one. All of the Hoxsey clinics admitted and treated any
cancer patient who came to them, even those that could not pay. Ausubels
book documents numerous times when Hoxsey exhibited generosity to
his patients above and beyond the call of duty, including fully treating
people who had used up their last dime on bus fare to get to the clinic.
Many times Hoxsey then drove them to a local place where they could
49 The Hoxsey Therapy
stay. In reality, Hoxsey was following the advice his father had given
him when he handed the responsibility of the family remedies over. His
father said:
Now you have the power to heal the sick and save lives. What Ive
managed to do in a tiny part of this state, you can do all over the country,
all over the world. Ive cured hundreds of people. You can cure thousands,
tens of thousands.
But its not only a gift, son; its a trust and a great responsibility. Abe
Lincoln once said God must have loved the common people because he
made so many of them. Were common, ordinary people. You must never
refuse to treat anybody because he cant pay. Promise me that!
In I954, an independent group of I0 doctors from various parts of
the United States made a point of investigating Hoxseys clinic in Dallas.
After the two-day inspection, which included examining hundreds of
case histories and talking to patients and ex-patients, this independent
group of physicians made a stunning public conclusion. Tey reported
that the Hoxsey clinic
. . . is successfully treating pathologically proven cases of cancer, both
internal and external, without the use of surgery, radium or x-ray.
Accepting the standard yardstick of cases that have remained symptom-
free in excess of ve to six years after treatment, established by medical
authorities, we have seen sucient cases to warrant such a conclusion.
Some of those presented before us have been free of symptoms as long
as twenty-four years, and the physical evidence indicates that they are
all enjoying exceptional health at this time.
We as a Committee feel that the Hoxsey treatment is superior to
such conventional methods of treatment as x-ray, radium, and surgery.
We are willing to assist this Clinic in any way possible in bringing this
treatment to the American public.
Here, nally, was the type of ocial medical endorsement that Hoxsey
had been looking for to help him spread the treatment to more and more
people. Unfortunately, this was not to be. Te report of the I0 indepen-
dent doctors was ignored by all inuential parties.
Tus, Hoxsey was not only powerfully opposed by Morris Fishbein
but also by others in the cancer industry. Te higher-ups in the AMA
may have been his most vehement opponents, but other organizations
such as the NCI and FDA also helped to suppress any fair assessment of
the Hoxsey therapy. Even though Hoxsey repeatedly pleaded with these
50 oursxair \oui caxcii
groups to conduct scientic studies on his formulas, and even though
thousands of patients were recovering from cancer as a result of Hoxseys
herbal mixtures, the ocial cancer industrys response was not to study it.
In fact, unbelievably, ocial representatives from the FDA would actually
go to patients houses, intimidate them, tell them they were being duped
by a quack, and take away their Hoxsey medicines.
Morris Fishbein eventually delivered a powerful blow by ocially
claiming Hoxsey as a hoaxer in a segment that was published in a Sunday
newspaper segment and read by about 20 million people. Hoxsey sued
Fishbein and the Hearst newspaper for libel and slander, and 50 of his
cancer patients testied on his behalf in court. Fortunately, Harry Hoxsey
won the lawsuit, although he was only awarded 2 dollars by the court.
Te following excerpt from Richard Walterss book, Options, lays to
rest any doubts that suppression of good, non-toxic cancer treatments
has truly happened. Referring to Dr. Morris Fishbein after the Hoxsey
lawsuit, Walters writes:
Te leader of Americas quack attack was now on the defensive.
Critics charged the AMA with being a doctors trade union, setting
national medical policy to further its own selsh interests. Te United
States Supreme Court agreed that the AMA had conspired in restraint
of trade. Dr. Fishbein was forced to resign.
In I953, the Fitzgerald Report, commissioned by a United States
Senate committee, concluded that organized medicine had conspired
to suppress the Hoxsey therapy and at least a dozen other promising
cancer treatments.
But despite his legal victory over Fishbein, Harry Hoxseys opponents
eventually proved too powerful and all his cancer treatment centers were
forced to shut down. Te Hoxsey clinic in Dallas closed its doors in
I960, and its long-time chief nurse, Mildred Nelson, ended up moving
the operation to Mexico where she faithfully administered the treatment
for many more years. Tus, the Hoxsey therapy was nally pushed out
of the country and eectively denied from the American public at large.
After a lifetime of ghting conventional medicine, Harry Hoxsey died
in I974. He had developed cancer of the prostate, and some sources refer
to how ironic it was that he couldnt cure himself of cancer. However,
Ausubel, who researched Harrys history more meticulously than anyone
else, says that he did cure himself of his cancer using his own remedy
and in fact died of other causes. Paul Peters, M.D., Harrys last doctor of
51 The Hoxsey Therapy
record, adamantly claimed that Harry died of liver trouble and a weak
heart. He vehemently said that before his death Harry was free of cancer.
But Dr. Peters was out of town when Harry died, and another physician
was required to sign the death certicate. Tis physician, not knowing
the true cause of death, merely looked at Harrys medical records, saw
that he had had prostate cancer, and wrote that down as the cause on his
death certicate.
Current Hoxsey Terapy
Eective cancer treatments dont die easily, however, and the Bio-
Medical Center in Tijuana continues to operate and administer the
Hoxsey therapy. Harrys nurse, Mildred Nelson, ran the center for 25
years after Harrys death and provided cures for many people until her
own death from a stroke in I999. Te Bio-Medical Center is now being
run by Mildreds sister, and information below indicates how to contact
this treatment center. Te Hoxsey therapy has been known to work suc-
cessfully for many dierent types of cancer, and the center in Tijuana
is currently claiming that the best responders to the treatment are those
diagnosed with lymphoma, melanoma, or other types of external skin
cancers. Some people nd traveling to Mexico for treatment a bit daunt-
ing, but the comparatively low price of this treatment makes up for that
diculty for many. Some also nd that using Laetrile along with the
Hoxsey therapy is helpful. (See Chapter 6 for a discussion of Laetrile.)
People with cancer who go to the Bio-Medical Center today do not
stay there as in-patients but make day visits over the border. Tese people
are dicult to follow up on because they tend to go back home to other
countries, so it is not easy to assess whether the treatment still has the
same ecacy as it did when it was under Harry Hoxseys administration.
Hopefully, the United States will pass more freedom of medical choice
legislation, and this amazing herbal treatment will someday be able to
return to its U.S. homeland and be developed and studied further.
52 oursxair \oui caxcii
Resources:
Physical Address: Mailing Address:
Bio-Medical Center Bio-Medical Center
3170 General Ferreira Col. Madero Sur P.O. Box 433654
Colonia Juarez San Isidro, CA 92143
Tijuana, Baja California
22150 Mexico
Phone: (01152664) 684-9011 Email:
FAX: (01152664) 684-9744 BioMedicalCenter@prodigy.net.mx
Treatment at Bio-Medical Center: Te total cost of treatment is about
$3,500. Patients pay a set lifetime rate that is the same for everyone
and covers as many visits and as much treatment as is needed. Patients
are asked to arrive by 9 a.x., Monday through Friday, and will be done
by 4 i.x. No appointments are necessary.
For a consultation with the Bio-Medical Center: Consultations are extremely
inexpensive. Bring any X-rays, blood test results, and so forth that are
less than one-month old. If you dont have these with you, you may be
charged to have them done there.
Books
Kenny Ausubel. When Healing Becomes a Crime: Te Amazing Story of the
Hoxsey Cancer Clinics and the Return of Alternative Terapies. Rochester,
Vermont: Healing Arts Press, 2000.
Richard Walters. Options: Te Alternative Cancer Terapy Book. New York:
Avery Penguin Putnam, 1993.
Video
Hoxsey: How Healing Becomes a Crime can be ordered by calling (505)
989-8575.
53 The Hoxsey Therapy
Websites
www.alkalizeforhealth.net/Lhoxsey.htm
www.yesyoucansayno.com/history.htm
www.whale.to/c/hoxsey.html
www.mnwelldir.org/docs/cancer1/altthrpy2.htm#Hoxsey%20Formula
55
4
Essiac Tea
N
o book on alternative cancer treatments would be complete without
a discussion of the herbal tea treatment called Essiac. Like the
Hoxsey therapy, Essiac has been used since the early I900s and also has
a colorful history. One of the Essiac herbs, burdock root, is also part of
the Hoxsey herbal therapy. While the Hoxsey herbal formula came to
America from a horse rancher, the Essiac herbal tea came to Canada as
a gift from Native America.
Te history of Essiac begins in the late I800s with a Canadian woman
who was suering from advanced breast cancer. She happened to meet
an Ojibwa Indian medicine man, who told her he could cure her of her
illness. She didnt want to have the surgery her doctors recommended, so
she decided to accept the medicine mans oer instead. He showed the
woman four herbs that grew naturally in her area and told her how to
pick them and brew them into a tea. He instructed her to drink the tea
every day. Te Canadian woman did as she was told and subsequently
completely recovered from her advanced breast cancer.
Tirty years later, in I922, this same woman was a patient in a Cana-
dian hospital in northern Ontario. Rene Caisse, the head nurse, was
bathing the now elderly woman one day and noticed a great deal of scar
tissue on the womans breast. When she inquired about it, the woman
told her about how she had been dying from breast cancer 30 years ear-
lier and was cured by an Indian herbal formula. Caisse was extremely
56 oursxair \oui caxcii
interested, especially since the elderly woman had not had a recurrence
of her cancer in 30 years. According to one account, Caisse wrote down
the names of the herbs from her patient in the hospital. According to
another account, she visited the medicine man herself and was given the
herbal remedy directly.
However it occurred, Nurse Caisse found that the four herbs were
sheep sorrel, burdock root, slippery elm bark, and turkey rhubarb root.
Tere may have been other herbs she was originally told about, too, but
these are the four she ended up using. Nurse Caisse was told that when
blended and brewed together in a certain way, these herbs had more cura-
tive power than any of the four herbs individually had.
About a year after receiving the herbal formula, Rene Caisses aunt
was diagnosed with stomach cancer that had metastasized to her liver.
Te doctors had given up on her aunt, so Caisse brewed the herbal tea
and administered it to her. Te tea worked and her aunt lived another
2I years.
Caisse then started collecting the wild herbs on a regular basis and
preparing larger and larger portions of the remedy in her kitchen. She got
permission from one doctor to administer the remedy to some terminally
ill cancer patients the Canadian medical profession had no cure for. Soon,
she was treating more and more cancer patients. When she wanted to pick
a name for her concoction, Caisse decided to spell the letters of her last
name backwards. Tat is how she came to name the herbal tea Essiac.
With the supervision of some doctors who supported her work, she
was able to leave the hospital and start up her own cancer clinic in Brace-
bridge, Canada. She was 33 years old at the time. From I934 to I942,
Rene Caisse treated thousands of cancer patients who had no other hope.
Tough she never claimed her treatment was a cure, it turned out to be
just that for many people. Caisses own mother developed liver cancer at
one point and Rene put her on Essiac. Her mother recovered and went
on to live another I8 years.
Most people who tried Essiac came to it as a last resort. Because so
many of these people were in very late stages or had already sustained
damage to their vital organs, not everyone was able to fully recover. For
many, Essiac was only able to control the cancer, and for still others it
was successful only at alleviating pain. But literally thousands of people
reported complete cures from their cancer. Nurse Caisse never required
payment for administration of her cancer therapy. She did, however, accept
57 Essiac Tea
donations from anyone who could aord to give them, and her clinic was
supported by these donations alone.
According to Dr. Gary Glum, an expert on Essiac who wrote the book
Calling of an Angel, the Royal Cancer Commission of Canada held hear-
ings in I937 and came to the conclusion that Essiac was a cure for cancer.
Finally, the Canadian Ministry of Health and Welfare and the Canadian
Parliament became involved. Around I938, grateful former patients and
friends of Rene Caisse petitioned the Parliament to give Caisse the legal
right to administer her remedy to anyone who asked for it. Te petition
was submitted to the Parliament of Ontario with an incredible 55,000
signatures on it. Tis action initiated a bill in the Ontario Parliament. If
passed, the bill would allow Rene Caisse to legally treat cancer patients
without the constant threat of arrest. It would also give credibility to
Essiac as a recognized treatment for terminally ill cancer patients. Unfor-
tunately, this unprecedented measure fell just three votes short of being
passed, and Essiac was not given the legitimacy it deserved.
Charles A. Brusch, M.D., was a well-known and highly esteemed doc-
tor in the United States who had been the personal physician to John F.
Kennedy. Dr. Brusch heard about Essiac and became very interested in it.
Between I959 and I962, Dr. Brusch worked closely with Rene Caisse and
together they treated thousands of cancer patients out of Bruschs clinic in
Massachusetts. Dr. Brusch spent about I0 years studying Essiac in depth
and using it clinically. After these I0 years, he concluded that Essiac is
a cure for cancer, period. All studies done at laboratories in the United
States and Canada support this conclusion. He even developed cancer
himself and used Essiac to bring about his own complete recovery.
According to Dr. Glum, the Memorial Sloan-Kettering Cancer Cen-
ter in New York also studied Essiac. However, some sources state that
Rene Caisse was very protective of her formula and would not reveal all
of the ingredients or methods of preparing it. Tese sources state that
Caisse only allowed Memorial Sloan-Kettering to study one of the herbal
ingredientsthe sheeps sorrel. Dr. Glum states that Dr. Chester Stock
at MSK did the research and discovered that the sheeps sorrel did have
powerful anti-cancer properties. Glum also claims that this information
was withheld from the American public, but was given to the Canadian
Ministry of Health and Welfare. After receiving this information, rather
than supporting the use of Essiac for cancer, the Canadian government
immediately banned the sale and distribution of the sheep sorrel herb.
58 oursxair \oui caxcii
(It is not banned in the United States or other countries, however.) One
can only guess at their reasons for doing this.
During the I960s and I970s, Rene Caisse tried to get various pharma-
ceutical companies interested in producing her formula for widespread use.
Te only stipulation she gave them was that Essiac be put to immediate
use with cancer patients. But Caisse would not give her formula to the
pharmaceutical companies for testing unless they signed the agreement
she requested, and without being able to test the formula rst, the phar-
maceutical companies would not sign the agreement.
Finally, in I977, just before her death, Rene Caisse sold her formula
to the Resperin Corporation of Toronto for a dollar. She also reportedly
gave her formula to two of her friends, Mary Macpherson and Gilbert
Blondin.
Rene Caisse had treated cancer patients with Essiac for almost 60
years before she died in I978 at the age of 90. Immediately after her
death, the Canadian Ministry of Health and Welfare went to her house
and destroyed all of her paperwork on the Essiac formula. Tey burned
her records in 55-gallon drums behind her house. Again, one can only
guess at their reasons for doing this.
Te Resperin Corporation took years to run tests on Essiac, and people
in Canada could then only obtain Essiac by having a doctors note saying
they had terminal cancer and needed Essiac on an emergency basis. Even-
tually, however, Resperin Corporation produced the Essiac formula for
widespread use. Tis version of it is now sold commercially out of many
health food stores as well as from many sites on the Internet. Resperins
Essiac comes in dry powdered form in a box with instructions on how to
brew it up as a tea at home.
But because of the delay by Resperin Corporation to market Caisses
herbal tea, another form of Essiac began to develop for commercial sale
in the I980s. Tis version of Essiac was backed by Dr. Brusch and was
based on his clinical work with Caisse and her herbal remedy. It came to
be called Flor-Essence.
Te development of Flor-Essence started out with a radio talk show
host in Canada named Elaine Alexander. Alexander had become inter-
ested in Essiac and had already interviewed many people who testied
to her that they had recovered from their cancer using Essiac alone. In
I984, she phoned Dr. Brusch and told him she was interested in doing a
series of radio shows about Essiac and told him she would like to inter-
59 Essiac Tea
view him on the air. He agreed to do this and the rst radio interview
lasted two hours.
In that rst radio show, Dr. Brusch told the public in no uncertain
terms that Essiac was, indeed, a cure for cancer. Te response from the
public was unlike anything Alexander had ever seen in her 20 years in
radio. All the phone lines into the station were jammed for hours with
people calling in. Before the rst show was over, several people had even
driven to the radio station and were waiting outside in the hopes that
they could get their questions answered!
Elaine did more on air interviews with Brusch and had terminal cancer
patients who had been cured by Essiac as guests as well. Her radio shows
on Essiac became a phenomenon and she was soon overwhelmed with
people needing her help as to what they could do and how they could
get Essiac. Some cancer patients got her address and began camping out
at her house to get advice and help.
For several years, Alexander and Dr. Brusch did their best to help the
people with cancer who were coming to them. Finally, in I988, Alexan-
der proposed to Dr. Brusch that the two of them become partners and
produce their own Essiac product. Tey both agreed at this point that it
would be best to circumvent the medical establishment, which up to this
point was not responding to Essiac in any helpful way. Tey decided to
drop the Essiac name because it was too closely associated with a cure
for cancer, and thus too controversial, and they decided to simply sell it
as an herbal detoxifying tea.
Brusch and Alexander looked for a manufacturing company that could
meet the standards required for producing a high-quality herbal prepa-
ration, and they settled on a company called Flora in British Columbia,
Canada. Te herbal tea was produced and sold in bottled liquid form,
and named Flor-Essence. Flor-Essence can be bought today at many
health food stores as well as over the Internet.
Currently there are two main versions of the Essiac herbal tea being
marketed. One is Essiac from Resperin Corporation, and the other is
Flor-Essence from the Flora company. Besides these two, there are count-
less smaller herbal companies and private herbalists that produce and sell
Essiac herbs to be brewed into tea at home. Tey all seem to have cura-
tive eects. Although the various forms of Essiac have never been fully
accepted as formal cancer treatments, they are still being used by many
people to help them recover from cancer. Right now, this herbal formula
60 oursxair \oui caxcii
is used in some form in every state of the United States, Canada, Mexico,
Australia, Europe, Asia, and Africa.
Tere is still some controversy, however, as to the details of the original
formula Rene Caisse used. Te Resperin Corporation claims they have
the true original formula containing just four herbs. Dr. Charles Brusch
and Elaine Alexander, however, assert that Brusch was given the true
original formula from Rene Caisse and that it contained the four herbs
Resperin uses, but also contains four additional herbs: blessed thistle, red
clover, watercress, and kelp. Tese herbs are added to their bottled version
of Essiac called Flor-Essence.
It seems impossible at this time to know who has the original formula
Rene Caisse used on so many thousands of patients. Other sources of
Essiac are sometimes referred to as Ojibwa Tea, Ojibwa Tea of Life,
or 4-Herb Tea.
It is dicult to know which form of Essiac tea is best to recommend.
I have read about and heard of some people with cancer getting well
through the use of pretty much all the versions available. However, I
have also heard of people for whom Essiac was not powerful enough to
achieve full recovery from. One experienced herbalist told me that the
quality of the herbs used is critical. Tere may be a big dierence between
the potency of herbs picked from good wild soil as opposed to chemi-
cally fertilized soil. And exactly how and when the herbs are picked and
brewed is possibly even more important. Many factors seem to contribute
to how potent or eective any herbal treatment will be. Also, Rene Caisse
injected the sheep sorrel into her patients and none of the herbal remedies
today use that approach.
Tere can be no debate that herbal remedies such as the Hoxsey therapy
and Essiac have, historically, been extremely powerful anti-cancer treat-
ments. In todays modern world, there are still people getting well from
cancer using these herbal treatments. Finding herbal sources today that
use good quality herbs and prepare the herbs optimally is the biggest con-
cern. Since it is dicult to be sure of the ecacy of any particular version
of Essiac, it might be best to use it in conjunction with another recovery
approach with which Essiac tea is compatible. Te only approach I know
of that is denitely not compatible with Essiac, is Protocel
eectively targets cancer cells and other unhealthy cells without harming
any of a persons normal healthy cells.
Protocel
can
be eective in improving a variety of health problems. It is important
to understand that Protocel
. Later,
it was renamed Cancell
and then nally Protocel
. Today, Protocel
is
the only true duplication of Jim Sheridans original Entelev
/Cancell
formula according to the Sheridan family. Te following is a brief history
of how this product came into being.
Jim Sheridan was born in I9I2 in a Pennsylvania mining town. His
father and both his grandfathers were coal miners. To help support his
family, he had to work side jobs while he was going to high school. Finally,
121 Protocel
does not hurt them. Tis is why Protocel
eectively
reduces their respiration ability just enough to push them down the redox
ladder to where they are fully in the primitive zone, or even past it. At this
point, the cancer cells are not able to produce enough energy to survive,
and they subsequently die o through the process of lysing. In one article,
Sheridan wrote that the way his formula aects cell respiration is
. . . by shunting o energy units of the cell as it is working, so the
energy is not going through the respiratory system. (An energy unit is
two electrons and a proton). Tus, work is being done by the cell, but not
respiration . . . If work is being done, but not respiration, the cell is forced
127 Protocel
, this egg
white-like material may come out of them through any avenue that the
body uses to get rid of waste. Tus, people using Protocel
is not
a collection of anti-cancer ingredients and none of the individual parts
are important in themselves. Protocel
directly kills cancer in this way, though technically there are no whole
dead cancer cells left over when Protocel
and Cancell
.
Tus, people have only been purchasing this formula as an ocial
product since the year 2000but many were able to use it for free at
least as far back as the I980s. When Protocel
Formula
23 and the original Cancell
Formula 50.
(NOTE: Anyone who is impressed with the following case stories
and interested in using Protocel
Case Stories
He went in for a general checkup and renal cell cancer was found in his
left kidney. Gunthers doctor told him that chemotherapy does not work
very well for kidney cancer, and he recommended that Gunther have his
kidney entirely removed.
While Gunther was thinking about this, he searched the Internet for
more information. Incredibly, he found four other people who had been
in a similar situation to him. Tey all four had renal cell cancer in one
kidney, and they all four had had their kidneys removed. Unfortunately,
they all four said that the kidney cancer had then metastasized to other
parts of their bodies. Te good news, however, was that all four of these
people had then recovered from their metastasized kidney cancer by using
Cancell
.
Toward the end of April, Gunther traveled to Germany. Someone
there convinced him to seek a second opinion about his kidney cancer.
He agreed to do this and had a consultation with a cancer specialist there.
Te German specialist came to the same conclusion as Gunthers American
doctor, and told him he should have his kidney taken out.
At this point, Gunther decided to have his kidney removed and made
an appointment with the German doctor for the surgery. But before the
surgery was performed, Gunther heard that a doctor back in the United
States at the Cleveland Clinic was one of the worlds best specialists on
kidney cancer. He immediately called from Hamburg to make an appoint-
ment at the Cleveland Clinic, cancelled his surgery, and ew back to the
United States to consult with this top kidney cancer specialist instead.
In Cleveland, another CT scan was performed and the specialist pro-
nounced again that Gunther had a dangerous renal cell tumor on his left
kidney. His right kidney looked ne with just a benign cyst on it. Tis
doctor said the same thing as the other two had. He suggested Gunther
have his kidney removed. Gunther nally scheduled the recommended
surgery with this specialist and it was set for mid-July I997. (He was also
still taking the Cancell
for
about two years (from April I997 to mid-I999), then stopped the Cancell
and didnt worry about it anymore.
In September 2000, however, Gunther became ill and developed a
high fever. After hearing about his history of cancer, the doctor did an
ultrasound on his kidney and surrounding areas. Te result was that the
doctor could not nd any tumor at all.
At the time of this writing, Gunther is now almost 87 years old and
more active than many young people. He swims laps every morning for
45 minutes, he is still active in business, and he travels around the world
quite a lot for pleasure. No one would guess that hed been diagnosed
with kidney cancer six years earlier. And no one would guess that he had
never gone through any surgery, chemotherapy, or radiation. Te only
thing he ever did was to take Cancell
.
Case Story #3Pancreatic Cancer
Pancreatic cancer is well known as one of the most deadly types of
cancer. So it was truly exciting to speak with a 69-year-old man who had
recovered from this type of cancer through the use of Cancell
alone.
His name is Bill.
In March of I988, Bill was diagnosed with pancreatic cancer and his
doctor didnt think he would live more than six months. He chose not to
do conventional treatment of any kind, and instead immediately started
taking Cancell
Case Stories
Case Story #4Breast Cancer Metastasized to Bones
A story of breast cancer that had metastasized to the bones was told
to me by a woman named Roberta. Roberta was 65 years old when I
spoke with her, but when she was only 4I, she was diagnosed with breast
cancer. Tat was in October I979. Back in those days, doctors didnt do
lumpectomies, they just went straight to mastectomy. So she underwent a
mastectomy immediately after her diagnosis and, during the surgery, ve
of her lymph nodes were removed to see if the cancer had already metas-
tasized. Unfortunately, it had. After the surgery, Roberta was treated for
about six months with chemotherapy and toward the end of that period
she also went through a three-week round of radiation.
Roberta went through the full treatment regimen that her doctor had
planned for her. But after completing it, she started having some physi-
cal problems as a result of the chemotherapy and radiation. One of the
problems was that, as a result of the radiation being targeted near her
throat, Roberta began having serious diculty swallowing. Te other
problem was that she suddenly developed insulin-dependent diabetes.
Tis last development was quite a surprise, since she had never suered
from any sort of diabetes before, nor had she shown signs that she was
starting to develop it.
After receiving the lumpectomy, chemo, and radiation, Roberta was
given a bone scan. But the results showed that the cancer was not gone
and had, instead, metastasized to her bones with spots on her clavicle and
ribs. Luckily for Roberta, she had heard about Entelev
.
Elonna was skeptical about Cancell
at rst. Her initial words to
her husband were, If there was a cure for cancer, dont you think they
would be using it instead of letting thousands of people die? But she
had no other choice and her husband seemed to have faith that Cancell
would work. On November I2, I989, Elonna started taking Cancell
.
135 Protocel
Case Stories
She decided to refuse the conventional treatments of chemotherapy and
radiation that had been oered to her since they could promise her no
more than six months anyway. She really wanted to be able to take care
of her babies and watch them grow up.
At the end of Elonnas second week on Cancell
to her around the clock.
According to Elonna, after several weeks, she began to notice an
improvement in her condition, though she still could not walk. However,
it was only I8 hours after her rst dose that she began to eliminate the
cancer waste product. She says, It literally poured out of me: I threw it
up; my bowel movements were extremely loose and stringy and frequent.
I lost it in my urine; my nose ran so much I had to keep a tissue with me
at all times. I sweated it out profusely; and I had hot and cold ashes and
night sweats. When the nurses would give me a sponge bath after a night
sweat, the water would be a golden brown color with what they referred
to as tapioca balls oating in it.
Te lysing symptoms Elonna experienced were worth it. Amazingly,
by February I990, only about three and a half months after she started
on Cancell
, new scans of her brain and entire spinal cord came back
negative for any signs of cancer.
Elonna stayed on Cancell
Case Stories
tumor, but proclaimed that they couldnt get it all. Her cancer had not
yet metastasized, but the tumor was shaped like a large comma and the
tail end of it, which would have been too risky to remove, still remained
in her body after the surgery. Sarah spent three weeks in intensive care
and then her doctors wanted to schedule her for more aggressive treat-
ment with chemotherapy. Sarah did not want to undergo this course of
treatment and atly refused.
Toward the end of the summer, Sarah had still not done any more
treatment of any kind since the surgery and was back to feeling very sick
every day. But by this time her daughter had heard about Protocel
and
she was able to convince her mother to try it. In August 200I, Sarah
started taking Protocel
and contin-
ued to decline conventional treatments. Over the next few months, Sarah
felt better and better and more than two years later, she was still feeling
great. At that time, a series of comprehensive lab tests all indicated that she
was in remission and as Sarah liked to say, on Protocel
and prayer!
Case Story #8Prostate Cancer
Sarahs 89-year-old husband, Bernard, also had a Protocel
story to
tell. At age 85, Bernard was diagnosed with prostate cancer. His doctors
surgically removed a tumor on his prostate and Bernard was scheduled
to get some follow-up treatments to make sure the cancer did not recur.
But unfortunately, Bernards doctor suddenly died, and as a result Ber-
nard did not get any more treatment of any kind for eight months. Ten
he heard about Protocel
alone, his PSA was down to 4.
Bernard never did any conventional treatment other than the surgery
for his prostate cancer. At the time of this writing, he is still doing ne
and considered cancer-free.
Case Story #9Prostate Cancer
Albert is 73 years old. Five years ago, Albert was diagnosed with
prostate cancer. A needle biopsy was performed that included ve or six
samples, and from these Alberts prostate cancer was given a Gleason
scale rating of 4.5. (Te Gleason scale is a scale from I to I0 that indi-
cates how aggressive, or fast-growing, a mans prostate cancer is.) Tus,
Alberts cancer was just about in the middle of this scale. His PSA level
at the time was I3, and his prostate gland was enlarged.
Luckily for Albert, he already knew about Protocel
at the time he
was diagnosed and he immediately went on the formula. Albert never
underwent surgery, radiation or any other conventional treatment for his
cancer. After six months on Protocel
Case Stories
him in horror. A CT scan showed that Steve had an abnormality in the
left frontal lobe of his brain. He was given a common anti-convulsant
drug called dilantin to keep his seizures under control. A few weeks later
after a biopsy, Steve was told that he had a malignant tumor, just under
the skull in his speech center, which was about 80 percent the size of
a golf ball. It was surgically removed and diagnosed as an anaplastic
astrocytoma, grade III. Steves prognosis was grim. He was told he had
about a I0 percent chance of living ve years, but only if he did numerous
rounds of radiation, likely to be followed by chemotherapy.
At this point, which was 35 days after his surgery, he underwent
another MRI. Te cancer he was dealing with was apparently extremely
aggressive (fast-growing) because this MRI showed that the tumor had
already grown back. Steve spent an arduous recovery after the surgery
and opted for the recommended 35 days of radiation treatments. But he
did only three days of treatments and decided he had gathered enough
evidence that he believed Protocel
Formula 23 alone. After four weeks on Protocel
,
and two months later another MRI was performed. Tis time the scan
showed that the tumor had greatly reduced in size. Two months more on
Protocel
and the tumor was even smaller and no longer enhancing! Tis
meant that the MRI no longer showed active cancer and the remaining
tumor mass could be considered benign.
Steve was told by others who had used the formula that, after about
four to ve weeks on Protocel
, and as of this
writing in March 2004, he is continuing on Protocel
.
Small brain tumors will also eventually completely disappear. However,
large tumors in the brain will sometimes only shrink to a point, then stop
highlighting and stop growing. At this point, some people have chosen to
have the benign mass surgically removed, while others have been able to
easily live a normal life with the benign mass still in their brain. Steves
experience is an important reminder that when an active tumor has become
benign, even though there is no discernable enhancement on an MRI,
there could still be some active cancer cells within the mass somewhere.
And these active cells could start growing again as soon as Protocel
is
stopped. Tus, it is probably best to stay on Protocel
indenitely as long
as there is any mass left in the brain at all.)
Case Story #IIChildhood Leukemia
Sydney is a wonderful seven-year-old girl. In I999, when she was only
two, she was diagnosed with acute lymphoblastic leukemia. Two-year-
old Sydney was given chemotherapy for about a year. At that point, her
doctors and family were hoping that she would be able to transition to
maintenance therapy, but a bone test in October 2000 showed that
she still had cancer in her bone marrow. Sydney had relapsed, and her
doctors wanted to perform a bone marrow transplant involving aggres-
sive chemotherapy at this point. Her family was told that even with the
bone marrow transplant, Sydney probably only had a I0 percent chance
of survival.
Before making a decision, Sydneys family sought a second opinion
from another prominent hospital. Te doctors at this hospital told them
that Sydney would probably only have a 5 percent chance of survival
after the transplant.
In January 200I, Sydneys family chose to decline the bone marrow
transplant which oered so little hope. Tey also declined any further
141 Protocel
Case Stories
chemotherapy or other conventional treatment. Instead, they started Syd-
ney on Protocel
, Cancell
, or Protocel
.
Like Roberta in case story #4, Kathy was another one of these people. In
late I99I, Kathy became sick. She was extremely tired and achy and had
lost 40 pounds. For a while, the doctors couldnt gure out what was
wrong. Finally, in March I992, they discovered that she was suering
from renal cell carcinoma in her right kidney. Later that month Kathy
went into surgery and her right kidney and surrounding lymph nodes
were removed. Te lymph nodes were clear, but the kidney tumor was big.
It measured 7 by I4 centimeters. Te surgeons actually had to remove
two of her ribs to get it out.
After surgery, Kathys doctors were going to discuss follow-up chemo-
therapy or radiation with her, but she didnt want to do either. She had
too many nurses in her family whod seen the horrors of these treatments,
and her own investigation indicated that there was no eective conven-
tional treatment for renal cell cancer anyway, other than surgical removal
of the kidney. And, with only one kidney left, this type of surgery was
no longer an option.
So, Kathy declined further treatment. But in June, she was worried
about her lungs and requested a chest X-ray. Te X-ray indicated that
something was there and the doctors then did a CT scan. Te scan showed
numerous nodules in both of Kathys lungs. To diagnose these nodules
142 oursxair \oui caxcii
more specically, Kathy underwent a two-hour needle biopsy procedure.
Te biopsy result came back as metastasized renal cell carcinoma, stage
IV. Te other result from the biopsy was that the procedure collapsed
one of her lungs, and Kathy had to recover in the hospital for ve days.
At this point, with metastasized renal cell cancer, Kathys doctors did
not recommend follow-up treatment. Tey did not say specically, but
their attitude suggested that there was no hope and they had nothing to
oer her. So she went home. She had already been looking into alterna-
tives and, fortunately for her, circumstances nally led her to Cancell
.
At the end of August I992, Kathy started taking Cancell
. She took
only one other supplement, which was Bromelain, along with it. Other
than the Cancell
, Kathy
got another scan of her lungs. Tis time, she only had two nodules left,
one in each lung. Tis was a great improvement since the doctors had
initially diagnosed her with numerous nodules. Ten in March, Kathy
went into surgery to have a swollen lymph gland in her collar bone area
removed. She was worried that it might be malignant, but the biopsy
showed there was no cancer in it. Tis was good news, but the really good
news was that the doctors did one more chest X-ray before the lymph
node surgery, and it revealed that the last two nodules in her lungs were
both gone. A few months later, in June I993, Kathy got a total body CT
scan, along with a variety of blood tests. All of the results came back the
sameno evidence of cancer anywhere!
Kathys metastasized renal cell cancer was completely gone after I0
months on Cancell
Case Stories
their stories and learn more about it from others. She continued this as
an annual tradition for many years before nally stopping it. According
to Kathy, I promised the good Lord I would do something to help more
people know about this.
Case Story #I3Stomach Cancer Metastasized to Lymph
and Bones
Another remarkable story of recovery from metastasized cancer belongs
to Robert. In May 2000, when Robert was 54, he and his wife were
vacationing in Las Vegas. One day, Robert suddenly fainted and then
began vomiting blood. He was rushed to the hospital, and after scoping
his stomach, the doctors told Robert he had stomach cancer, stage IV. Te
scope had revealed a 5.8 centimeter tumor. Also, the wall of his stomach
was about 3 inches thick around the tumor instead of the normal I-inch
thickness. Te doctors gave Robert 2 pints of blood to get him back home
so that he could be treated by his local doctors.
Once home, Roberts doctors performed a cauterization in his stom-
ach to stop the bleeding and administered antibiotics to him. More tests
revealed, however, that Roberts stomach cancer had already metastasized.
He was soon diagnosed with MALT lymphoma, which is a cancer of the
stomach lining, as well as non-Hodgkins lymphoma. (MALT stands for
mycosa-associated lymphoid tissue.) As if that were not enough, a bone
scan and bone marrow biopsy then showed he had cancer in his bones
as well, and another scan showed two spots on his liver.
Roberts doctors recommended a chemotherapy regimen called CHOP
along with radiation directed at the stomach tumor. (CHOP stands for
three chemo drugs and a steroid: cyclophosphamide, doxorubicin, vin-
cristine, and prednisone.) Tey told Robert and his wife that if he did
not undergo this type of treatment, he would probably live no more than
three months.
But Robert refused all chemotherapy and radiation and just took
Protocel
Formula 23 in distilled water. He also started taking an Ellagic Acid
supplement, enzymes, and aloe vera juice for detoxing and cleansing. After
a while, Robert started experiencing a lot of odd stu coming out of his
body in his bowel movements and also saw that his urine was often very
bubbly in the toilet bowl.
Exactly two months after starting Protocel
.)
Robert continued to take Protocel
each year,
which is about a two-month supply, as a maintenance program for the
rest of his life. Roberts recovery from metastasized cancer is an incred-
ible success story.
What did Roberts doctor think of his recovery? In late December
2000, when Robert was told that all his cancer was gone, his wife asked
his main doctor what he thought Roberts recovery could be attributed to.
Te doctor knew all along that Robert was taking Protocel
that
did it. Te doctors reply was that it was probably the strong antibiotics
that had been administered to Robert for his stomach ulcerations early
in the summer that brought about his remarkable cure.
Case Story #I4Cervical Cancer, Stage 3B
Janis was another person who underwent an amazing Protocel
recovery.
At only 48 years old, she was diagnosed in January 2002 with small-cell
cervical cancer, stage 3B. Prior to the diagnosis, she had been quite sick
for more than six months but had been misdiagnosed as having polymy-
algia rheumatica. Her doctor had placed her on a very heavy regimen of
prednisone at the amount of 80 milligrams a day for ve-and-one-half
months. By the time they realized she had cervical cancer, the tumor
was very large and had probably been stimulated to grow quickly by the
145 Protocel
Case Stories
high doses of prednisone which are capable of suppressing the immune
system.
In January 2002, Janis started bleeding profusely. She was rushed to
the hospital where she was given seven units of blood. She was told that
she nearly died, but as a result of this episode, she was nally diagnosed
correctly. Janis was told she had a large tumor on her cervix (about 8 cen-
timeters, or 4 inches across) that had attached to her pelvic wall. Because
her cancer was small-cell, surgery was out of the question. Janis was
told that if surgery were performed on small-cell cervical cancer, the
small cancer cells would escape into the bloodstream and quickly spread
to her spine and brain.
Te very day after her diagnosis, Janis was started on beam radiation
treatments. She continued to receive this type of radiation ve days out of
each week for three months. During that time, she was also treated with
two lots of radiation implants. Along with the radiation, on her second
week after diagnosis, Janis was started on chemotherapy as well. Te che-
motherapy continued throughout the entire three months of treatment.
By the end of the three months of aggressive radiation and chemo-
therapy, however, Janiss cancer had not responded to the treatment and
her tumor was even larger than before. Moreover, she was so sick at this
point she was throwing up every half hour and couldnt even keep a tiny
bit of water down. Her bowels had completely seized up and stopped
functioning due to the heavy amount of pain medication she had to take.
Her weight had plummeted from 240 to I40 pounds, and she was very
near death.
At this point, her doctors could no longer successfully rehydrate Janis,
and they concluded that one more treatment of chemotherapy would kill
her. Her doctor nally arranged for hospice care and told her husband that
if Janis were extremely lucky, she might live three months. But realistically,
he said, she probably would live only two to four more weeks.
Te very day Janis was started on hospice, in April 2002, her hus-
band Ralph began searching the Internet for another solution. He
found a doctor of naturopathy who knew about and had recommended
Protocel
she
threw up for the very last time. After seven and a half weeks on Protocel
,
she was nally out of pain and able to stop all her pain medication. Tis
allowed her bowels to start working again. Also, at this point, she went
back to her doctor for a checkup on her cancer. Her doctor was amazed
to see Janis walk into the oce. Moreover, examination showed that the
tumor had already reduced half in size!
When Janis went back about four months later, her tumor was mea-
sured at only 2 centimeters, which was less than one-quarter its original
size, and she was back to living normally. After being on hospice with only
two to four weeks to live, Janis had gotten her life back! She continued
to feel better and better, and began spending much of her time helping
others to recover from cancer using Protocel
.
Unfortunately, Janis felt so well that she stopped using Protocel
too
soon. (As noted in case story #I0, it is imperative that people do not stop
taking Protocel
after
diagnostic tests come back all clear.)
Sadly, a number of months after stopping Protocel
, Janis suered a
recurrence of her cancer in her liver. By the time it was noticed, it was too
late for Protocel
longer before
stopping it, she would not have experienced the metastases to the liver
and would be alive today.
Case Story #I5Childhood Brain Cancer
Nicki is an eight-year-old girl, currently living a completely normal life.
But just over three years ago, soon after she turned four in June 2000,
Nicki developed a fever and had a grand mal seizure. She was rushed to
a hospital emergency room where a CT scan was taken, then transferred
to the hospital, where doctors surgically inserted a shunt to treat the
hydrocephalus condition that had developed. After that, a biopsy was
performed on Nicki which showed she had a slow-growing tumor in her
brain. Te biopsy diagnosis came back low-grade astrocytoma, grade
I to 2, and was located in the basal ganglia and thalamus regions. Te
147 Protocel
Case Stories
doctors concluded that the tumor had grown to the point where it was
pressing on a ventricle in Nickis brain, and this is what caused the seizure
and the hydrocephalus.
Because Nickis tumor was octopus-like and had tentacles inltrating
the rest of her brain, it was considered non-operable. She was also consid-
ered too young to undergo radiation. So, after recovering in the hospital
for a few weeks, Nicki was started on chemotherapy. Nickis mom, Vicki,
was led to believe by the doctors that they would be giving Nicki some
new type of chemo that had been achieving great results. Te doctors
also said that Nicki had a strong likelihood of living ve years, which
they considered to be a very good prognosis. (Tis, on the other hand,
did not sound so good to Nickis mom.) Te chemotherapy regimen that
was prescribed was procarbazine, vincristine, and CCNU.
According to Vicki, administering the chemotherapy to her daughter
was a terrible ordeal. Te chemo was in capsule form, but the pills were
large and very dicult for Nicki to swallow. Tey had to hold her down
and force the pills into her. Forcing these pills down at times caused
little Nicki to cough up blood. Vicki hated to do it, but she wanted her
daughter to live, so they continued with these pills for about I0 months.
Finally, one doctor told Vicki she could open up the capsules and mix
the contents into some sweet food for her daughter to eat, but this ended
up a disaster. Nicki got red all over and covered with hives. Paramedics
had to be called, and they gave her an injection of Benadryl.
After I0 months of chemo, Nickis tumor was still unaected. It had
not decreased in size, although it had not increased either. After Nickis
bad reaction to the opened-up pill, the doctors decided to switch her to
a dierent chemotherapy regimen. Tis time, they put her on vincristine
and carboplaten. Tis second protocol was so devastating to Nicki that her
mother had them stop it after only three treatments. Nickis blood counts
had dropped severely, she needed a blood transfusion, and her mom felt
deep down that the new chemo regimen was killing her little girl.
Vicki just couldnt put her daughter through any more chemotherapy.
None of the treatments had caused a reduction in the size of the tumor.
Te very night Vicki said enough, and took Nicki home from the hos-
pital, she read about Protocel
.
She was fortunate to not suer any serious neurological damage or notice-
able cognitive impairment from either the cancer or the chemotherapy.
Whether or not Nicki sustained minor neurological damage is still pending,
but she does not appear to have any signicant problems. Now, in 2004,
Nicki goes to school, plays, and does everything else eight-year-olds do.
She experienced little in terms of visible lysing signs during her recovery.
Since her MRI in June of 2003, her brain tumor has remained stable in
size and it is most likely that the tumor is now completely benign. Nicki
has just started second grade and is able to perform on the same level as the
other children and shows no symptoms whatsoever of having cancer!
Nickis mother, Vicki, claims that what the doctors told her when they
rst prescribed the chemotherapy, was not true. Tey told her that the
chemo they wanted to put Nicki on was new and had been achieving
very good results. Vickis subsequent research, however, showed that the
chemo they prescribed had actually been around for about 30 years and
was not achieving great results according to everything she read. Looking
back on it now, Vicki can see how much she needed to trust the doctors in
the beginning. She says she understands people who hear about Protocel
but dont choose to use it. Vicki says, If I had been told about Protocel
when Nicki was rst diagnosed, I wouldnt have believed it could work
either. I know I wouldnt have put her on it then. I would have still gone
along with whatever the doctors said we should do. Now, she just feels
grateful that she came across Protocel
Case Stories
completely disappear. However, large tumors in the brain may sometimes
only shrink to a point, then stop highlighting and stop growing. Tey may
be seen as having gone dormant so-to-speak at this point. If this happens,
it might be best to continue taking Protocel
could be
stopped after using it for 6 months to a year after the surgical all-clear
point to make sure every last cancer cell has lysed.)
Te above case stories show how powerful this easy-to-use and inex-
pensive liquid formula can be for treating cancer in the elderly, middle-
aged, young adults, and even small children. To read about and listen
to more Protocel
alone, I
highly recommend Pamela Hoeppners book, Te Breast Stays Put: No
ChemoNo RadiationNo LumpectomyNo Tank You. In this very
personal account, Hoeppner does an excellent job of presenting how to use
Protocel
eectively for cancer. She also details with great humor and
words of wisdom what it is like to deal with doctors, family and friends
while bravely choosing to use an alternative approach for a life-threatening
disease. For information on how to order Te Breast Stays Put, see the
ad at the back of this book or go to www.TeBreastStaysPut.com. Tere,
you will also nd additional recovery testimonials from others who chose
to use Protocel
/Cancell
formula never
got approved by the FDA. And if a medical treatment is not approved
by the FDA and endorsed by the leading cancer organizations, doctors
generally wont hear about it. If a doctor does hear about it, he or she will
not have any accepted source to go to for more information about the
treatment and would not be legally allowed to prescribe it even if he or
she wanted to.
How did Jim Sheridans formula get suppressed? As is commonly the
case, it happened over a number of years and as a result of a variety of
events. It was not, however, a result of Sheridans not going through the
right channels, or not working with the right organizations. In fact, Jim
Sheridan worked from I935 to I937 in the analytical lab at Dow Chemi-
cal Company in Michigan, from I950 to I953 at the Detroit Institute
of Cancer Research (now called the Michigan Cancer Foundation),
152 oursxair \oui caxcii
and from I96I to I963 at the Battelle Institute in Columbus Ohio (an
organization that commonly tested new chemo agents for the National
Cancer Institute.)
One of the early suppressive events occurred when Jim Sheridan was
working at the Detroit Institute of Cancer Research. At that time, the
Pardee Foundation was the source of funding for the research Sheridan
was doing. Also at that time, Sheridans formula was resulting in an 80
percent cure rate in laboratory mice with cancer. According to jour nal
writer Marcello Gallupi, who researched and wrote articles on the Entelev
/
Cancell
,
and within a few months, Jim Sheridan was suspiciously red from the
Detroit Institute of Cancer Research. Sheridan later heard that all the
results of his research at the Institute had been burned!
Te next event to block Sheridans formula from being ocially ana-
lyzed (and thereby kept out of mainstream medicine) occurred in I963.
He had been working for two years in the Biosciences Division of the
Battelle Institute in Columbus, Ohio. At that time, Battelle Institute was
a research center where many promising chemotherapeutic agents were
being tested for the National Cancer Institute. Sheridans formula was
also being tested there. After I0 months of assessing the formula, which
was having very good results with cancer, Dr. Davidson of the Battelle
Institute requested permission from the NCI to test Entelev
in an NCI
laboratory. But Dr. Davidson asked if the test could be executed over
153 Protocel
had
been put on clinical hold because of lack of data assessing its toxicity.
Te FDA then informed Jim that he needed to have an LD-50 test
performed on his formula. Te LD-50 is a toxicity test using animals
that is done in various FDA-approved laboratories around the country
to establish the safety level of a product.
Sheridan had already had several minimum lethal dose (MLD) tests
using animals done on his formula before the FDA granted him this IND
number. MLD testing is where a technician injects a group of mice with
the material being tested in bigger and bigger doses. At the point where
50 percent of the mice die from the material, the minimum lethal dose
amount is established. Te reason Sheridan had done several of these tests
155 Protocel
. Unfortunately,
however, this doctor was from another country and before he could do
the research, he found himself being threatened with deportation.
Another way that Sheridan tried to get his formula into mainstream
medicine was by attempting to get pharmaceutical companies interested
in it. Each time a pharmaceutical company looked into it, they would
be very interested at rst. But as soon as they found out that the formula
was not something they could patent and thereby make exorbitant prots
from, the pharmaceutical companies always completely lost interest.
In the early I980s, another development occurred. However, this time
it was a very fortunate one. A metallurgist and engineer named Ed Sopcak
156 oursxair \oui caxcii
got involved with Sheridans formula. Sopcak was already in business for
himself and decided to take on the task of producing Entelev
in large
quantities so that it could be available at no cost to cancer patients. Sopcak
believed that Entelev
.
From about I984 to I992, Ed Sopcak gave away about 20,000 bottles
of Cancell
to
treat their cancer. According to Sopcak, four local TV stations had been
invited to lm the event and air it on the news. But, unfortunately, none
of the TV crews showed up. One station claimed it was too short-staed,
and the three others that had been invited claimed that the FDA had
threatened to have their licenses revoked if they covered the event. Tus,
the media coverage was controlled and eectively blocked by the FDA.
(Whatever happened to freedom of the press and fearless journalism?)
Finally, on November I3, I990, the National Cancer Institute agreed to
test the formula once again, this time in vitro, which meant they would
administer it to various cancer cell lines in petri dishes. Even though this
was just a 48-hour test not using animals, it is still a valid test often used
for early evaluation of a new treatment. Te Cancell
formula proved to
be highly eective against all the strains of cancer that the NCI tested it
on. Jim Sheridan now felt renewed hope that it would nally be approved.
But he was shocked when he received a letter from the NCI stating that
they were not planning to pursue his formula as a medical treatment.
At this point Jim Sheridans son, James, was amazed and decided to
get involved. James Sheridan is currently, and was also at that time, a
district court judge for the State of Michigan. Judge Sheridan called the
NCI directly for an explanation and spoke to Dr. Ven Narayanan, who
was the head of drug testing for the NCI at that time. When asked why
157 Protocel
on
eight dierent types of cancer. Te ninth graph shows a superposition of
all the eight previous graphs. Te original data was requested by Dr. John
Zimmerman, director of the Bio-Electro-Magnetics Institute of Reno
Nevada, through the Freedom of Information Act. Te National Cancer
Institute supplied Dr. Zimmerman with the test results for these graphs
and the NCI cover letter along with the original NCI data can be found
in the BEMI Currents Journal, Volume 3: Number 4 of March I993. An
article written by Jim Sheridan and edited by Dr. Zimmerman, which
explains the 9 graphs, is also printed in that same issue.
A brief explanation of these graphs is warranted here. Te vertical
axis on the left of each graph represents the percentage of growth in the
cancer cells tested. On this left axis, 0 means no growth, 30 means 30
percent growth, 30 means 30 percent death of cells, and I00 means
that virtually all the cancer cells in the petri dish are dead at this point.
158 oursxair \oui caxcii
Te horizontal axis on the bottom of each graph represents the dos-
age of Cancell
used in
micrograms per milliliter (g/ml), and in a Log scale. Tis means that
the I, 2, 3, and 4 on the bottom horizontal line are powers of I0.
(Tus, I actually means I0 g/ml, 2 means I00 g/ml, 3 means I,000
g/ml, and 4 means I0,000 g/ml.)
Te dierent types of solid, dotted and dashed lines on each graph
represent dierent specic cell lines for each type of cancer tested. Tese
cell lines are dened underneath each graph.
To anyone looking at these graphs, two main characteristics jump out.
Te rst characteristic is that, except for the leukemia cell lines, all other
types of cancer tested (non-small cell lung cancer, small cell lung cancer,
colon cancer, central nervous system cancer, melanoma, ovarian cancer,
and renal cancer) proved to respond with either I00 percent cell death,
or very near to I00 percent cell death within a certain dose range over
a very short period of time. In the case of a devastating disease such as
cancer, a substance that can simply bring cancer growth to zero is quite
an accomplishment. One that can cause almost I00 percent cell death
in a 48-hour period is a remarkably good result and denitely worth
looking into!
Te second characteristic that jumps out is that the optimum dose
range on all the graphs was approximately between I00 and I,000 g/ml.
After that, as the dose amount is increased by factors of ten, the amount of
cell death decreases. Tis means that at much higher doses, the Cancell
formula was actually less eective at causing cancer cell death. What is
evident from this characteristic is that Cancell
,
being non-toxic, could be taken indenitely without harming the body.
At the time of this testing, people who had used Cancell
to fully recover
from their cancer had used it for much longer periods than 48 hours.
Te benets to using a non-toxic treatment approach for cancer cannot
be overstated. Besides the fact that toxic treatments can have extremely
serious side eects (such as liver, kidney, and heart damage) to the point
that the side eects themselves can be life-threatening, there is also
another issue. Tis is the issue that toxic conventional approaches such
as chemotherapy and radiation do not allow for continual use. Tey are
so toxic that continual use would kill the patient before the cancer could.
So, toxic treatments are always administered with treatments spaced out
in some way. But cancers best attribute is its ability to grow new cells
164 oursxair \oui caxcii
fast. Tis means that, in-between the toxic treatments, the cancer cells
grow back. And those cells that grow back the fastest are those cells that
have some amount of resistance to the treatment.
In other words, when a cancer patient needs a few days or weeks for
their body to recover from the toxic cancer treatment being given them,
the cancer cells may also recover during this time. Tey may even start
to grow faster than before due to the bodys immune system having also
been weakened by the toxic treatment. Eventually, a persons body may
not be able to recover anymore because it has been too weakened by the
treatment.
With non-toxic treatments, however, this vicious cycle is avoided. For
instance, Protocel
was that, as
a cancer treatment in the initial stages of testing, it passed with ying
colors. Te only logical conclusions as to why it was never pursued further
would have to be that either: (I) the institutionalized procedural bias was
too strong, or (2) the NCI just didnt want to pursue it even though they
could see that it worked.
Te nal blow to Cancell
ocially
evaluated and accepted, his successful non-toxic formula for treating
cancer was eectively kept from widespread availability to the public
through a variety of ocial actions over a span of many years. As with
other successful non-toxic alternative cancer treatments, his formula
165 Protocel
, the
exact version of Jim Sheridans formula was not available for about seven
years (between I992 and I999). But in April I999, the Sheridan family
was able to get the formula produced once againthis time for sale to the
public. It was re-named Protocel
, and Protocel
.
As to the ocial toxicity test, another LD-50 test was requested and
run on the formula before Protocel
taken
four or ve times a day is less toxic to the body than taking one aspirin
a day. Te non-toxic aspect of Protocel
,
Cancell
, or Protocel
is a unique prod-
uct that was developed specically for treating cancer and that it
has brought about countless cancer recoveries over the past two decades.
However, the National Cancer Institute and FDA were not interested
in pursuing it as a cancer treatment. So, the only way this remarkable
approach could be made available to the public was to sell it as a dietary
supplement. As in other similar cases, this created the unfortunate conun-
drum that any company selling Protocel
, when
the updated second edition was produced this chapter was signicantly
expanded to include even more information.
Since this chapter is very detailed and only about how to use
Protocel
s
action.
4. Be sure to drink plenty of good water each day, besides other liquids.
(Preferably, at least a half gallon of water a day.)
5. Try to promote at least one bowel movement every day to support your
bodys ability to process out lysed material. (Use extra ber or a mild
laxative if needed.)
But, even though using Protocel
bottle
before measuring out each dose. Tis is because a small amount of sed-
iment-like substance settles at the bottom and you want that substance
to be as evenly mixed into the formula as possible.
Once the Protocel
instead of water. (Just enough to cover the taste and gulp it down quickly.
Protocel
should not be allowed to sit in juice for any length of time). Or,
a person can add just enough water to their dose to gulp it all down at
once and then follow that with a glass of pure water to wash it down.
Te following instructions apply to basic starting doses. For certain situ-
ations, or after being on Protocel
) is gener-
ally taken four times around the clock with each dose being a quarter
teaspoonful. Tese doses should be spaced out as equally as possible over
each 24-hour period. For one person, taking their doses at 6 a.x., I2
noon, 6:00 i.x., and midnight might be convenient. For another, taking
their doses at 8 a.x., 2 i.x., 8 i.x. and 2 a.x. might be easiest. It doesnt
matter what time of day you take your doses so much as it matters that
you space them out as equally as possible around the clock.
For optimum results, it is best not to let more than six hours lapse
between any two doses. Te goal with Protocel
) on the other
hand, is generally taken ve times around the clock for cancer with each
dose being teaspoonful. Tese doses should also be spaced out as equally
as possible over each 24-hour period. Again, never going more than six
170 oursxair \oui caxcii
hours between any two doses is going to facilitate the fastest recovery.
Tus, a sample schedule for Formula 23 for cancer might be 7 a.x., II:30
a.x., 4:00 i.x., 8:30 i.x., and 2 a.x.
With either the Formula 50 or the Formula 23, some people like to
double their bedtime or middle-of-the-night dose to give their cancer an
extra punch, and thats okay. But if cancer breakdown starts happening
too fast, all the doses can be kept at the same amount. Doubling the dose
at bedtime was originally recommended to people who could not get back
to sleep if they took a dose in the middle of the night, and it was thought
that a double dose before bed would help the Protocel
formula.
Some people nd it dicult to accurately measure their dose with the
medicine dropper that comes with the formula. If this applies to you, one
tip is to go to a drug store and look at the baby supplies section. Usu-
ally, you can nd a plastic baby medicine syringe that sucks up medicine
and has markers for and teaspoonful, etc. Tis works quite well for
Protocel
dosing and may help in keeping your dose size accurate and
consistent, whether you are sticking to the recommended teaspoonful
or are increasing your dose to teaspoonful or more. (See later section
called "Variations on Dosing.") Some people nd that simply using a
measuring spoon works best for them, which is also ne. Te important
thing is to pay attention to detail and maintain a consistent accurate
dosing without missing doses for as many months as are needed to get
rid of your cancer.
Dont Give Your Cancer Cells a Bowl of Soup!
Ed Sopcak, who had the best track record of recoveries from cancer
patients he helped to use Cancell
may remain to some extent in the body for more than 8 hours,
171 Protocel
works by signi-
cantly interfering with the ATP production of anaerobic cells. Te small
eect Protocel
in
regular, evenly spaced out doses, without missing doses, a person can
systematically starve their cancer cells to death.
However, beyond six hours after any dose, the level of Protocel
remain-
ing in your body may not be able to perform its job I00 percent. With
the goal being to starve your cancer cells to death, going more than six
hours between any two doses is like giving your cancer cells a little bowl
of soup, so-to-speak, on the seventh or eighth or ninth hour between doses.
Your cancer cells are not going to starve to death if you keep feeding them
every night (or any other time you go more than 6 hours between doses).
Tus, for optimum results, never go more than 6 hours between doses so
that you dont give your cancer cells a bowl of soup!
For adults and children, Protocel
in juice for any length of time is not recommended. If a person wishes
to carry one or two premixed doses of Protocel
be mixed
into distilled water only. As long as distilled water is used, these premixed
doses can then be carried in ones pocket, purse, or glove compartment
and kept for hours at a time. Alternatively, a small plastic bottle of pure
Protocel
has a shelf life of many years. It does not spoil after the bottle
has been opened, therefore it requires no refrigeration. Te best way to
store it is simply on a shelf or counter where it is not in direct sunlight.
Pre-prepared doses can be carried around during the day for hours in
small containers if that helps a person stick to their schedule, or set out in
a small closed container overnightbut only if mixed in distilled water.
Protocel
bottle vigorously each time, then quickly measure out your dose.
If you do not shake the bottle vigorously right before each dose, then by
the time you are into the latter half of the bottle, there will be a higher
ratio of sediment to liquid than there was in the rst half of the bottle.
Jim Sheridan and Ed Sopcak used to always tell people to shake the bottle
vigorously to get an even amount of liquid to sediment, and virtually all
the people who have used this formula successfully have done so.
Protocel
experts have agreed that this is not the best way to look at it. What appears
to be more accurate is that either formulation will usually work for any
anaerobic condition or type of cancer, however the Formula 50 seems to
work a little better for some types of cancer and the Formula 23 seems
to work a little better for others. Any possibility that the Formula 50 is
stronger in some cases is made up for by the fact that people generally
173 Protocel
Formula 50.)
Anecdotal Guide for Which Formulation to Start With
Formula 50 Formula 23
Adenocarcinoma Bladder cancer
Cervical cancer Brain cancers (other than GBM)*
Colon cancer Breast cancer
Esophageal cancer Kidney cancer (renal cell)
Glioblastoma Leukemiaacute
Leukemiachronic Multiple Myeloma
Liver cancer (primary) Neuroblastoma
Lung cancer Prostate cancer
Lupus Wilmes tumor
Melanoma Viral infections***
Non-Hodgkins lymphoma Auto-immune disorders
Ovarian cancer Crohns disease
Pancreatic cancer Endometriosis
Sarcomas IBS or UC
Stomach cancer Multiple Sclerosis**
Squamous cell cancer Parkinsons
Troat cancer Pets with any condition****
Uterine cancer Psoriasis
Viral infections***
Mononucleosis
* For people with primary brain cancer, Formula 23 has been the preferred ver-
sion except for use against glioblastomas. Te 23 has had an excellent track record
174 oursxair \oui caxcii
with all types of astrocytomas and oligodendroglioma. However, if one is dealing
with Glioblastoma Multiforme, they may want to use Formula 50, which appears to
have had the best track record with that particular type of brain cancer. For all other
types of cancer in the brain that are NOT primary (in other words it is metastasized
cancer from some other part of the body), then users should pick the formulation that
applies to the primary site. In other words, for a person with lung cancer mets to the
brain, the Formula 50 is indicated for lung cancer and should be used. If they have
breast cancer mets to the brain, then Formula 23 is indicated for breast cancer and
should be used. Whenever dealing with cancer in the brain of any type, one needs
to be cautious of not promoting too much edema too quickly, and the prescribed
use of steroids or anti-seizure medications may be necessary until Protocel
has had
time to reduce enough of the cancer load so that pressure in the brain is not an issue.
Steroids and seizure meds will not interfere with Protocel
s action.
** Many people with multiple sclerosis have experienced wonderful improvements in
their condition through the use of Protocel
for MS may also want to supplement daily with: I,000 mg borage oil, 3 tablespoons
granular lecithin, and 2 tablespoons extra virgin cold pressed olive oil. Tese extra
supplements are thought to help the body rebuild new myelin sheath. Another way
it is thought that Protocel
and should
probably be avoided when using this formula.
*** Many people with various viral conditions have also experienced remarkable
recoveries, and both the Formula 23 and the Formula 50 have been successfully used
against viruses. Te reason that Protocel
correctly in general.
Keeping to your daily schedule and not missing doses unless absolutely
necessary is critical. Watching your progress and increasing the dosage
over time if needed can also be very important.
Only take Formula 23 or Formula 50 at any given time. In peoples
eorts to ne-tune their own lysing process and recovery, they may end
up with part of a bottle of Formula 23 and part of a bottle of Formula
50. If this happens, do not mix the two formulations together. Formula
50 and Formula 23 should always be kept in separate bottles, and people
should only use one or the other for any given period of time.
Avoid Taking Any Supplement or Treatment Tat Might
Interfere With Protocel
. But, when
using the Protocel
,
drinking water that has been disinfected with a small amount of ozone is
ne. Tis is because, when ozone is used on municipal or bottled water
for disinfectant purposes, the ozone has virtually always dissipated com-
pletely or converted back to O by the time you drink it.
Cesium. Many people who read how powerful both Cesium High pH
Terapy and Protocel
.
7I4X. Te compatibility of 7I4X and Protocel
are unknown, so it
would be best to avoid doing the two together.
Antineoplaston Terapy. Te compatibility of Antineoplaston Terapy
and Protocel
is unclear,
however according to anecdotal cases, it appears that people don't seem
to respond as well to Protocel
or
not, but there is some suspicion that it might. Terefore it would be best
to avoid. Te suspicion is based on the fact that Dr. Johanna Budwig,
developer of the axseed oil and cottage cheese approach, stated that her
method of treatment helped to "normalize" cancer cells. Since Protocel
is
trying to make cancer cells more "primitive" (which goes in the opposite
direction), the two approaches may counteract each other.
Most Chemotherapy Drugs. Jim Sheridan stated that chemotherapy
may interfere with this formula by changing the level on the oxidation-
reduction ladder at which Protocel
?")
MAY Be Taken While Using Protocel
, or took no more
than two or three of the supplements on the May Be Taken list along
with their Protocel
.
Keep in mind that many alternative non-toxic approaches to cancer fol-
low the philosophy that one must ood the body with nutrients, detoxify
the body, and follow a very strict diet. Tat is because those approaches
tend to rely primarily on making the body as strong as possible so that
ones own immune system can get rid of the cancer. Protocel
follows a
dierent philosophy. Protocel
s abil-
ity to starve the cancer cells.
Another thing to remember is that when Ed Sopcak was giving out
Cancell
and possibly some Bromelain (an enzyme) along with it. Tat was
it! Tey didnt alkalize, they didnt juice, they didnt drink green drinks,
they just ate what was considered to be a normal healthy diet.
Tose people who do want to use other supplements while taking
Protocel
can consult the previous list for items that are believed to be
compatible. However, restricting ones use of these supplements to as few
as possible is still advisable.
180 oursxair \oui caxcii
When in Doubt, Do Without
Since it is so important not to interfere with the way the formula
works, it is best to avoid any supplement, herb or treatment while using
Protocel
unless you know from the literature sent with the product, or
from anecdotal reports, that the item you wish to take will not interfere
with what Protocel
but many
DIM supplements have vitamin E added. You may do best nding a DIM
supplement to use that is a brand with no vitamin E added. Another type
of situation is the following: A woman might wish to use Haelen, which
is a powerful cancer-ghting beverage made from fermented soy beans
known to help ght breast cancer. Because soy isoavones are listed as
compatible with Protocel
.
Prescription Medications and Hormone-Blocking Drugs
Many people have successfully used Protocel
.
Tamoxifen is a hormone-blocking drug given mainly to women with breast
cancer and it changes the metabolism of the cancer cells to some extent.
(Refer to Chapter I9 to read about how Tamoxifen is a "cytostatic" drug
that blocks estrogen and puts cancer cells into a sort of sleep state.) Tis
alteration of the cancer cell metabolism may interfere with how Protocel
was designed to work on the cell respiration of cancer cells. Unfortunately,
some women who have used Protocel
, testosterone-
blocking drugs make a man more estrogen-dominant and estrogen fuels
prostate cancer growth. Tus, taking a testosterone-blocking drug may
make it harder for Protocel
to ght your cancer, you may want to consider discontinuing it.
Whenever possible, take prescription medications separate from your
Protocel
can often
improve other health conditions a person may have, such as high blood
pressure, arthritis, chronic fatigue, some forms of diabetes, Crohns dis-
ease, multiple sclerosis, viral infections, endometriosis, hemorrhoids, and
psoriasis. So it sometimes happens that while a person is using Protocel
182 oursxair \oui caxcii
for cancer, he or she may see an improvement in these conditions and
require less prescription medication over time. It is important, therefore,
for people to be aware of this and carefully monitor the dosage of any pre-
scription medications they are takingespecially in cases where a person
is taking blood pressure medication or insulin. People who require insulin
should monitor their blood-sugar levels more than once a day while on
Protocel
. Te
simple most common recommendations are to:
I. Eat a normal, well-balanced diet. It is generally recommended that
people taking Protocel
are referred to as
lysing symptoms. In other words, a perfectly healthy person could take
Protocel
everyday and not experience any symptoms at all, because they
wont be having a lot of lysing occurring. Protocel
is a mucousy excretion of egg white-like material that may be noticed
draining out of the nose, being coughed up from the lungs, or coming
out in the feces. Tis is because, as the cancer cells lyse, they break down
into their basic protein parts and the body has to process this dead cancer
cell debris, or protein material, out through any orice it can. A runny
nose is quite common, and as long as the mucous is not a greenish color
and there is reason to believe it is not from a cold or allergies, it is usually
an indication of lysing. For anyone using Protocel
for a while. Tis is lysed material and a good sign that the
Protocel
is
draining energy from ones normal cells. It just means that the body is
working hard to process out the lysed material (or broken down cancer.)
Tus, extra tiredness is simply a detoxing symptom. If a person has very
little cancer in their body to begin with, such as right after having a tumor
removed surgically, then they will most likely not experience any tiredness
185 Protocel
wont
work on slow-growing malignant cancers, it just means that those people
with a slow-growing cancer may need to be more patient.
For people using Protocel
. Tis
may involve dizziness, foggy thinking, or motor problems if those were
the initial symptoms when diagnosed. Te reason for this is that when
a tumor or tumors are starting to lyse in the brain, the resulting eect
may be a mild edema. Most people will get through this period just ne
if they know what to expect. If any of the lysing symptoms get to be too
much, adults can reduce their Protocel
need to be on a prescription steroid for edema or a prescription anti-seizure
medication. Tese types of meds are often necessary to control pressure
and uid build-up in the brain long enough to allow Protocel
to work.
Over time, these meds can be reduced gradually under the supervision
of a doctor as the cancer goes away.
What if You Start Getting Headaches While Using Protocel
?
Daily headaches are not a normal lysing symptom except when there
is cancer in the brain. If a person starts getting regular headaches while
taking Protocel
time to work.
Unfortunately, some people are unaware that their cancer has already
gone to their brain when they start taking Protocel
operates
in a fundamentally dierent way than doctors are used to. Tis means
that lysing symptoms, such as temporarily elevated cancer markers, will
not necessarily be understood correctly by oncologists or other doctors.
Some people may choose to not get cancer marker blood tests at all in
the rst six months or so in order to not have to deal with doctors being
alarmed. Others just explain to their doctor that the alternative approach
they are using causes marker levels to rise as the cancer breaks down and
that other types of diagnostic tests may be best to use for a while.
Assessing Your Progress and Using Scans
Some people using Protocel
,
even though they are breaking down. Tis is because tumors may sort of
liquefy and spread a little as the cancer cells lyse (like an ice cube melting
and forming a puddle). And very large tumors may take so much time
decreasing in density that they don't actually show reduction in size until
the fourth month or so. However, smaller tumors do often show a decrease
in size on scans within the rst few months, sometimes even as quickly
as after just a few weeks on Protocel
. Before
starting Protocel
wasn't working
and would probably have stopped taking it.
191 Protocel
to work
on them. Tis has not yet been proven and some people seem to experi-
ence some eect on benign tumors. But there have also been cases where
Protocel
can be tried, but if it doesnt work the person may want to switch
to another approach that has had success with benign tumors.
Will Protocel
on topically wher-
ever lesions are accessible on the surface, but this should only be done in
addition to taking Protocel
formulations. And,
for many people, that is the exact dosing that they stay on throughout
their entire cancer recovery. However, sometimes varying the dosing can
be a good idea and may even in a few cases make the dierence between
full recovery or not.
Higher Doses. To give themselves the best possible chance, some
people may wish to start out at teaspoonful each dose instead of for
either formulation. Tis may not sound like a big dierence, but with
Protocel
50) at his own expense and gave away more than twenty-thousand bot-
tles of it to cancer patients. He always told people to spread their doses
194 oursxair \oui caxcii
out evenly around the 24-hour clock and never go more than 6 hours
between any two doses.
Ed Sopcak had the best track record of cancer recovery for those
people he helped to use this formula. Years later, some people found that
a lot of people could still get well if they doubled their bedtime dose
and took their next dose in the morning 8 hours later. Tis certainly has
worked in many cases, particularly for those cancers that are either slow-
growing or have been caught very early. (Such as prostate cancer caught
early.) However, this author believes that taking a dose in the middle of
the night and never going more than 6 hours between any two doses is
still the most optimum way to use Protocel
Take?
It is impossible to give a time-scale for recovery that would apply
to every cancer patient. Keep in mind that Protocel
formula stopping
the progression of the cancer and stabilizing tumor growth. Tis, in itself,
is a wonderful thing. It generally takes longer than two months for most
people to experience a noticeable reduction in the size of their tumors, but
some cases do see tumors go down within the rst couple of months.
It helps to keep in mind that the speed at which Protocel
can totally
rid someone of their cancer is still remarkably fast when compared to con-
ventional treatments like chemotherapy and radiation. Tese conventional
treatments may cause fast tumor regression, but because they so often do
not completely get rid of the cancer, tumors will many times grow back
and must be treated a second or even a third time over a several-year period.
Te initial reduction of tumors under these circumstances (called remis-
sion) may be fast at rst, but short-livedand rarely results in a fully
cancer-free state. Whereas, with Protocel
?
Tis is a very important question. Radiation will not interfere with the
action of Protocel
alone.
If this is not the case, however, then it might be best to either decline
the radiation or at least make sure that the radiation treatments are con-
sidered low-dose or short-term. People doing Protocel
and radiation at
the same time generally do not need to complete the full course of radia-
tion that would normally be prescribed for the same situation without
Protocel
and
should be avoided in most cases to give Protocel
.
Te only exception to this rule is when the chemotherapy agent is an
anti-metabolite type of chemo drug. Te anti-metabolite chemo agents
push the energy level of cells down and therefore tend to work well with
Protocel
. Tey are:
I. 5FU (Fluorouracil)
2. Xeloda (Capecitabine)
But people also need to be well informed whenever they make a choice
to use chemo. Even anti-metabolite chemotherapies can damage nor-
mal, healthy cells. Any chemo is toxic and can potentially cause serious
side eects and possible long-term damage to the heart, liver, kidneys,
brain, and nervous system. Tus, the risks versus the benets must be
weighed.
When it comes to any other type of chemotherapy besides the two listed
above, one should consider that there is a risk that the chemo will make
197 Protocel
can
if it isn't interfered with. Tus, in most cases, people should seriously
consider declining the use of chemo if they are using Protocel
.
Too many people hear of someone that did ne while using chemo-
therapy and Protocel
s action.
One eye-opening case I personally followed was of a woman with
metastasized ovarian cancer who had been on chemo for a long time.
While she was in-between chemo treatments, she started using Protocel
and began experiencing signs of lysing and saw positive changes in a
lymph node tumor on her neck. She also began feeling better. But her
oncologist soon convinced her to go back on the chemo and she didnt
feel she could say no to her doctor. Tough she stayed on Protocel
, all
her signs of lysing stopped as soon as she resumed the chemo and she
had no more indications that the Protocel
does
not get rid of people's active cancer by being a powerful anti-oxidant. Te
anti-oxidant capacity of Protocel
as soon
as their scans or other tests show no more signs of cancer, there may still
be a signicant number of cancer cells in their body that are still alive
and ready to begin proliferating again. Tere have been some people who
stopped using Protocel
after their
cancer is no longer detectable is up to each person. Since Protocel
is not
toxic to the body like chemotherapy or radiation, people can continue
taking it indenitely if they choose to. At least one woman has taken it
for over I5 years with the only eects being that she feels great and never
seems to come down with a cold or u (since Protocel
to treat
their cancer is stopping too soon. Another mistake people often make is
reducing their dosing after the all-clear point. One woman used Protocel
23 to get her bladder cancer to completely disappear from all scans and to
199 Protocel
.
Some people do choose to use Protocel
, and it is
exciting that some veterinarians have even started using or recommend-
ing the formula for their canine and feline cancer patients. It also works
remarkably well for any viral condition, so giving your dog or cat Protocel
for either cancer or a viral disease is well worth trying. Most animals appear
to respond faster than humans and, though dosing 4 times a day is still
often optimal, 3 times a day usually works for pets. (For some exciting
dog recovery testimonials, visit the home page of www.OutsmartYour
Cancer.com.)
Although there is a lack of information about using Protocel
for birds
or reptiles, excellent reports have come in about giving Protocel
to a
dog, cat, or horse. Most likely any other mammal, such as a ferret, goat,
or pot-bellied pig, would also respond quite well. Usually, pet owners
will mix the formula into any type of pet food or other treat the animal
likes. One colorful story comes from a family that treated their female
dog Dink for cancer by putting a few drops of Protocel
onto a piece
of bread and throwing the bread up into the air. Dink would then hap-
pily leap up, grab the bread in her mouth, and gulp her cancer treatment
down. Other pet owners choose to mix the Protocel
every 8
hours (three times a day).
A great horse story was related by one woman who treated her 20-year-
old horse named Ladd for melanoma with Protocel
on her horse.
Every morning and evening, she would core an apple, put I teaspoonful
of Protocel
into the inner part of the apple, and give the apple to her
horse. (Tus, the horse received I teaspoonful of Protocel
twice each
day). Ladd loved the taste of the formula so much that if any accidentally
spilled on the ground, he would eagerly lick it up. After about three to
four months of doing this regularly, all of Ladds melanoma was gone,
and he was a completely normal horse again with no spots and no bulg-
ing mass in his ear.
To conrm the stories I heard about using Protocel
on a few
of his dogs and cats. An example of a success story he had was with an
201 Protocel
Formula 23, the dog was feeling a lot better and, in the second month,
stopped vomiting altogether. Te dog continued to feel better and better
throughout the year, and by October of 2002 all of his tests and blood
work were completely normal. In about nine months, this extremely sick
dog showed no more signs of cancer.
Te most remarkably fast recovery that this veterinarian observed,
however, was when he used Protocel
23 every eight hours. (Tree times, spaced out as evenly as possible,
over every 24-hour period.)
For medium sized dogs: teaspoonful of Protocel
23 every eight
hours. (Tree times, spaced out as evenly as possible, over every 24-hour
period.)
For large dogs: I/3 teaspoonful of Protocel
23 every 8 if possible;
every I2 hours otherwise. (Can be placed on the inner part of a cored
apple or other treat.)
Administering the 3 daily doses as evenly spaced out as possible, every
8 hours, keeps a level amount of Protocel
203 Protocel
for Cancer?
Tis is a question that cannot be answered with specic numbers
because no formal clinical trials or even informal human case studies have
ever been done on Entelev
, Cancell
, or Protocel
. What we do know
is that countless cancer patients have achieved full recoveries through
the use of this formula alone and that their stories along with the NCI
in-vitro studies done in I990 (see pages I59I63) show that this formula
kills cancer very well.
However, whether or not a person achieves a full recovery depends on
many factors and these factors greatly impact its success rate. Obviously,
it is extremely important that Protocel
since they
usually contain mercury, formaldehyde and other toxic substances. Tese
can weaken the immune system and put a toxic load on the body.
And too many cancer patients have successfully reached the all-clear
point according to diagnostics only to stop too soon and then suer a
cancer recurrence. Friends or family of these people may think that the
204 oursxair \oui caxcii
Protocel
will not work during those periods, but simply means it may
be a more dicult situation and progress should be carefully monitored
to gauge the response to the formula. Again, in these situations, larger
or more frequent doses may be needed. (Some people even increase their
dosing of Protocel
, ask for
Dr. Kimberly Cassidy (Doctor of Naturopathy)
Renewal and Wellness, LLC (South Carolina)
(888) 581-4442, (864) 962-8880, (866) 776-8623
Mon.Turs. 9:00-5:00 / Fri. 9:00-4:00 EST
Orders can be placed by phone or online at:
www.Protocel.com or www.WebNd.com
206 oursxair \oui caxcii
For purchases Health-E-Options (Victoria, Australia)
in Australia: (+61) 03-8648-5606
email: sales@healtheoptions.com.au
www.healtheoptions.com.au
(In Australia, Protocel
50 in the U.S.)
Cost of Treatment: Protocel
Support Forum
www.elonnascorner.com
207
I3
Flaxseed Oil and Cottage Cheese
A
truly remarkable all-natural cancer recovery approach is the Flax-
seed Oil and Cottage Cheese diet developed by German biochem-
ist Dr. Johanna Budwig. Dr. Budwig held a Ph.D. in natural science,
went through medical training to become a physician, and was schooled
in pharmaceutical science, physics, botany, and biology. Because of her
important contributions to science and medicine, she was nominated by
her peers to receive a Nobel Prize seven dierent times!
Dr. Budwigs most important contribution to the world involved her
pioneering research into the roles of essential fatty acids. Her discoveries
began in the I950s, and over time, she illuminated a common causative
factor behind many of our modern degenerative diseases, including cancer.
In a nutshell, Dr. Budwig found that the widespread dietary habits of our
modern world tend to promote a dangerous deciency in the essential
fatty acids so important to good health. She discovered that, as a result
of modern food industry practices, we no longer eat enough good oils
in their natural states, and instead, eat too many chemically altered oils
that are damaging to our health. Tis tends to create a situation where
we become decient in two of the most important categories of essential
fatty acids: the omega-3 and omega-6 fatty acids.
Dr. Budwig found that in order to mass produce and distribute food
products high in oils (e.g., salad dressings, cooking oils, margarine, etc.),
modern food manufacturers put these products through chemical processes
208 oursxair \oui caxcii
to deliberately alter the makeup of the oils. Tese alterations are done
because most healthful oils easily go rancid once they are processed out
of the natural foods they are found in, such as vegetables, sh, seeds, and
nuts. Once these oils are exposed to heat and sunlight for periods of time,
as they would necessarily be through shipping and storage, they can eas-
ily degrade into a spoiled state. Tus, manufacturers of common food
products such as margarines and bottled oils used in cooking or salad
dressings, must put the oils they market through chemical processes so
they can be packaged, shipped, and left to sit on store shelves for long
periods of time.
Te process of chemically altering natural oils is good for the manufac-
turers prots, but bad for the consumers health because these processes
turn good, healthful, natural oils into harmful oils, or pseudo fats, as
Dr. Budwig called them. Some of the most health-damaging pseudo fats
are the hydrogenated and partially hydrogenated fats and oils, but many
of the processed poly-unsaturated fats can be harmful as well.
It might surprise many people that all margarines and virtually all fried
foods include these extremely harmful fats. Many other common foods
contain harmful fats as well. For instance, any solidied peanut butter
that does not show a layer of oil at the top of the jar when sold is made
up of altered, harmful oils.
History and Teory
It wasnt until the late I920s that essential fatty acids were begin-
ning to be understood and categorized by researchers. Although food
industries were producing substances such as margarine since the I930s,
they did not understand all the eects these altered oils would have on
people. When Dr. Budwig began studying them in the I950s, she was
able to discover much more about the metabolism of oils in the body
than had previously been known to the scientic world. She began her
research by rst studying and categorizing thousands of blood samples
from people who were seriously ill, then comparing those samples to
the blood of people who were healthy. One of the things Dr. Budwig
discovered was a strange greenish-yellow substance in the blood of
people with debilitating chronic illnesses. Tis was not found in the
blood of people who were healthy. What was alarming was that this
greenish-yellow substance appeared in place of healthy, red oxygen-
carrying hemoglobin!
209 Flaxseed Oil and Cottage Cheese
Dr. Budwig saw this greenish-yellow substance over and over in the
blood of people with cancer, in particular. She also discovered a marked
lack of phosphatides (an important fatty compound) and lipoproteins (fats
bound to proteins) in the blood of cancer patients. After more research,
Dr. Budwig discovered that these anomalies were linked to a severe de-
ciency of omega-3 and omega-6 essential fatty acids (EFAs). Tey are called
essential because they are critical to good health and are substances our
bodies cant make and therefore must be supplied through diet.
Tere are a variety of omega-3 and omega-6 essential fatty acids which
are found in many dierent natural foods that we eat. In general, certain
ocean shparticularly the oily, cold-water sh such as tuna, salmon,
and mackerelare the foods highest in the omega-3 essential fatty acids,
and certain seeds and nuts are the foods highest in the omega-6 essen-
tial fatty acids. (I like to remember this general rule by saying to myself,
Omega-3 from the sea; omega-6 from the sticks.)
Some food sources have both types of EFAs, however. When Dr. Bud-
wig discovered a link between the deciency of these essential fatty acids
and many degenerative diseases, she looked for a natural way to replenish
them. She settled on axseed oil because it is an extremely rich source
of both omega-6 and omega-3 fatty acidsand because it is particularly
high in the very important omega-3s, which tend to be the most de-
cient. Unrened, cold-pressed axseed oil contains a whopping I5 to
25 percent linoleic acid (omega-6), and an incredible 50 to 60 percent
alpha-linolenic acid (omega-3). (NOTE: Flax seeds are called linseeds
in many places, so the term axseed oil refers to the same thing as the
term linseed oil.)
Dr. Budwig discovered that omega-3 and omega-6 essential fatty
acids play a critical role in protecting us from cancer, especially in the
following three ways:
I. Tey help maintain the health and integrity of cell membranes
2. Tey help promote oxygen transport into cells
3. Tey are required in the bodys production of prostaglandins
She also found that people tend to be more decient in the omega-3s
than the omega-6s. Tis may be because people in the modern world tend
to have more sources of omega-6 EFAs from other seed oils in their diets,
such as saower oil, sunower oil, corn oil, sesame oil, and soybean oil.
210 oursxair \oui caxcii
Lipids and Cell Wall Integrity
Every cell in our body is covered with a protective membrane, or cell
wall, that is made up of lipids (fats). In his book, How to Fight Cancer
and Win, William L. Fischer states:
Each cell in this miracle we call the body is protectively covered with
a sheath of fats. Te cell body (plasma) is interlaced with little lipid veins,
often called the nerves of the cell. Tese lipid veins are the connection
between the nucleus and the outer membrane. Tey inuence the care
and feeding of the cell and the process of normal cell division by the use
of tiny electrical impulses.
Dr. Budwig came to believe that cancer was a result, not of too much
cell growth, but of faulty cell growth, or cell division. She proposed that
this faulty cell division was caused by not enough essential fatty acids in
the cell membrane along with an accumulation of harmful manmade fats
in the cell membrane. In her book, Flax Oil as a True Aid Against Arthri-
tis, Heart Infarction, Cancer and Other Diseases, Dr. Budwig explains the
important role of the lipoid membrane in the process of cell division:
In growing cells, we nd a dipolarity between the electrically posi-
tive nucleus and the electrically negative cell membrane with its highly
unsaturated fatty acids. When the cell divides, it is the cell nucleus which
begins this. Te cell body and the daughter cell are then separated and
tied o by the lipoid membrane. When a cell divides, its surface area is
larger and must, of necessity, contain enough material in this surface
with its fatty acids, to be able to divide the new cell completely from
the original. Normal growth is always distinguished by a clearly dened
course of action. In all our skin and membranes, in that of adults too,
there are continual growth processes. Te old cells have to be shed with
new ones being formed underneath. When this process is interrupted,
it means the body is beginning to die.
Dr. Budwig reasoned that the common deciency of essential fatty acids
in cancer patientsevidenced by a marked lack of phospholipids in their
bloodwas why cancer cells often have multiple sets of chromosomes.
Te normal cell would attempt to divide but wouldnt have enough lipids
necessary to complete the formation of the new cell membrane. Rather
than one mother cell becoming two daughter cells, the mother cell would
become one daughter cellbut the mother cells chromosomes would have
already divided and replicated themselves. Tus, according to Dr. Budwig,
211 Flaxseed Oil and Cottage Cheese
the daughter cell becomes an abomination with too many chromosomes
due to lack of material for building new cell walls.
Lipids and Oxygenation
Te oxygen utilization of every cell in our body depends on essential
fatty acids. For instance, without natural, unaltered linoleic acid (omega-
6), the body cannot produce hemoglobin. And without hemoglobin, the
blood cannot carry oxygen to all the bodys cells. Another way that EFAs
oxygenate cells is by attracting oxygen to the cell via the cell membrane.
When a cell has a normal and healthy cell membrane, this membrane is
full of highly unsaturated essential fatty acids. Te unsaturated aspect
of the lipids means that they have lots of unbound electrons looking for
something to bind to. One thing they love to bind to is oxygen. Tis
then brings oxygen to the cell, which supports and stimulates the respi-
ratory process of the cell itself and promotes better transport of oxygen
into the cell.
Taking a closer look at the mechanics of cells, every cell wall (or cell
membrane) is made up of lipids (or fats). Te most common lipids in
the membrane are the omega-3 essential fatty acids and cholesterol. Te
polyunsaturated EFAs found in virgin, cold-pressed, unrened axseed
oil are electron-rich. Tese natural polyunsaturated fats greedily bind to
oxygen and proteins. When absorbed into cell walls, they attract oxygen
to the cell. When bound to sulfur-based proteins, they are water-soluble
and free-owing and their electron-rich characteristic is reserved as a form
of energy that the body can use when it needs to.
Te problem with pseudo fats and oils that have been chemically
rened and altered for marketing is that, in order to extend the shelf life
of these oils, the vital electron cloud of the essential fatty acids has been
destroyed. Te resultant eect is that these essential fatty acids can no
longer bind to proteins to make them more assimilable by the body, and
they can no longer attract and bind to oxygen. William L. Fischer explains
this in How to Fight Cancer and Win:
Te chemical processing of fats destroys the vital electron cloud,
demonstrated in the foregoing material to be of immense importance
to the functioning of every cell in the body. Once the electrons have
been removed, these fats can no longer bind with oxygen and actually
become an obstacle to the process of breathing. Te heart, for instance,
rejects these fats, and they end up as inorganic fatty deposits on the heart
212 oursxair \oui caxcii
muscle itself. As we pointed out earlier, a diseased heart and its aortas
clearly show deposits of these worthless, electrically dead lipids.
Chemically processed fats are not water-soluble when bound to protein.
Tey end up blocking circulation, and they damage heart action, inhibit
cell renewal, and impede the free ow of blood and lymph uids. Te
bioelectrical action in these areas slows down and may become completely
paralyzed. Te entire organism shows a measurable loss of electrical energy
that is replenished only by adding active lipids to the diet.
Unfortunately, the amount of manmade, partially hydrogenated oils
known as trans-fatty acids is extremely high in modern Western diets.
Tese trans-fats are so similar to cholesterol that our bodies cannot tell
the dierence. Tey are mistakenly used by the body in place of good
cholesterol to build cell membranes. Tis then causes these cell mem-
branes to lack a vital electrical charge that would normally attract oxy-
gen. Without sucient oxygen, the cellular environment becomes more
and more anaerobic. Te damaging trans-fats also impede the cellular
exchange of nutrition and waste products through the membrane, or cell
wall. Tey may even contribute to adult-onset diabetes because insulin
is a large molecule that cannot easily pass through cell walls made up of
manmade pseudo-fats.
As mentioned in previous chapters, Dr. Otto Warburg believed that
insucient oxygen is the key reason that normal cells turn into cancer
cells. He also reportedly proved that, by reducing the oxygen levels in
tissues by about 35 percent, he could consistently induce the development
of cancer. Dr. Budwig stated that Dr. Warburg believed the insucient
uptake of oxygen by cancer cells was somehow linked to fat metabolism
and that Warburg tried to prove this theory by working with oils. But
according to Dr. Budwig, Warburg was not successful because he did
not use the right type of oils in his studies.
When Dr. Budwig discovered the role that omega-3 and omega-6
fatty acids play in oxygenating cells, she believed that she had found the
missing link Dr. Warburg had been looking for. In other words, she had
found the reason cells sometimes resorted to anaerobic functioning!
Lipids and Prostaglandins
Another important function of the omega-3 and omega-6 essential
fatty acids is that they can be converted by the body into prostaglandins.
Prostaglandins are hormone-like substances that have far-reaching eects
213 Flaxseed Oil and Cottage Cheese
on many dierent systems of the body. Tere are more than a dozen dif-
ferent prostaglandins that our bodies manufacture, none of which can
be biosynthesized without sucient essential fatty acids from our diet.
EFA-derived prostaglandins regulate kidney function, inammation
response, and immune functioning in our bodies. Tey also help to keep
blood vessels elastic, regulate blood pressure, inuence platelet stickiness,
and are necessary for proper metabolization of cholesterol. (Tese last
functions of prostaglandins are largely why sucient EFAs in the diet
are important to cardiovascular health.) Tus, the prostaglandins play
many roles in a healthy, well-functioning immune system and help the
body to resist the development of cancer. And natural, unaltered EFAs
are critical to the production of prostaglandins.
So, What Does Cottage Cheese Have to Do With It?
By now, you are probably wondering what cottage cheese has to do
with anything. Obviously, what Dr. Budwig discovered was how impor-
tant essential fatty acids are. Te way that cottage cheese comes into play
is the following. In researching how to most eciently get the depleted
essential fatty acids back into our bodies, Dr. Budwig found that the bodys
assimilation and use of essential fatty acids was greatly enhanced when the
fatty acids were combined with sulfur-based proteins. In fact, nature has
provided this combination already for us since most of the natural sources
of essential fatty acids, such as milk, nuts, and seeds, also contain sulfur-
based proteins.
Sulfur-based proteins are also found in many other foods, such as
onions, leeks, chives, garlic, and yogurt. In her attempt to reverse advanced
degenerative diseases, Dr. Budwig believed she needed to quickly replen-
ish her patients bodies with sucient EFAs, and axseed oil was the
highest source around. Ten, she searched for the richest dietary source
of sulfur-based proteins to go with the axseed oil. She nally settled on
a food called Quark. Quark is common in Germany and is similar to
cottage cheese and yogurt. However, Quark is dicult to obtain out-
side of Germany. Next to Quark, cottage cheese is the richest source of
sulfur-based proteins and is the most commonly used option around the
world for the Budwig cancer approach. By combining axseed oil with
the sulfur-based proteins in Quark or cottage cheese, the essential fatty
acids bind to the sulfur-based proteins, and this makes them water-soluble
and much more bio-available to the body.
214 oursxair \oui caxcii
Dr. Budwig also discovered that there were certain vitamin and min-
eral co-factors that aided the body in its use of the essential fatty acids.
Te primary co-factors are vitamins B, B, and C, and the minerals
magnesium and zinc. Tese nutrients are all required by the body to
make prostaglandins.
Tus, though the essential fatty acids are the main dietary factor needed
for recovery from degenerative diseases such as cancer, simply ingesting
axseed oil alone will not work as well as combining the axseed oil with
foods rich in sulfur-based proteins. In fact, there is some evidence that
taking axseed oil daily without sucient sulfur-based proteins in the
diet may even be harmful. (Tis is why some recent scientic studies that
test the use of axseed oil alone for cancer do not show results anywhere
near what Dr. Budwig was able to achieve.)
In case after case, Dr. Budwig found that thoroughly mixed axseed
oil with cottage cheese was an ecient and successful way of replenishing
the bodys levels of essential fatty acids. She proved that, through the use
of her special dietary approach, the anomalous greenish-yellow elements in
her patients blood would disappear over about three months and would
be replaced by healthy red blood cells. Normal levels of phosphatides
and lipoproteins would reappear in the blood as well, and tumors would
disappear. Dr. Budwig reportedly accumulated over I,000 documented
cases of cancer recoveries with her special dietary approach!
As a result of her in-depth research and clinical practice, Dr. Budwig
claimed the following:
Lipoproteins can be found in all biochemically active tissues and always
contain highly unsaturated fatty acids and sulfur-rich proteins.
Anesthetics and certain drugs, such as barbiturates, sleeping pills, and
painkillers, can separate highly unsaturated fatty acids from sulfur-
containing proteins.
Hard carcinoma tumors can be dissolved with serums high in essential
fatty acids and organically bound sulfur.
Polymerized pseudo-fats of marine origin (such as sh and whale oils)
that have been radically altered by being subjected to high tempera-
tures for use in margarines, have been isolated from soft tumors.
215 Flaxseed Oil and Cottage Cheese
Opposition and Suppression
History tells us that the many health benets of ax have been appre-
ciated for thousands of years. Flax was cultivated in Babylon as early as
5,000 n.c. Hippocrates wrote about the healing benets of ax. And
ancient scripts from India claim that a yogi must eat ax daily in order
to achieve the highest state of contentment and joy possible.
Unfortunately, in the modern world, big businesses have gotten in
the way of some of our most ancient healing traditions. Dr. Budwig
met with ferocious opposition from various powers in the food industry,
particularly from the margarine producers. She was the rst scientist
to oppose the modern practice of altering of oils for commercial distri-
bution purposes. Her conicts started with Professor H.P. Kaufmann,
who was the head of the German Institute she was doing her research at.
Kaufman also happened to be a very famous lipid expert who had been
nicknamed Te Pope of Fats and Oils. He held patents for some of the
hydrogenation processes that produced the very polymers Dr. Budwig
claimed were harmful to our bodies and which she had isolated from
soft tumors. Tus, even though her research was sound, he had a strong
nancial interest in the use of these polymers, or pseudo-fats, particularly
by the margarine industry.
According to Johanna Budwig, Dr. Kaufmann tried to bribe her with
money to keep her from publicizing her discoveries about oils. She refused
his bribe, whereupon he supposedly denied her any further access to the
research institute facilities he headed. When Dr. Budwig tried to move
to another institute where she could continue her research, she found her
access blocked by what she felt was an industry-wide conspiracy against
her. Apparently, the Pope of Fats and margarine industry moguls had
mobilized in some way to keep her from continuing her work in modern
scientic laboratories. She also found herself blocked from publishing her
research in scientic journals. Her only recourse then was to write books
and share her information with the public that way.
Te one good that came from Dr. Budwigs banishment from further
laboratory research was that she spent more time working with patients
in a clinical setting. It is unfortunate, however, that she was not able to
continue her formal research, which might have given us an even better
understanding of fat metabolism and its connection with serious illnesses
such as cancer.
216 oursxair \oui caxcii
Dr. Budwigs Dietary Protocol
Anyone wishing to use Dr. Budwigs approach should be aware of the
protocol she recommended. Te basic rules of her approach are listed below,
but I do not recommend that readers rely solely on what is written here.
If you are interested in using the axseed oil and cottage cheese diet to
recover from an illness, please refer to the books and Internet sites listed
at the end of this chapter for more detailed information about what other
dietary restrictions or supplements may be helpful.
Primary ingredient: Toroughly mixed low-fat cottage cheese (pref-
erably I percent organic) with unrened, virgin, cold-pressed axseed
oil. Te ratio of these two items may vary depending on the severity of
disease, but the minimum ratio is I tablespoon axseed oil to cup cot-
tage cheese. For patients with serious illnesses such as cancer, Dr. Budwig
suggested anywhere from 3 to 6 tablespoons of axseed oil per cup of
cottage cheese per day. Using a blender or other sort of electrical mixer
is important to optimally mix the oil and cottage cheese and thus bind
the essential fatty acids with the sulfur-based proteins. Various fresh or
frozen fruits, honey, and/or stevia can be added to the mix to make it
tasty. Lowfat or skim milk or unsweetened fruit juice can also be added.
Keep the blended mix refrigerated and eat it throughout the day.
If preferred, low-fat plain yogurt may be substituted for cottage cheese.
However, since yogurt is not quite as high in sulfur-based proteins as cot-
tage cheese is, one should triple the amount of yogurt used.
People who are allergic to dairy products have varied responses to this
mixture. Some nd that, even though they are generally lactose-intolerant,
they tolerate the FSO/CC mixture just ne. Others may want to look into
dierent sources of sulfur-based proteins that may be used instead of cot-
tage cheese or yogurt (though it may be dicult to achieve the optimum
eect with other substitutions.) One possible non-dairy substitution is a
special supplement in capsule form that contains dried sulfurated proteins.
Natures Distributors, based in Arizona, sells this type of supplement.
Teir phone number is (800) 624-7II4, and their non-dairy substitute
for cottage cheese sulfurated proteins is called Companion Nutrients.
Natures Distributors claims that one capsule of Companion Nutrients
can activate the essential fatty acids in one tablespoon of ax oil.
Along with eating one of the above mixtures every day, Dr. Budwig
included some dietary restrictions in her healing approach to help pro-
mote recovery. Tese restrictions are the following:
217 Flaxseed Oil and Cottage Cheese
Foods to Completely Avoid
Rened sugar (Unsweetened grape juice and honey okay)
All animal fats
All salad oils, including commercial mayonnaise
All meats containing chemicals, hormones, or preservatives
Butter
Anything hydrogenated (such as margarine or fried foods)
Fresh vegetable juices, such as carrot, celery, apple, and red beet, are
ne. Dr. Budwig also thought it essential to drink a warm tea, such as
peppermint, rose hips, or grape tea, three times a day. (Black tea before
noon is okay.) For those who would sorely miss butter and mayonnaise,
there is a special axseed oil spread that can be prepared and used as
well as a special axseed oil mayonnaise. (For more details on how to
prepare these, refer to Chapter 7 of Fischers book, How to Fight Cancer
and Win. Chapters 6 and 7 of Fischers book present an excellent in-depth
description of Dr. Budwigs protocol for cancer.)
Remember to use only unrened, cold-pressed axseed oil that is sold
in a dark (light-blocking) bottle and kept refrigerated at all times. Barleans
is an excellent brand and is very high-quality oil. For best results, use
the bottled liquid oil rather than capsules and keep the bottle refriger-
ated. It takes about I4 capsules of axseed oil to equal just I tablespoon
of the bottled oil, and many times the bottles of capsules are allowed to
sit on store shelves or warehouses in the heat which can cause the oil to
become rancid.
Flax seeds freshly ground at home in a coee grinder and used immedi-
ately can be added to the daily mixture. But do not grind your ax seeds
at a health food store, then drive home and expect them to still be good.
Dr. Budwig claimed that the oils in freshly ground ax seeds can go bad
in just I0 to I5 minutes! Tere are more details to this diet that can be
obtained from the resources listed in the back of this chapter. Tese should
be studied and followed carefully if you have life-threatening cancer and
choose to use this approach.
Although some people have a remarkably fast disappearance of tumors
using this approachsometimes in just a few monthsothers may take
longer. Dr. Budwig recommended that people using this dietary treatment
218 oursxair \oui caxcii
for serious illnesses stay on it for three to ve years to achieve complete
healing. According to Dr. Budwig, people who break the rules of the diet
(for example by eating preserved meats, candy, etc.) may grow rapidly worse
to the point where they cannot be saved. However, some people have just
used axseed oil thoroughly mixed into cottage cheese on a daily basis,
without adhering to the other aspects of Budwigs dietary protocol, and
have still done quite well. To be on the safe side, however, it is probably
best to stick as closely to her original protocol as possible.
Here are two simple recipes that can be tried. Te rst creates a soft-
yogurt consistency and can be poured into a bowl to eat with a spoon.
Te second creates a milkshake consistency and can be poured into a
glass to drink.
I. Mix in a blender these ve ingredients:
I cup low-fat, organic cottage cheese
4 tablespoons unrened, cold-pressed axseed oil
2 fresh peaches (sliced), or other fresh fruit
I tablespoon honey
Juice from lemon
2. Mix in a blender these nine ingredients:
I cup unsweetened grape or pineapple juice
I banana, cut up
I cups frozen, dark cherries
cup low-fat cottage cheese
I cup plain, nonfat yogurt
cup freshly ground axseeds
2 tablespoons raw wheat germ
2 to 3 tablespoons axseed oil
I to 2 tablespoons honey
You can create your own unique recipes for combining axseed oil and
cottage cheese. Pineapple is another tasty fruit to mix with it, for example.
Just be sure to also supplement with co-factors that help the activation of
the essential fatty acids. A daily multiple B vitamin (or wheat germ) and
a daily multiple mineral supplement of some sort are a good idea. Tere
are some excellent cancer recovery stories to be found in Fischers book,
219 Flaxseed Oil and Cottage Cheese
How to Fight Cancer and Win, and there are many others that can also be
found on the Internet. (www.healingcancernaturally.com has an excellent
compilation of recoveries using this diet for both humans and pets with
cancer.) Te following case stories were recorded from interviews with
people I contacted and spoke with myself.
Case Stories
Case Story #IMetastasized Prostate Cancer
Cli Beckwith is an American man who has done a great deal to spread
the word about the use of axseed oil and cottage cheese for cancer. (I
use his full name here because he publicly posts his story on his website:
www.beckwithfamily.com.)
In January of I99I, Cli was diagnosed with prostate cancer. Initial
bone scans and other tests indicated that the cancer had not spread, so
surgery was recommended. During the operation, however, Clis surgeon
discovered that his cancer had in fact metastasized to his lymph glands.
Because of this, Cli was diagnosed as stage IV, and the operation was not
completed. His doctor said that, since the cancer was in his lymph system,
it would not do any good to cut it out locally at the prostate gland.
At that point, it was decided to use the drugs Lupron and Eulexin to
block his production of testosterone. Cli went on the drugs, but in the
meantime, he also found out about Dr. Budwigs axseed oil and cottage
cheese approach. He read that most people are about 80 percent decient
in omega-3 and that Dr. Budwig had worked with cancer patients who
sometimes had only a few hours to live and restored them to health.
So Cli gave it a try. For two and a half years he put about half a cup
of cottage cheese and some fruit, such as crushed pineapple or frozen
strawberries, mixed with just 2 tablespoons of axseed oil and a little
honey, in the refrigerator. He ate that throughout the day. When he was
rst diagnosed, Clis PSA count was 75. After just six months of eating
the axseed oil and cottage cheese on a daily basis, Cli had another PSA
test done. He got a call from his doctors oce the following Monday
and the oce girl exclaimed, Mr. Beckwith! Your count is completely
normal! Clis PSA was down to 0.I.
For the rst four years, Cli continued to get PSA readings at six-
month intervals, and every time, his count was between 0.0 and 0.I6.
He had continued on the hormone blockade throughout these years, so
220 oursxair \oui caxcii
the axseed oil and cottage cheese mixture was not the only thing he was
doing. Cli knew that the hormone-blocking drugs could also eectively
lower PSA counts for a while. But when he asked his doctor if he had
expected the counts to go down that much, the doctor said, No way!
After I995, Cli was no longer on the Eulexin and Lupron and was
just using axseed oil and cottage cheese. In the years since stopping
the hormone-blocking drugs, his PSA level has varied just a little more.
As of this writing, in August 2003, Cli is still doing great and has no
clinical signs of metastasis to other organs. He is 82 years old, and his
PSA count has remained in a normal range for a man of his age. Best of
all, Cli has already lived about I2 years longer than his doctor thought
he would.
Over the years, Cli has helped many people with his Internet site
and also with an audiotape about axseed oil and cottage cheese that he
created to give out to people who needed information. He has known
of over I00 people who have successfully used this method of treatment
to help them recover from all types of cancer. He has even known some
stories of axseed oil and cottage cheese working to help dogs recover
from cancer.
Unfortunately, Cli has also known people who were getting well
using the FSO/CC combination (their cancer markers were going down,
symptoms were going away, etc.), but were convinced by their doctors
to do more chemotherapy or radiation. Many of these people who had
been beating their cancer by replenishing their essential omega fatty
acids then died after doing conventional treatment. Apparently, many
of these peoples doctors could see that their patient was recovering from
cancer but couldnt accept that they were doing it without the help of
conventional medicine.
Case Story #2Metastasized Pancreatic Cancer
William is a 72-year-old man whom friends and family have always
called Huck. About I0 years ago, at the end of I993, Huck suddenly
became very ill. He was overcome with extreme pain and nausea, and was
rushed to a nearby hospital emergency room. Doctors there were unable
to nd the problem, so they sent him home. However, the symptoms kept
returning, with Huck suering from about a half-dozen painful attacks
by the end of January. He was nally admitted to the hospital in late
January of I994 to undergo more tests. Te doctors suspected a problem
221 Flaxseed Oil and Cottage Cheese
with his pancreas but hospital tests still showed nothing. A CT scan also
showed nothing unusual.
Because of his severe pain, Huck requested that his gallbladder be
removed in case that was the problem. Tis surgery was done on Febru-
ary 7' and went smoothly. For a few days, Huck seemed to feel better,
but then the pain returned in the same place it had been before. He saw
some other specialists, but they couldnt nd anything, either. Toward
the end of April, Huck had lost 50 pounds and suered his worst attack
of pain ever.
Finally, in May of I994, another CT scan was done, and this time it
showed some serious changes in his pancreas. Te doctors could now see
that Hucks pancreas had tripled in size since his rst scan in January. He
was referred to a pancreatic surgeon, who tried an endoscopic procedure
to learn more details of what was going on. Unfortunately, that did not
reveal anything either. So the next day, Huck went into surgery. After
opening him up, the surgeon found malignant pancreatic cancer that
had metastasized (stage IV). Hucks primary tumor in the pancreas was
about the size of two slightly attened lemons. It was also obvious now
that the tumor had reached out and grown around the blood vessel run-
ning between the pancreas and liver, as well as around another primary
blood vessel.
Te surgeon knew there was no way he could surgically remove all of
the cancer and didnt even try to cut it out. Te only thing the surgeon
did before sewing Huck back up was to take a few ne needle biopsy
samples. (Te needle biopsies came back from the lab indicating that the
type of pancreatic cancer was adenocarcinoma.) After surgery, Huck
was told he would probably not live more than three months. Huck and
his wife, Nan, were told that neither chemotherapy nor radiation would
help, so no treatment was recommended.
Huck and Nan left the hospital with a terrible diagnosis, but they
didnt give up. Tey looked into alternative approaches. First, Huck
started drinking six I2-ounce glasses of fresh vegetable juices each day
and improved his diet. By the end of June, he also started getting Laetrile
treatments at an alternative clinic. Every day (except Sundays) for three
weeks, he received intravenous Laetrile along with DMSO and massive
amounts of vitamin C. After that, Huck switched to oral Laetrile tablets.
Huck added other supplements to his daily regimen, too, as well as Essiac
tea. Ten, around mid-August, Huck and Nan found out about axseed
oil and cottage cheese, so he started taking I tablespoon of axseed oil
222 oursxair \oui caxcii
with I tablespoon of cottage cheese after every meal. His total intake of
oil was 3 tablespoons a day.
Huck never did any conventional treatment for his cancer but gradually
began to feel better and better. In December I994, he was feeling very
well and had put back on 25 pounds. Another CT scan was performed,
and unbelievably, just seven months after being diagnosed with metasta-
sized pancreatic cancer, his doctor could not nd anything abnormal on
the scan at all! Te doctor was stunned. He called in the radiologist to
look at the scan with him, but the radiologist could not nd any cancer
or anything else out of the ordinary, either.
On December 28, I994, a blood test was taken to measure levels of a
pancreatic cancer marker. Tis test is called the CA-I9-9. For this test, the
normal range is between 0 and 37. Hucks test came back at I7. Over the
years, Huck continued to get regular CT scans. Every time, the results
showed him to be clear of cancer. In April I997, he had another CA-I9-9
test done. His count this time was I4.
Huck gradually stopped using the axseed oil and cottage cheese as
well as the Laetrile tablets. He went back to eating a normal, healthy diet,
and he continues to take some supplements. He has had no recurrence
of cancer since, and his doctor has had a hard time believing it. At rst,
Huck would receive a phone call from his doctors oce about every three
months, just to see how he was doing. After a while, his doctors oce
only called him every six months, then once a year. Finally, the doctors
oce stopped calling him.
Hucks story is truly an amazing one. People who are diagnosed with
stage IV pancreatic cancer are given virtually no chance for long-term
recovery by standard medical practices. Probably everything Huck did
worked together to help him get well. Laetrile treatment can be a very
powerful approach but does not appear to have high success rates for
metastasized cancer when the intravenous part of the treatment is only
done for three weeks. Usually, patients must keep coming back for intra-
venous Laetrile treatments in order to fully recovery. Although it is hard
to be sure, Huck and Nan believe the axseed oil and cottage cheese
combination had the biggest impact.
Case Story #3Breast Cancer
Hucks wife, Nan, now has her own cancer story. In October 2002,
Nans breast started hurting and she noticed a big lump that had not been
223 Flaxseed Oil and Cottage Cheese
there before. She had undergone a mammogram just a couple of months
before, and, strangely, it had showed her to be ne. But with the lump
clearly observable now, she was given an ultrasound. Te ultrasound
showed that Nan most denitely had a tumor, and a needle biopsy came
up with the diagnosis of lobular inltrating carcinoma.
Nans doctor immediately recommended a mastectomy followed by
chemotherapy. Nan had seen too many other people die after going through
chemo for cancer, and she had also seen her own husband recover with-
out it. So, she refused all surgery and chemotherapy. She started eating
axseed oil and cottage cheese every day instead. Her conventional doctor
refused to monitor her progress if she didnt do the standard treatments,
so she had to look around for another doctor who would. Luckily, she
found one with whom she could work.
Nan did not do any Laetrile treatments as her husband had done
because the doctor who administered them to Huck had since moved. She
started with 6 tablespoons of axseed oil mixed with cottage cheese every
day. She also cleaned up her diet, avoided all junk food, and took lots of
vitamin and mineral supplements. After a few months, Nan reduced her
intake of axseed oil to 3 tablespoons a day.
When Nan had been diagnosed with breast cancer in October 2002,
her tumor was almost as big as a golf ball. Another ultrasound in January
2003 showed that the tumor was stable in size (showed no increase). A
full-body CT scan was done, and there was no indication that the cancer
had spread to any other areas. In July 2003, the breast tumor was down
to the size of a marble. Te pain in Nans breast has been gone since mid-
November, and she feels great otherwise. Nan continues to diligently eat
her axseed oil and cottage cheese on a daily basis.
Case Story #4Prostate Cancer
Because of Cli Beckwiths inuence, many other men with prostate
cancer have found out about using axseed oil and cottage cheese and
have their own great success stories. Seventy-eight-year-old Chester is one
of them. Seven years ago, Chester was diagnosed with prostate cancer. At
diagnosis, his PSA count was 24. Chesters doctors administered radiation
ve days a week for a total of 39 treatments. Chester also started taking
axseed oil and cottage cheese on a daily basis.
For the rst ve months or so, Chester took 6 tablespoons of axseed
oil a day. After that, he went down to 2 tablespoons a day and has stayed
224 oursxair \oui caxcii
on that ever since. Chester just puts the oil in a bowl, stirs in about half
a cup of cottage cheese, and eats it. From 24, his PSA count went down
to I2, which is the level it stayed at for over three years. Ten, his count
went down even more, and for the last few years has remained at 5.
Chester feels great and still works in his own barbershop, where he
tells anyone who is interested about the healing wonder of axseed oil
and cottage cheese.
Case Story #5Brain Cancer
Tom Rolland was only 37 years old when, on February I0, 2002,
he was rushed to the hospital with a splitting headache and projectile
vomiting. He thought he just had a very bad migraine, but was to nd
out instead that he had a malignant brain tumor. Two days later, he was
rushed into surgery, and the resultant biopsy on his tumor came back
with a diagnosis of glioblastoma multiforme, stage IV.
Although Toms surgeon said he had removed all of the cancer he
could see, Tom was told he would probably only live about six months if
he did not undergo post-operative radiation treatments, and only about a
year if he did do the radiation. Tis prognosis was due to the reality that
glioblastomas virtually always grow back quickly, even if all of the visible
tumor has been removed. And radiation is only a palliative treatment in
these cases, not a curative one. Tom gave the radiation a try, but stopped
it after only ve days of treatments because it made him feel so awful.
Being Christians, Tom and his wife, Kelly, decided it was time to seek
guidance, and they went to their church. Tey had Tom anointed with
oil and hands laid on him in prayer by the elders of the church (according
to James 5:I4). Tey also began to look into holistic methods of ghting
cancer. After all, there was nothing conventional medicine could do that
would oer him a chance of long-term cure.
Trough other members of the church, Tom and Kelly then found out
about Dr. Budwigs axseed oil and cottage cheese treatment and they
started Tom on this in March 2002. For the rst three months, Tom
mixed cup of low fat (2 percent) cottage cheese with I tablespoon of
axseed oil twice a day. Tus, every day he took a total of just 2 table-
spoons of axseed oil with cottage cheese. He also took three 750 mil-
ligram capsules of shark cartilage three times every day. On top of that,
Kelly frequently rubbed frankincense oil on Toms head because they had
heard that this oil has anti-cancer properties.
225 Flaxseed Oil and Cottage Cheese
Tree months after his diagnosis and surgery, Toms MRI looked very
good. His brain was clean and the hole where they had removed the tumor
was empty except for a tiny line around a portion of the inside. Toms
doctor thought this line could be either (I) scar tissue, (2) a benign bit of
tumor, or (3) re-growth of the glioblastoma. After the three-month mark,
Tom and Kelly added Graviola tincture to his daily regimen. (Tom took
the Graviola for about nine months.) Tey also had Tom take daily supple-
ments of borage seed oil, CoQ, and a barley/mineral supplement called
AIM Garden Trio. And he cut back on his intake of meat and sugar.
At the six-month mark, Tom had another MRI, and this time his brain
was completely clean! Tere was no cancer visible anywhere. Toms doctor
said it was a miracle, and that in I4 years of practice, he had never seen
anything like it. All of Toms MRIs since then have been clean, and he
just had his I8-month MRI. Still no sign of cancer!
Tom has been given his life back, and he and Kelly have posted his story
on the Internet to help others. Teir website address is: www.axoife.
com. Tey dont know what caused his brain tumor, but they suspect that
it may have been caused by articial sweeteners. Before he was diagnosed,
Tom had been regularly drinking at least 2 liters of diet soda every day.
Now, of course, he no longer ingests articial sweeteners, and he, Kelly,
and their two children are very happy he found out about axseed oil and
cottage cheese. Tom and Kelly feel very strongly that their prayers were
answered and say, We believe that the Lord provided all of the informa-
tion to get Tom well and we have to give Him the Glory.
Cli Beckwith reports that most of the people he has seen recover
from cancer by using axseed oil and cottage cheese did not know about
Dr. Budwigs other rigid dietary requirements. Tus, it appears that it is
possible to get well without following her full strict protocol. But according
to Cli, some of those who did not keep up the axseed oil and cottage
cheese after their cancer went away found themselves facing a recurrence
of cancer in a few years. It is possible that if one does not follow Dr. Bud-
wigs full dietary protocol for three to ve years to fully heal the body,
then one may have to stay on the daily axseed oil and cottage cheese
indenitely to avoid having their cancer come back.
Some experts believe that although axseed oil is eective in treating
degenerative diseases, it might be too rich in omega-3 fatty acids to be used
on a daily basis for more than ve years. In other words, at some point,
a person should go back to consuming a two-to-one ratio of omega-6s
226 oursxair \oui caxcii
to omega-3s. Udo Erasmus, author of Fats Tat Heal, Fats Tat Kill,
states that a person using axseed oil as their sole source of essential fatty
acids will develop an omega-6 deciency over time. He claims to have
remedied this problem by creating his own mixed oil blend with added
sunower and sesame oils. Tis product is called Udos Choice Blend.
It also contains the omega-9 essential fatty acids, and may be something
to consider using once normal health has been regained.
However, it is rare that a person will be using the axseed oil as his or
her sole source of EFAs. Tis is because most people do get some signi-
cant amounts of the omega-6 fatty acids from other dietary sources. For
anyone wishing to check the levels of omega-3 and omega-6 fatty acids
in their bodies, there is a laboratory in Asheville, North Carolina, that
can tell you what your levels are from a simple blood test. (For contact
information, see Resources at the end of this chapter.)
It is still somewhat unclear as to why Dr. Budwig chose axseed oil
as the best way to replenish EFA deciency when much of her research
seemed to indicate that the omega-6 EFAs were the more important de-
ciency involved in cancer. It is speculated that, though the omega-6s are
extremely important, we tend to be more decient in omega-3s. Tis may
be because there are numerous other vegetable oil sources of omega-6s
in our diets. Tus, we tend to be much more decient in omega-3 than
omega-6. Regaining a balance between these two EFAs is very important
in the process of regaining health. Dr. Budwigs clinical results from work-
ing with very ill people certainly proved that the axseed oil combination
of essential fatty acids is extremely eective.
Treatment and Guidance
Unfortunately, Dr. Budwig died in 2003 at the age of 94. She had
suered a fall from which she was unable to recover. Specic doctors or
clinics that specialize in the use of Johanna Budwigs approach to healing
are not easy to nd, so the axseed oil and cottage cheese diet is almost
always a self-administered cancer therapy at this point. Te exception to
this rule is Las Mariposas Clinic in Spain. It uses an omega-3 approach,
along with other supportive non-toxic techniques, and I have heard they
have a very high cure rate for cancer.
For those people who are not able to attend the Las Mariposas Clinic,
there are some very helpful Internet support groups dealing with the use
of axseed oil and cottage cheese for cancer. Tese can be searched for
227 Flaxseed Oil and Cottage Cheese
online using the common abbreviations FSO/CC, or FO/CC. In
addition, there is a cancer coach named Bill Henderson whose contact
information and book are listed below. Bill is an expert on many dier-
ent alternative cancer treatment methods and is particularly experienced
in helping people to use Dr. Budwigs approach for optimum results. I
have heard great reports from people who have worked with him and I
highly recommend his book and coaching service.
Resources:
Las Mariposas Clinic Phone: (34) 952-057171 or (34) 619 966281
Malaga, Spain www.mariposasclinic.com
Great Smokies Diagnostic Lab
(To Measure Your Omega-3 and Omega-6 Levels )
800/522-4762, Ext. 343 or 828/253-0621
Coaching Service
Bill Henderson, author of Cancer-Free: Your Guide to Gentle, Non-toxic
Healing, 3rd Ed., provides coaching for those who wish to use the axseed
oil and cottage cheese approach along with other supportive supplements
or treatments. To nd out about his service, go to www.beating-cancer-
gently.com.
Books
William L. Fischer. How to Fight Cancer and Win. Baltimore: Agora
Health Books, 2000.
Bill Henderson. Cancer-Free: Your Guide to Gentle, Non-toxic Healing,
3rd Edition. Booklocker.com, Inc., 2008.
Udo Erasmus. Fats Tat Heal, Fats Tat Kill. British Columbia, Canada:
Alive Books, 1993.
Dr. Johanna Budwig. Flax Oil As a True Aid Against Arthritis, Heart
Infarction, Cancer, and Other Diseases. Vancouver, Canada: Apple Pub-
lishing, 1994.
228 oursxair \oui caxcii
Websites
www.budwigcenter.com
www.whale.to/cancer/budwig.html
www.healingcancernaturally.com
www.beating-cancer-gently.com
www.aspartame.ca/page_c1.htm
www.beckwithfamily.com
www.mnwelldir.org/docs/cancer1/budwig.htm
www.road-to-health.com/news/36/budwig.htm
www.fatsthatheal.com
229
I4
Te Rife Machine
I
n this chapter, well look at another of the early non-toxic cancer treat-
ments. Tis approach from the early I900s may have been the most eec-
tive method of treating cancer ever developed, but it is a dicult approach
to acquire in its original form these days. Still, since it is an option many
people will hear about, and since it will hopefully be resurrected in its
original form someday, it is an approach worth knowing about.
In the I920s and I930s, an American named Royal R. Rife developed
an audio frequency-emitting device that, when directed at a person with
cancer, was able to send frequencies into the persons body that would
destroy micro-organisms he found to be causally associated with cancer.
Over a number of months of treatments, cancer patients of all types got
well. Tis approach involved a theory of cancer that we have not yet
discussed. Tis theory has to do with the concept that certain types of
micro-organisms are involved in the development of cancer. It may sound
hard to believe, but the fact is that research by numerous highly respected
scientists has supported this theory repeatedly.
To the misfortune of the entire world, Rifes approach was never fully
accepted into mainstream medicine and was never used in a widespread
way. However, there are still some forms of Rife Machines in existence
today and some people claim to have achieved complete cancer recovery
through their use. Te current diculty for cancer patients is determining
which of the machines available today are similar enough to the original
230 oursxair \oui caxcii
Rife Machine to be eective. It appears that none of the Rife machines
sold today are exactly the same as the one Royal Rife developed and used.
Although some modern Rife Machines may be close to the original and
be eective for some people, others may be quite far from authentic with
little eectiveness.
Terefore, if you are considering using a Rife Machine for cancer, it
is important to understand the history and issues to look into. Hope-
fully, someday, the original Rife method will be reproduced in all of its
authentic aspects and will once again be available to the world.
History and Teory
Royal Raymond Rife was born in the late I800s and was undoubtedly
one of the great scientic geniuses of the 20th century. At a young age,
he became interested in becoming a medical doctor and attended Johns
Hopkins University to pursue this dream. During his studies, he realized
he was really more interested in the eld of bacteriology, and decided to
specialize in that. Rife began photographing specimens for Heidelberg
University, and because of his great contribution to that institution, he
was awarded an honorary doctorate of parasitology in I9I4. Realizing
the restrictions of microscope technology, Dr. Rife became very involved
in the eld of microscope development, and studied for a while with some
of the worlds top German microscope specialists.
Jobs in bacteriology were scarce, however, so when Dr. Rife returned
to the United States he took a position as a chaueur for a wealthy busi-
nessman in San Diego, California. Tis businessman was Henry Timkin,
a leader in the ball-bearing industry. Timkin discussed with Rife some of
the production problems he was having, and Dr. Rife was able to develop a
new type of motor for Timkins business. Te motor and other innovative
improvements to Timkins ball-bearing business ended up saving Timkin
millions of dollars and, in appreciation, Timkin set up a life-time stipend
for Dr. Rife. Te stipends monthly payments allowed Rife to focus his
eorts on his work in bacteriology. A number of other wealthy people
also believed in Rifes abilities and helped nance a privately owned and
fully equipped laboratory for his work.
Finally free to do his work in microbiology without restriction, Rife
began to experiment with a bold new idea he had been toying withthat
of electrically stimulating micro-organisms as a method of aecting them.
Rife then made a discovery that should have been heralded later in all the
231 The Rife Machine
history books. He discovered that, by using audio frequencies, he could
actually kill micro-organisms. Finding that dierent frequencies were
required to kill dierent organisms, he named each specic frequency the
M.O.R., or Mortal Oscillatory Rate, for each particular organism.
Rife soon faced a big problem, however. He wanted to include viruses in
his study and realized that, in order to see such small organisms, he would
have to somehow get around a limiting problem. Tis was the problem
that standard microscopes could only magnify up to 2,500 times diameter.
It was a mechanical problem that resulted from how microscopes were
made, and was due to the limiting factor that no micro-organism could
be seen if it was smaller than half a wavelength of light in size.
By I920, Rife had solved this problem by single-handedly developing
a new type of microscope. Rifes innovative microscope could magnify
up to 9,000 diameters with clarity! Tis was far more powerful than
any other microscope yet developed in his time. He then began seeing
and categorizing forms of micro-organisms that had never been clearly
observed by anyone before.
But Rife soon encountered another problem. Tere were even more
micro-organisms that he and other researchers could not see because the
organisms themselves were smaller than the molecules in the dyes or acids
used to stain specimens for observation. To get around this problem, Rife
devised and patented a totally new way to observe specimens under a micro-
scope without staining by focusing on the spectrographic light properties
which coordinated with the chemical makeup of the micro-organisms he
was trying to study. In order to do this, he employed numerous quartz
lenses immersed in glycerin. What Rife did is dicult to explain in simple
terms, but basically he gured out a way to stain his specimens with
light instead of dye. Rifes new microscope was eight times more power-
ful than the best microscopes used by physicists of his day.
Troughout the I920s, Dr. Rife kept searching in his laboratory for
the cause of cancer. He believed it would be a virus-like organism. In
I932, he found two forms of just such an organism. One form, which
he called BX, was the organism that caused carcinomas, and the other
form, called BY, was the organism that caused sarcomas. He also found
that this virus-like organism was pleomorphic. In other words, the cause
of cancer was an organism that could take more than one form. In one
form, it was benign and not cancer-causingin another form it was
cancer-causing.
Pleomorphism was an idea supported by the I9th-century French
232 oursxair \oui caxcii
scientist, Antoine Bechamp. In those early days of microbiology, Antoine
Bechamp and Louis Pasteur were the leaders in a huge battle of ideas
regarding the forms microbes could take. Pasteur believed that microbes
were distinct organisms with distinct, or unchanging, characteristics. In
other words, every microbe is either a particular form of bacteria, or a
particular form of virus, yeast, or fungi throughout its life cycle, and there
is no crossover between forms. Pasteurs theory of microbes is referred to
as monomorphism.
Bechamp, on the other hand, argued that micro-organisms may not
necessarily be limited to one distinct form. In his view, micro-organisms
were capable of being pleomorphic, or capable of having more than one
form in a given life cycle. Tis meant that the shape of a microbe could
drastically change (i.e., a rod-shaped bacteria could turn into a spheroid-
shaped bacteria) and the size of a microbe could drastically change during
the life-cycle of a single organism. Bechamp argued that micro-organisms
could undergo these changes in response to the state of health of the host
organism in which the microbe lived. Bechamp believed, for instance,
that bacteria could actually devolve into a much smaller form which he
called microzymia. His theory of pleomorphism included the possibil-
ity that bacteria could turn into virus-sized organisms in some situations
as a response to their environment.
A key turning point in history occurred when Pasteurs ideas won out,
which caused monomorphism to become the basis of todays modern views
in microbiology. But many reputable scientists of the 20th century have
since proven Bechamps ideas of pleomorphism to be correct and have
continued to debate the issue.
One important aspect of Rifes work to understand is that, in the early
I930s, viruses were just beginning to be dened. Scientists knew quite a
bit about bacteria already and had devised special lters that could lter
out certain bacteria from the media or environment they were in. Te
size of an average bacterium is about I micron (or I/25,000 of an inch in
length). But the largest virus is only about to this size. Tis means
that most viruses are too small to be seen by any normal light micro-
scope. (Although they can be seen now under an electron microscope,
the electron microscope kills the specimen, so they can not be seen in
their living state.)
Because viruses could not be seen in the early I900s, scientists had to
rely on the process of ltering out viruses from cultures and then detect-
ing them by other means. Te ltering process was done using lters with
233 The Rife Machine
pores too small for bacteria to pass through. Scientists decided that any-
thing that passed through these special lters must be something dierent
from bacteria, and they referred to the organisms that passed through
as lterable viruses. (Eventually, the word lterable was dropped and
they were just called viruses.) In the early days, this ltering process
was the only way to designate the dierence between bacteria and viruses.
Although more ways of dening viruses have since become accepted,
there is still debate as to whether certain organisms are actually viruses
or bacteria, and some organisms previously categorized as viruses have
since been proven to be lterable bacteria instead.
Given the many shortcomings in microbiology in the I930s, Dr. Rifes
discoveries were phenomenal. He was not only able to nd a micro-organ-
ism involved in the development of cancer for the rst time in history,
but he was also able to prove the organism was pleomorphic, with the
smaller life-cycle forms having the characteristics of a virus! Eventually,
Dr. Rife identied four distinct forms that this cancer-causing organism
could take within its life cycle:
I. Te BX virus (cause of carcinoma)
2. Te BY virus (cause of sarcoma and larger than BX)
3. Monococcoid form (can be seen through standard microscopes in the
blood monocytes of more than 90 percent of cancer patients)
4. Crytomyces pleomorphia fungi
Amazingly, Dr. Rife was able to culture the BX cancer virus from a
fungoid organism. He then used this virus to directly produce cancer in
hundreds of laboratory animals. He also proved that any of the above
four forms of one organism could change back into the BX cancer virus
within 36 hours. In fact, he was able to complete the cycle of virus to
cancer and back to virus I04 times. He could observe and document all
of this with his powerful microscope, something other scientists could not
do. Tere is no doubt that Rife found a micro-organism involved in the
development of cancer. And his discovery was veried and documented
by other prominent microbiologists who visited his laboratory.
Even now, with the electron microscope, the back and forth culturing
of a micro-organism from bacterial form to viral form cannot be observed
because the electron microscope virtually destroys any virus that is put
234 oursxair \oui caxcii
under it. What Dr. Rife discovered wasand still isground-breaking
news. However, although he proved a micro-organism connection to
cancer, he also discovered that this did not mean cancer is an infectious
disease. Te key is that the organism is pleomorphic and only takes a
cancer-causing form when a persons inner environment, or state of health,
is poor or unbalanced. So, this micro-organism was not something people
could catch from one another. In fact, it was something we all have in
us in its healthy form. It is only when our inner environment becomes
unhealthy that this organism turns into its unhealthy form.
Royal Rife was not some unknown kook. Over the years, he was
given I4 government awards for scientic discoveries, was visited and
acclaimed by world experts in medicine and microbiology, and had his
accomplishments written up in many newspapers and magazines. A
prominent professor, Arthur I. Kendall, Ph.D., and a prominent physician,
Milbank Johnson, M.D., soon began collaborating with Dr. Rife. Drs.
Kendall and Rife both observed normal tuberculosis bacteria convert to
a lterable type of bacteria the size of a virus, something not previously
observed. Dr. Kendall, Dr. Johnson, and many other medical specialists
were extremely impressed with Dr. Rifes accomplishments and whole-
heartedly supported his work.
But Dr. Rife did not stop at simply nding the pleomorphic micro-
organism responsible for cancerhe also found a way to destroy it. To do
this, Rife experimented with a wide variety of audio and light frequen-
cies to nd just the right frequency, or M.O.R., that would kill what he
called the cancer virus. He only used sine waves, which are pure tones
or frequencies. (Most sound is made up of a jumble of frequencies, as is
most light. However, a sine wave is a single frequency.) X-ray tubes were
the prominent medical technology of the day, so Rife worked with that
mode of delivery. Once he found the cancer virsuss M.O.R., he could
then deliver that devastating frequency to the organism. Rife could liter-
ally see cancer viruses moving around alive under his microscope, then
briey zap them with the correct frequency from his ray tube, and
immediately observe that all the viruses on the same slide, which had
been moving around only seconds before, were now dead! Tis way, with
the help of his microscope, he could determine which sine waves would
kill the organism in a particular human.
Since audio waves do not broadcast eciently, more research and
experimentation was required for Rife to be able to successfully deliver
the mortal oscillatory rate of frequency to cancer organisms deep inside
235 The Rife Machine
tissues of living animals. Rife solved this problem of delivery by using a
carrier wave. In other words, the audio frequency which turned out to
be the specic M.O.R. for the cancer virus would not penetrate tissue
deeply enough for many internal cancers, so Rife ingeniously modulated
(or piggy-backed) the desired audio frequency to another frequency
that could penetrate deep tissue. If he hadnt done this, he would have
only been able to treat cancers on or near the surface of the body. Te
two frequencies travel together but remain separate and distinct. Rifes
records later showed that he used frequencies ranging from the audio
range to I7MHz, and that he also experimented with many dierent
carrier frequencies.
Rifes theory that the BX virus caused cancer was proved to be sound
when he injected 4II laboratory mice with the BX virus and produced 4II
corresponding tumors. Ten, he was able to use his ray tube to completely
eliminate the cancers in many of these animals. Rifes method was not
directed at killing the cancer cell itself. Rather, he found the BX or BY
virus to be inside each malignant cancer cell and that killing this micro-
organism would cause the malignant cell to also die o.
In I987, after doing a great deal of research, author Barry Lynes wrote
the denitive book on Royal Rife and his cancer cure. Tis excellent book,
Te Cancer Cure Tat Worked: Fifty Years of Suppression, is packed with
fascinating information and is available today and well worth reading.
According to Barry Lynes, By the end of I932, Rife could destroy the
typhus bacteria, the polio virus, the herpes virus, the cancer virus and
other viruses in a culture and in experimental animals.
0
In I934, Dr. Milbank Johnson set up a committee of leading medi-
cal experts to oversee human trials in a southern California clinic where
Rife could start treating terminally ill patients who had no other hope
for cure. Te initial results were astounding. In just 70 days of treatment,
this committee of physicians pronounced I4 out of I6 patients with termi-
nal cancer cured. Tus, this rst human trial showed a success of 87.5
percent. Moreover, after 60 more days of treatment, the remaining two
patients from the original trial were also pronounced cured. Tis meant
that within I30 days, or just a little over four months, all I6 terminally
ill cancer patients were pronounced cured by the committee of medical
experts. After this amazing success, other doctors obtained ray tubes
and operated them in their own clinics with a general success rate of
about 90 percent.
Te cancer treatment itself was totally non-toxic. It caused no tissue
236 oursxair \oui caxcii
damage whatsoever, and a person receiving Rifes frequency treatment
could not feel or hear anything. Tey merely saw a tube light up for
three to ve minutes, and the treatment was done. Te only slightly toxic
aspect of the treatment resulted from the die-o of the cancer micro-
organisms. In fact, Rife discovered with his human cancer patients that
the treatment was most eective when given at the rate of only three to
ve minutes exposure to frequency every other day. Tis was because he
found that if he treated his patients every day, the toxins released by the
dead micro-organisms accumulated too fast in the patients bodies and
caused toxic overload. When he limited treatment to every other day,
however, patients responded with incredible recoveries.
During the I930s, Rife collaborated with many cancer researchers
and doctors. Several reputable physicians began using Rifes frequency
instrument on their patients with great success. Tey began seeing can-
cers of all sorts disappear. Tey also observed other conditions unexpect-
edly resolving after treatments with the ray tube. Tese other conditions
included syphilis and gonorrhea.
But the original ray tube Dr. Rife built was too cumbersome and
expensive to market to doctors and clinics worldwide. It lled almost
a whole room. So he signed an agreement with business colleagues to
form a company called Beam Ray Corporation that would begin build-
ing Dr. Rifes frequency instruments for the purpose of selling them to
medical practitioners. Unfortunately, however, not all of the businessmen
involved were conscientious enough to make sure the machines were built
correctly and according to Rifes specications. His rst business part-
ner, Philip Hoyland, built the machines to emit harmonics of frequencies
in order to save money, rather than building them to just emit specic,
clean frequencies. Beam Ray Corporations machines understandably
performed poorly and Dr. Rife was not happy with what the corpora-
tion was doing.
Ten, events took place that ended up bringing about the nal down-
fall of the Rife frequency technology. Tese events began when Morris
Fishbein, the head of the American Medical Association (AMA), tried to
buy into Beam Ray Corporation. Basically, Fishbein was attempting to
take control for his own nancial gain, but he only wanted to give Royal
Rife a small royalty on the machines. (Tis was the same man who had
tried to gain ownership of the Hoxsey therapy for his own prot.)
After all of Dr. Rifes work, the business deal Fishbein oered was
scandalous. Dr. Rife refused Fishbeins unfair business deal, and as a
237 The Rife Machine
result, Fishbein went all out to destroy Beam Ray Corporation. Te AMA
led expensive lawsuits and Beam Ray went bankrupt as a result of legal
battles. To complicate matters, Philip Hoyland reportedly turned against
Rife and also tried to take over total control of Beam Ray Corporation.
Court transcripts from a I938 trial show that Hoyland even tried to claim
he was the originator of some of the technology, instead of Rife.
Later, in the I950s and early I960s, Dr. Rife worked with another
man, John Crane, with whom he formed a company called Life Labs.
Tey modied the technology again to produce a slightly dierent version
of his instrument. Tis one was also portable but used round disks that
came in contact with the body. However, once again, Crane disregarded
some of Rifes suggestions when he built the product. Ten, Crane started
making changes he did not tell anyone about. For instance, he lowered
Rifes frequencies by a factor of I0 so that the machines would fall below
the I0,000 hertz level. It is believed that Crane did this to avoid FCC
regulations that were just coming into place at the time. Tis drastic low-
ering of frequencies meant that the I950s Rife machines could no longer
achieve the impressive results of Rifes earlier I930s machines.
Tus, Life Labs Rife Machines were not working as well as they could
have. At the same time, Morris Fishbein was continuing to do everything
he could to stie Dr. Rifes technology. Doctors were put under pres-
sure from the AMA to not use Rifes machines anymore. As with Harry
Hoxseys herbal remedy, Morris Fishbein used his power as head of the
AMA to stop any progress on treating cancer that he himself could not
prot from. Ten, with just the right timing to put the nal blow on
Dr. Rifes technology, penicillin and other marketable antibiotics began
to take the limelight in medicine. Since Rife had refused to sell Beam
Ray Corporation to Fishbein, Fishbein made sure that the AMA pushed
the concept of ghting diseases with antibiotics rather than with Rifes
technology. Tragically, ghting microbes with frequencies soon fell out
of medical favor.
Nevertheless, Dr. Rife did not give up. He continued to improve
his machine, and in the I950s, he tried again to get the medical com-
munity interested in his methods. Dr. Rife had developed a smaller and
less expensive form of equipment to try to entice doctors to buy them.
Unfortunately, doctors were still being inuenced to use antibiotics, and
the medical community never showed signicant interest in Dr. Rifes
technology again. In I97I, Rife died without ever seeing a widespread
use of his incredibly successful method of treating cancer.
238 oursxair \oui caxcii
In Te Cancer Cure Tat Worked, Barry Lynes sums up Morris Fish-
beins inuence as follows:
. . . within the few, short years from I934 to I939, the cure for cancer
was clinically demonstrated and expanded into curing other diseases on
a daily basis by other doctors, and then terminated when Morris Fish-
bein of the AMA was not allowed to buy in. It was a practice he had
developed into a cold art, but never again would such a single mercenary
deed doom millions of Americans to premature, ugly deaths.
Partly as a result of Barry Lyness book, an underground interest in
the Rife Machine sprang up once more in the I980s and I990s. Many
dierent engineers started building Rife Machines according to blueprints
and records from Rifes original papers. Pros and cons about current-day
Rife Machines aboundsome seeming to work well and others seeming
to not work at all.
One problem is that many of the modern frequency machines claim-
ing to be Rife Machines do not use any carrier wave. Yet, the carrier wave
was an important aspect of Rifes technology and the only way to get the
mortal oscillation sine wave to deep tissue cancers. Another problem is
that some current-day machines do not transfer the frequencies prop-
erly for various reasons. Even though the specic frequencies that Rife
discovered to be M.O.R.s for many dierent organisms and diseases are
actually presented on the Internet, the method of delivery is critical for
these frequencies to be eective. And this appears to be the main reason
why many modern day Rife devices are not as eective as the original
technology was.
It is worth mentioning again that, although Rife found a micro-
organism to be a causal factor to cancer, this did not mean he was proving
cancer to be an infectious disease. In fact, it is most likely that the cancer-
causing micro-organism Dr. Rife identied is within each and every one
of us. Rife agreed with and conrmed Bechamps earlier theory that it
is a bodys inner environment which ultimately inuenced the form the
pleomorphic cancer organism would take. If a persons inner environment
was healthy, then it would remain in its harmless form. If, on the other
hand, a persons inner environment was not healthy, it could devolve
into one of the forms that might cause cancer. (See the next chapter on
7I4X for a similar conclusion made by the French hematologist, Gaston
Naessens.)
Tus, to some extent, both Rife and Antoine Bechamp looked at
239 The Rife Machine
various pleomorphic forms of bacteria as the symptom of disease, not the
cause of disease. Royal Rife, himself, said:
In reality, it is not the bacteria themselves that produce the disease,
but the chemical constituents of these micro-organisms enacting upon
the unbalanced cell metabolism of the human body that in actuality
produce the disease. We also believe if the metabolism of the human
body is perfectly balanced or poised, it is susceptible to no disease.
Tus, it is best to not conclude from this chapter that cancer is a disease
that can be caught by being near someone who has cancer. Instead, we
need to realize that our common ideas about how micro-organisms are
linked to diseases have been molded by one narrow medical viewpoint
that of monomorphism. We must be open to the reality that ideas in
science get molded by various ideas of the times. Barry Lynes makes the
astute observation that Pasteurs monomorphic view of micro-organisms
probably won out for two main reasons: (I) It was a simpler theory and
much easier to understand. And (2) it applied more directly to infectious
diseases which were the biggest problem of that era. (I would also add
that monomorphism won out as the reigning viewpoint in part because
no one had a microscope capable of seeing micro-organisms change
from one form to another.)
It is time for medical science to rethink its reigning theories, espe-
cially since a huge problem of our era happens to be chronic degenerative
diseases in their many formsand some degenerative diseases, such as
cancer, may be better explained by Bechamps theory of pleomorphism.
According to Barry Lynes, the powerful Memorial Sloan-Kettering Can-
cer Center in New York is currently a leading institutional opponent of
the concept of pleomorphismeven though, in I975, Sloan-Ketterings
own studies reportedly showed pleomorphic bacteria-virus in all of their
cancer blood tests. According to Barry Lynes, Sloan-Kettering buried
these laboratory results.
Last but not least, scientists still need to have the right type of micro-
scope in order to view pleomorphism, and even today that type of micro-
scope is not prevalent. Rifes Universal Microscope was virtually lost
to medical science, and there is a rumor that there is only one original
Rife microscope left in existence today. However, there dont appear to be
any institutions trying to duplicate its technology. Although the average
person probably believes that modern medical practices are always based
on true science, there is a great deal of evidence indicating otherwise. As
240 oursxair \oui caxcii
can be seen with the history of Royal Rifes technology, a certain amount
of medical practice is based on professional biases and prot margins of
big business.
And, of course, unfortunate timing was a factor. Antibiotics were
highly protable for pharmaceutical companies to market. Tey also hap-
pened to work quite well for infectious diseases, so it was easy for doctors
and the public to wholeheartedly support them. But the downsides to
antibiotics are showing up more and more with virulent drug-resistant
bacteria becoming more prevalent and side eects to antibiotics taking
their toll. Medical frequency technology, such as Rife created, is much
cleaner with no side eects, and does not create drug-resistant bacteria.
Moreover it works on viruses, which modern medicine still has not been
able to fully conquer.
It is very interesting to note that, in the May 2003 issue of Readers
Digest, there was an article about some new and promising treatments for
breast cancer. On pages 6467, the article talks about one of these new
treatments, called RFA (radiofrequency ablation). RFA is a recently
developed technique whereby a probe is inserted into or next to a tumor
and a certain radio frequency is then emitted for about 23 minutes. With
an ultrasound, the technician performing this procedure can then see the
dark tumor mass become the same grainy gray as the rest of the breast
tissue. Surgeons can then simply go in and remove the tumor, which has
become dead tissue.
Tis Readers Digest article stated that RFA has also been used on
liver cancer since the early I990s, and is currently being tried on breast,
kidney, and lung cancer. One study at Houstons M.D. Anderson Cancer
Center is referred to where 20 women with breast tumors were treated
with RFA. Tis study was small but achieved great success. Out of the
20 subjects, I9 were shown to have had the cancer completely killed!
Te current success of RFA shows that Rifes frequency technology was
based on sound principles, but I wonder if Rifes discoveries will ever be
given credit. No mention of Rife is made in the Readers Digest article
and the modern RFA procedure is referred to as new and experimental.
Too bad the article does not mention that an even more powerful form
of frequency treatment for cancer was administered totally noninvasively
as far back as the I930s.
Maybe one day, we will yet again have Rifes original technology avail-
able to us. Until then, anyone considering using a Rife Machine today
or other similar type of device for cancer should thoroughly research the
241 The Rife Machine
specic device being considered, and make sure that it has been used suc-
cessfully by others with your type of cancer.
Resources:
Book
Barry Lynes. Te Cancer Cure Tat Worked! Ontario, Canada: Marcus
Books, 1987.
Video
Te Royal Rife Story: Historical Documentary, 60 minutes. To order,
call (800) 550-5119. [Tis is an excellent production packed with fas-
cinating information.]
Websites
www.Rife.org
www.scoon.co.uk/Electrotherapy/Rife/BeamRay/
www.scoon.co.uk/Electrotherapy/Rife/BeamRay/Analysis/index.htm
www.royalrife.com
243
I5
7I4X
A
nother unique and fascinating approach that also addresses the rela-
tionship of micro-organisms to cancer is 7I4X. It was developed
by Gaston Naessens, a French biologist and hematologist. While still in
France, Naessens developed two anti-cancer products that created quite
a stir. One was called Ana-Blast and the other was called GN-24. In
I964, Naessens immigrated to Quebec and introduced his innovative
cancer treatments to Canada. In the I970s, Naessens replaced Ana-Blast
and GN-24 by what he called 7I4X, which has now been used by thou-
sands of people to help them recover from cancer and other degenerative
conditions. Considered by many to be a genius, Naessens has become
known in the world of alternative cancer treatments as French Canadas
Wizard.
Naessenss personal background illustrates his creative intellect. He
was born in I924 and, as young as ve years old, built a small functional,
automobile-like vehicle. Next, he built a homemade motorcycle. At age I2,
Naessens built an airplane that ew! When Naessens was old enough to
attend college, he studied physics, chemistry, and biology, and later went
on to study hematology (the study of blood).
Early on, Naessens had a premonition of sorts that there were tiny
particles moving around in blood. But with normal light microscopes of
the I940s, nothing like that could be clearly discerned. So, like Royal Rife,
244 oursxair \oui caxcii
Naessens decided a more powerful microscope (in terms of resolving power)
was needed and he enlisted the aid of some German optical specialists to
manufacture aluminum mirrors for him. Te optical specialists were not
aware of what Naessens was going to do with the mirrors, but they were
to go in the new microscope that Naessens was developing.
Naessenss new microscope, which he called the Somatoscope, was
much more powerful than any other light microscope commonly used
at the time. It used an innovative combination of laser and ultraviolet
light technology and produced a magnication of 30,000 times with
a resolution of I50 angstroms! Any light microscope with a dark eld
condenser can observe live material, so that aspect of the Somatoscope
was not unique. However, the conventional eld of hematology has gen-
erally shown little interest in observing live material and the observation
of living specimens has been a foreign concept to their staining methods.
Te Somatoscope did not require staining a sample before viewing it as
other microscopes did, and this made a big dierence in observing living
organisms in blood.
Te ability to observe behavior and life cycles of living microscopic
organisms in blood made the Somatoscope in some ways superior to
the electron microscope, which was developed later. As mentioned in
the previous chapter, the electron microscope can achieve much higher
magnication (enlargements into the millions of times), but can only
observe dead or static specimens. Tus, it is of little value in observing
actual behavior changes or life cycle changes that might occur in micro-
scopic organisms.
Using his own special microscope, Naessens was able to study the tiny
blood particles he had previously noticed. He could now observe them
with detail and clarity in their living state. Eventually, he identied a
number of dierent micro-organisms that he concluded were all stages
of development for one sub-cellular organism commonly found in blood.
Naessens called this organism a somatid. He believed that somatids
were distinct from bacteria and viruses and, because he could observe
these organisms in their living state, he was able to discern two separate
life cycles for them. One life cycle tended to occur in the blood of healthy
people and the other life cycle tended to occur in the blood of unhealthy
people. (Tis corresponds closely to what Royal Rife discovered and the
work of each of these geniuses supports the work of the other.)
In healthy individuals, the somatids appeared to display what Naes-
sens called a microcycle consisting of 3 dierent forms the somatids
245 714X
would take. In unhealthy individuals, however, the somatids appeared
to display a much longer macrocycle, consisting of I6 dierent forms
that the somatids would take. Tis macrocycle was a more complex life
cycle that Naessens observed in the blood of people with degenerative
diseases. Naessens theorized that somatids play an important role in
the body and that it is normal for them to be found in everyones blood
in their microcycle life stages. But he theorized that when somatids are
exposed to trauma, such as pollution, radiation, and so forth, they can
then enter into a wild and uncontrolled growth cycle (the macrocycle),
which can lead to cancer.
Just as interesting as Naessenss discovery that somatids have dierent
life cycles in healthy versus unhealthy people was his discovery that soma-
tids are everywhere in nature and seem to be an integral part of everything.
In the human body, he found that somatids play a role in the cell division
process of normal cells. According to one source,
What Naessens discovered was that somatids were everywhere, in the
sap of plants, in the blood of animals, and even in lifeless organic matter
like ashes. When he cultured the somatid life cycle, he discovered that
somatids are resistant to acids and bases as well as heat and that they
cannot be cut with a diamond. Cell division cannot take place without
the somatid. Somatids, according to Naessenss theory, release the growth
hormone trephone, which enables cells to divide and multiply. Naessens
believes that the electrically charged somatid is the original spark of life,
the point in which energy condenses into matter.
In other words, Naessens believed somatids to be basic living par-
ticles indispensable to life, and by culturing the somatids and using
his special microscope he could verify their micro and macro cycles.
(Apparently, other scientists who observe these same particles with nor-
mal microscopes generally refer to them as brin formations.) In terms
of how they are involved in the division of normal healthy cells, Naes-
senss theory proposes that when somatids are in their healthy 3-stage
microcycle, they produce just the right amount of a growth hormone-like
substance. Tis substance keeps healthy body cells reproducing at their
correct rate. Naessens called this hormone-like substance trefons (also
spelled as trephones). However, when a persons body is seriously stressed
or weakened, then the somatid shifts into its longer unhealthy I6-stage
macrocycle that includes forms resembling bacteria, viruses and yeasts.
In this extended cycle, the somatids produce excessive amounts of trefons
246 oursxair \oui caxcii
and cause normal, healthy body cells to undergo abnormally fast cell
growth, which can then develop into cancer.
Naessens theorized that a healthy body can hold somatids to their
3-phase cycle by having ample blood inhibitors to keep the soma-
tids functioning normally. Tese blood inhibitors in a healthy person
consist of certain enzymes, hormones, and minerals. Naessens believed
that inadequate nutrition and stress could reduce the amounts of these
inhibitors in the blood and thus allow somatids to shift into their longer
I6-phase cycle.
Naessenss theory of reduced blood inhibitors being a contributing fac-
tor to cancer is consistent with many of the nutritional deciency theories
of cancer development. And his observation that, at dierent life cycle
stages the somatids could resemble either bacteria, yeasts, or fungi, is also
consistent with many ndings over the last century that have indicated a
connection between cancer and various yeasts or fungi.
Tus, there was no doubt in Naessenss mind that the somatid microbes
were involved in the development of cancer, but it was not in the way
that we normally think of microbial involvement. As Dr. Rifes research
suggested, Naessenss research also suggested a type of pleomorphism
whereby common microbes (somatids) in every persons body could,
under certain conditions, change into a dierent form of microbe that can
cause cancer. Some of these forms could be so dierent from the original
microbe that to any observer it would appear that a common bacterium
was actually pleomorphing into a virus or fungus.
An important aspect of Naessenss discovery was that when the soma-
tids switched to their longer life cycles as a result of trauma and/or insuf-
cient blood inhibitors to control them, they then started secreting excess
amounts of their hormone-like substance, which would cause cells to
replicate too fast. Te resultant eect would be a conglomerate of cells
multiplying at an accelerated rate in close proximity to each other and
beginning to form a tumor.
Once Naessens had formulated his theory on how cancer gets started,
he worked to nd a solution for it, which he eventually did. To understand
his solution, we have to understand another interesting fact Naessens
observed. He realized that fast-replicating cancer cells required much
more nitrogen to survive than normal cells do and that they would often
steal the nitrogen away from healthy cells in order to subsist. Naessens
also observed that, in a healthy body, the immune system usually attacks
and destroys any out-of-control conglomerate of cancer cells before the
247 714X
conglomerate gets too big. But Naessens discovered that, if this group
of renegade cells is able to reach a critical mass, then the conglomerate
of cells (or tumor) starts to act like its own entity and begins to emit a
substance Naessens called Co-carcinogenic K Factor (CKF). Teoreti-
cally, CKF paralyzes the immune system by masking the cancer cells
from recognition. CKF thus frees the young tumor from attack by the
body and the cancer cells are able to steal as much nitrogen as they need
from surrounding healthy cells.
Naessens felt that if he could stop cancer cells from producing this
Co-carcinogenic K Factor, then a persons immune system would be able
to recognize and attack the cancer cells. He was nally able to develop
an aqueous solution he called 7I4X. 7I4X is an innovative mixture
of camphor, nitrogen and mineral salts specically created to supply the
cancer cells of the body with the extra nitrogen they need so the tumor
does not have to excrete CKF in an attempt to obtain more nitrogen.
When it does not secrete CKF, it is not hidden from the immune system
and the bodys own defenses can then attack the cancer. Tus, the main
way that 7I4X works against cancer is not by directly killing cancer cells,
but by debilitating the cancers ability to mask itself. Te persons own
immune system then kills the cancer cells.
Naessens found that camphor has a special anity for cancer cells, so
he used natural camphor as the base to carry the nitrogen to the cancer.
Naessens also included ammonium salts in 7I4X because he believed
that they could help to liquefy the lymph uid and increase lymphatic
ow. Tis could help the lymph system deal with toxins better and could
activate certain kinins that inhibit abnormal cell growth. Also found
in 7I4X are I8 dierent minerals in trace element form.
Gaston Naessens designed 7I4X to improve the natural defenses of
the body and to stimulate the immune system. It does not kill abnormal
or cancerous cells, but rather helps the body defend against them and
heal from degenerative diseases and immune-deciency disorders. 7I4X
is administered by injection directly into the lymph system. As a general
agent for healing, it performs two distinct functions:
I. It removes toxins from circulation by liquefying the lymphatic uid.
2. It helps the body to repair itself.
7I4X is not a cytotoxic product, such as chemotherapy, and can be
used safely for any length of time with no negative side eects. Injections
248 oursxair \oui caxcii
are self-administered just under the skin with a very small 3/8-inch needle
and perinodally around a lymph node in the groin area. It is sold by
Cerbe Distribution, Inc., located in Quebec, Canada. Te product comes
with very clear instructions on how to use it, and Cerbe also oers a phone
service that answers inquiries.
7I4X is usually administered through perinodular injection once a
day for 2I days straight. After two days of rest, the injections are repeated
again for 2I days, and this cycle is repeated over and over until the per-
son is disease-free. Te perinodular injections are the main treatment
and cover the main large lymphatic circulation. In some circumstances,
where the disease is localized in the upper body and/or in the upper right
areas, 7I4X may be given by inhalation as well to cover the small lym-
phatic circulation. Tis inhalation, or nebulizer method, is considered an
add-on treatment to be used along with the injection, not instead of it.
Te nebulizer add-on is recommended when there is cancer in the right
breast, the lungs, the esophagus, or anywhere in the head.
How long the treatment takes for each individual will vary. Tis is
partly because each person metabolizes the product at his or her own pace,
and also because the body tends to clean itself before repairing itself.
Tus, the more a person has used toxic treatments such as chemotherapy
or radiation prior to starting 7I4X, the more cleaning out needs to be
done by the body before repair can begin. It is probably safe to say that
the prognosis is best when 7I4X is started immediately after diagnosis.
7I4X can also be used safely while doing conventional cancer treatments,
and in those cases, it can reduce the side eects of the toxic treatments.
Cerbe Distribution recommends that 7I4X be used for a minimum of six
to eight consecutive cycles when a conrmed cancer diagnosis has been
received. Once a person is cancer-free, then a maintenance program of
one or two cycles twice a year is recommended.
Tere is no doubt that 7I4X has brought about truly astounding recov-
eries for many people with late-stage cancer. Most of these people had
reached the point where their disease was not responding to conventional
treatments and their doctors had no other options to oer them. Many
of these remarkable case stories have been documented by physicians or
other reliable sources, and many others can be found throughout the
Internet. Some examples that I found are the following:
Jacques Viens was 39 years old when he had seven-eighths of his
stomach removed, according to writer Stephanie Hiller. Te cancer had
already spread to the lymph. Since there seemed to be no hope of recovery,
249 714X
his doctor oered him 7I4X. Four months after taking 7I4X he was
healthy enough to go hunting and soon resumed his job.
Marcel Caron had intestinal cancer but refused to have his intestine
removed. His wifes breast cancer had been successfully treated with 7I4X
and so he tried it as well. Sixty-ve days after he started treatment, no
cancer was found in Carons body. Eight years later he is still healthy.
Anne Vignal, wife of the former French Counsel General in Que-
bec, sought out medical opinions and was told she could not conceive
children. She was also told that her infertility was due to a lethal form
of leukemia and she had only three to ve years to live. She took 7I4X.
She is now cancer-free and the mother of a healthy son.
Te story of a I7-year-old boy named Luke Stevens is yet another
remarkable story. In August I995, Luke (the son of a South African
chiropractor) developed a giant cell tumor on his knee. Tis grew so
rapidly that it destroyed most of Lukes upper tibia. According to one
source, Surgeons removed the tumor and rebuilt the boys tibia. Four
months later, Mr. Stevenss body rejected his bone graft and the tumor
returned with a vengeance, breaking through the skin and growing into
a hideous, st-sized mass. Stevenss father grew disillusioned with oncolo-
gists, ignoring their advice to amputate his sons leg and begin massive
chemotherapy.
Lukes father found out about 7I4X and his son began that treatment
instead of undergoing amputation and chemotherapy. Lukes condi-
tion rapidly improved and, according to the same source as above, the
tumor disappeared. Subsequent X-rays documented I00 percent bone
regeneration, considered medically impossible. Today, at 2I, Mr. Stevens
attends university and rows on his schools team. He gives all the credit
to Dr. Naessenss therapy. About two-and-one-half years after he was
diagnosed with cancer, Lukes diagnostic tests showed him to be cancer-
free and he has been cancer-free ever since.
Here are 7I4X testimonies from two dierent physicians:
Dr. Florianne Pier, a Belgian physician, reported that over a four-
month period she had treated seven cancer patients with 7I4X. Te
product prolonged the lives, and eased the deaths, of two terminally
aicted patients, she said, and has allowed the other ve who came
to me with seriously advanced cancerous states, to see every one of
their symptoms disappear and to take up their lives as if they had never
incurred the disease.
Dr. Raymond Brown of New York City, a former Sloan-Kettering
250 oursxair \oui caxcii
cancer researcher, told a pretrial press conference how he had treated one
of his own patients with 7I4X for a pancreatic cancer that had proven
resistant to all other forms of treatment. Naessenss therapy had prolonged
the patients life well over expectancy and kept him free of side eects, he
said. Dr. Brown declared that while 7I4X was not a panacea, it deserved
a place in the arsenal of weapons available to ocial medicine.
0
In Canada, 7I4X is still not a fully approved cancer treatment. It is
only allowed for use against cancer on an emergency basis through the
Canadian governments Special Access Program. Tis means that any
Canadian physician wishing to ocially use 7I4X for a cancer patient
must request special authorization to do so on compassionate grounds.
Since January I990, when 7I4X was introduced as an emergency drug
in Canada, to June 2003, I8,366 authorizations were given to I,684
doctors to use 7I4X on behalf of 4,030 patients.
However, 7I4X can be obtained by individuals outside of Canada
without a physicians authorization. Although 7I4X is not approved as a
cancer treatment in the United States, people in the United States can
order this non-toxic compound by simply phoning Cerbe Distribution
in Quebec and having it mailed to them. Te promise of cancer recovery
through this form of treatment is somewhat dicult to ascertain for any
particular person, and may have a lot to do with how soon one starts to
use it after diagnosis. Unfortunately, since the law in Canada only allows
7I4X to be prescribed by doctors as an emergency drug, it is often given
to patients who are so far along in their disease that they are beyond
recovery through any means. Even in these cases, 7I4X has often been
known to improve the patients quality of life (less pain, more appetite,
more energy, etc.). Tere is no risk associated with using 7I4X because
there are no adverse side eects.
Many of the full recoveries involving 7I4X have been achieved without
any other treatment used. But there have also been people who achieved
remarkable recoveries when they combined 7I4X with other alternative,
non-toxic treatments. For example, there is one well-known story of a
teenage boy named Billy Best, who was cured of his Hodgkins lymphoma
in just two and one-half months by the combined use of 7I4X, Essiac
tea, nutritional supplements, and a healthy diet. His story is presented
at www.BillyBest.net.
As we have seen with many other eective alternative non-toxic cancer
treatments, the general rule is that there will be attempts at suppression.
Gaston Naessens, unfortunately, had to deal with this as well. In the mid-
251 714X
I950s, Naessens started to have trouble with the medical authorities in
France. When his unorthodox methods began having incredible success
in the I960s, his laboratory was closed by these authorities, his equip-
ment was conscated, and he was ned for practicing medicine without
a license. Tis prompted Naessens to move to Canada in I964 where he
was able to continue his work for a number of years in a privately funded
laboratory outside Montreal. However, in I989, Naessens was brought to
trial by the Quebec medical authorities. It was a long and dicult trial
where testimony was heard from both patients and physicians who had
used 7I4X for cancer, AIDS, and other degenerative conditions. Dozens
of demonstrators rallied outside the courthouse throughout the proceed-
ings and carried banners in support of Naessens.
Some impressive cancer recovery stories were brought to light through-
out the court battle. For example, one man named Roland Caty testied
that he had been diagnosed with adenosarcoma of the prostate. His con-
ventional doctor recommended he have all of his sexual organs removed.
When Roland refused, his doctor told him hed be dead in three months.
Instead, Roland began to inject himself with 7I4X and achieved a com-
plete recovery. At the trial, Roland Caty told the press, And here I am
testifying to you, eleven years after I got well.
Marcel Caron, another ex-cancer patient, testied with his story.
Marcel had been diagnosed with cancerous intestinal polyps eight years
earlier. As with Roland Caty, surgery was recommended to Marcel by his
conventional doctors. However, Marcel refused because his brother had
died after surgery years before for the very same condition. According to
Marcels court testimony, he used 7I4X instead, and after just 2I days
of treatment he was cancer-free.
Fortunately, this trial resulted in acquittal for Naessens in December
of that same year (I989). In fact, the jury turned in not-guilty verdicts
on all counts. In January I990, the Canadian Federal Government then
hurriedly introduced 7I4X for use as an emergency drug.
So, how has Canadas powerful neighbor, the United States, reacted to
7I4X? In I974, Dr. Raymond Brown from New Yorks Memorial Sloan-
Kettering Cancer Center visited Gaston Naessens and investigated 7I4X.
He was very favorably impressed and wrote an extremely enthusiastic
memorandum about Naessenss work. Below is an excerpted paragraph
from what Dr. Brown wrote:
What I have seen is a microscope that reveals with spectacular clar-
ity the motion and multiplicity of pleomorphic organisms in the blood
252 oursxair \oui caxcii
which are intimately associated with disease states. Te implications . . .
are staggering . . . It is imperative that what its inventor, a dedicated
biological scientist, is doing be totally reviewed. I am convinced that he
is an authentic genius and that his achievements cut across and illumine
some of the most pertinent areas of medical science.
At rst, Memorial Sloan-Kettering was reportedly very interested in
Dr. Browns report. But then they supposedly lost interest in pursuing
7I4X. Some speculations are that Sloan-Kettering dropped their interest
in 7I4X like a hot potato when they found out that the American Cancer
Society had blacklisted Naessens. Apparently, the American Cancer Society
was Sloan-Ketterings biggest monetary contributor in the I970s.
Ten, in 200I, the U.S. National Cancer Institute suddenly put 7I4X
on a fast-track for review. Tis was supposedly in response to patients
in Massachusetts and media reporters making allegations that an inves-
tigation of 7I4X had been covered up the Dana-Farber Cancer Institute
in Boston. In August 200I, Cerbe, Inc. submitted I6 in-depth cases of
patients who had used 7I4X successfully for long-term recovery. Gaston
Naessens and his wife, Jacinte Naessens, attended a press conference in
Boston, and were accompanied by successfully treated 7I4X patients.
One of these patients, I4-year-old Katie Hartley, spoke at the press
conference. In April I995, when Katie was seven years old, she was diag-
nosed with a malignant tumor (undierentiated sarcoma) that was grow-
ing inside her head. It was rst noticed when one of Katies eyes started
to protrude from its socket. Te sarcoma was the size of a tangerine, and
Katies doctors from the Dana-Farber Cancer Institute prescribed che-
motherapy. Katie went through nine of the thirteen weeks of chemo that
had been prescribed. She had to stop it early because of debilitating side
eects of the treatment.
Next, Katie went through six weeks of radiation, after which she was
too weak to continue any further conventional treatment. Her tumor began
to grow again and her doctors sent her home and told her family that she
only had a couple of weeks to live. Katies mother frantically searched for
other options, and in January I996, started her on 7I4X. Tey gave her
injections in the morning and nebulizer treatments at night. A year and
a half later, tests showed that Katies cancer was completely gone.
Te NCIs Oce of Cancer Complementary and Alternative Medicine
(OCCAM) was initially responsible for the review of 7I4X. After that,
it was supposed to go to the Cancer Advisory Panel for Complementary
253 714X
Alternative Medicine (CAPCAM). At this point in time, it is unclear
what the results of the NCI investigation have been or whether they did,
indeed, investigate it.
7I4X is not expensive compared to conventional cancer approaches
and costs about 300 U.S. dollars per 2I-day cycle. Te number of cycles
required for recovery will vary from case to case, but is usually six to eight
cycles, or until conventional tests show remission. No signicant dietary
changes are required, though it is recommended to reduce ones intake
of red meat and dairy products. In terms of other supplements that may
or may not be used in conjunction with this treatment, it is merely sug-
gested that people using 7I4X stay away from supplementation of the
following: vitamin E, vitamin B, and all anti-angiogenic herbs or drugs
(e.g., bindweed, shark or bovine cartilage, or thalidomide). Te amount
of vitamin E or B ingested from a normal diet, however, is ne.
Gaston Naessens is considered by many to be a great contributor to
the eld of microbiology, and his work impacts the treatment of not only
cancer, but other terrible diseases including HIV/AIDS as well. (Tese
other applications of 7I4X are beyond the scope of this book.) Christopher
Bird, co-author of the best-selling book Te Secret Life of Plants, wrote a
detailed book about Gaston Naessens and his struggles with organized
medicine. His book is called Te Persecution and Trial of Gaston Naessens:
Te True Story of the Eorts to Suppress an Alternative Treatment for cancer,
AIDS, and Other Immunologically Based Diseases.
For those people who use 7I4X for cancer, the results can vary quite
a bit and some people feel that the perinodal injections are too painful.
However, sometimes recoveries are simply astounding. To read about and
listen to more current recovery stories from people who have used 7I4X
for cancer, go to www.7I4X.com and click on Testimonials.
Resources:
CERBE Distribution, Inc. (819) 564-7883
5270 Mills Street, Rock Forest www.cerbe.com
Quebec, J1N 3B6
Canada
254 oursxair \oui caxcii
Book
Christopher Bird. Te Persecution and Trial of Gaston Naessens: Te True
Story of the Eorts to Suppress an Alternative Treatment for Cancer, AIDS,
and other Immunologically Based Diseases. Tiburon, California: H. J.
Kramer, 1991.
Video
For around $10, you can purchase an information and instruction video
about 714X by calling the above phone number.
Self-Treatment at Home: 714X is relatively inexpensive and costs only
about $300 per month (and an extra $150 for those who also need to
use the nebulizer). Te number of months of treatment will vary for each
individual.
Websites
www.cerbe.com
www.7I4X.com
www.luminet.net/~wenonah/new/naessens.htm
www.BillyBest.net
255
I6
Cesium High pH Terapy
C
esium high pH therapy is yet another powerful and highly impres-
sive approach for outsmarting cancer. It has brought about some
remarkable recoveries for people with primary cancers as well as late-stage,
metastasized cancers. Tough temporary side eects from this therapy
are often felt, such as diarrhea and tingling sensations in the skin, when
used properly it is a non-toxic approach that targets cancer cells but leaves
healthy cells unharmed.
A particularly positive aspect of cesium high pH therapy is that it can
often quickly reduce the severe pain that accompanies advanced cancer.
It is also sometimes able to reduce large tumors faster than many other
approaches. Tus, for people whose disease is so far advanced that they
may not have time for another alternative approach to work, or are in
such severe pain that they are on heavy narcotics which may be shut-
ting down their bodily functions, cesium high pH therapy may be their
best treatment option. On the other hand, a downside to this approach
is that it is dicult to nd qualied experts who can give guidance for
best results. Some are listed at the back of this chapter, but hopefully
more practitioners will adopt this approach over time and become avail-
able for consultation.
Like Protocel
biochemically interferes with the cell respiration of cancer cells by block-
ing their production of ATP, cesium raises the pH within the cancer cells
to such a high alkalinity that the cancer cells can no longer function and
they die o as a result. Te premise for this approach is based on the fact
that anaerobic cells are much more acidic than normal healthy cells and
must maintain their acidic intracellular environment in order to survive. A
more detailed explanation will follow in the next section but, in a nutshell,
cesium high pH therapy alkalizes cancer cells to death from the inside out !
Cesium has been used to treat cancer in humans since the I980s. But
it has recently been made easier and more eective as a treatment with the
development of liquid ionic minerals. And as you will see, it is because
of this liquid ionic form of cesium that this approach is now more avail-
able to the public for self-administration and bringing about some truly
astounding recoveries for cancer patients.
History and Teory
Te pioneer of cesium high pH therapy was physicist Aubrey Keith
Brewer, Ph.D. Dr. Brewer lived from I893 to I986 and was a highly
esteemed American physicist who focused his research on the study of
cell membranes. For a period of time, he held the position of chief of the
National Bureau of Standards Mass Spectrometer and Isotope section.
Dr. Brewer proved with spectrographic analysis that cancer cells have
an anity for cesiummeaning they readily absorb cesium through
their cell walls. Te fact that cancer cells have an anity for cesium is
also evidenced by the common current-day use of a radioactive isotope
of cesium as a marker in conventional oncology for tracing how well
chemotherapy agents get into tumors.
Dr. Brewer developed his theory of how cancer could be treated with
cesium (the non-radioactive form) based on his understanding of the
physics of cell membranes and the fact that cesium is the most alkaline
mineral. He wrote a number of scientic articles on his theory, and in the
late I970s, initiated animal research studies at three U.S. universities
rst using rubidium (the second most alkaline mineral), then using cesium
chloride. (Cesium Chloride, or CsCl, is also referred to as cesium salts.)
All three university studies proved that high pH therapy was, indeed,
eective against malignant tumors in mice. In fact, these tests showed
marked shrinkage of mouse tumors within just two weeks.
257 Cesium High pH Therapy
Being a Ph.D. physicist and not an M.D., Dr. Brewer could not legally
conduct human clinical trials himself. However, he was able to follow
and write about the clinical work done by several physicians who were
administering cesium to some of their late-stage cancer patientspeople
who had been given up on by conventional medicine and had no other
hope. Two of these physicians were Dr. Hans Nieper of Germany and
Dr. H.E. Sartori of the United States. In I98I, Dr. Brewer was able to
follow the treatment of 30 late-stage terminal cancer patients and the
results were extremely positivefar better than any results conventional
medicine could achieve.
In I984, Dr. Brewer published his ndings in Pharmacology Biochemis-
try and Behavior. In the article, Dr. Brewer explained the cesium approach
to cancer in great scientic detail, and also proposed his understanding
of how normal cells can become cancer cells. Starting with the widely
accepted knowledge that normal healthy cells have membranes which
allow the free exchange of both oxygen and glucose and maintain stable
intracellular environments at around 7.35 pH, Dr. Brewer proposed that
there is a sequence of four main steps that occur as the healthy cell turns
into a cancer cell. Tese steps are summarized below:
How a Healthy Cell Becomes a Cancer Cell
I. When carcinogenic materials, such as environmental toxins, attach
themselves to the outer surface of the cell membrane, the membrane
may become damaged. Tis process involves two factors: (a) the pres-
ence of carcinogenic-type molecules primarily of the polycyclic type,
and (b) an energized state of the membrane, which may result from
prolonged irritation. (Dr. Sartori also felt that X-rays, parasites, or other
factors may damage the cell membrane as well.) At some point, the
membrane of the normal cell may become so damaged and altered that
it can no longer pass certain materials easily. In particular, the dam-
aged cell membrane may no longer be able to readily pass magnesium,
calcium, or sodium into the cell. Since oxygen transport depends on
two of these elements, calcium and magnesium, the cell then becomes
oxygen decient. However, a damaged cell membrane can still pass
potassium, cesium, and rubidium. Since glucose transport depends
on potassium, glucose continues to be fully supplied to the damaged
cell while oxygen is no longer being fully supplied. Without sucient
oxygen to maintain aerobic functioning for energy, the cell reverts to
258 oursxair \oui caxcii
the fermentation of glucose for energy in order to survive. Tus, it
turns into an anaerobic cell.
2. Fermentation of glucose produces lactic acid as a byproduct, and this
lowers the intracellular pH of the cell. Te cell pH drops internally
from the normal 7.35 to around 7, and then to the extremely acidic
pH level of about 6.5. In very advanced stages of cancer, the cell pH
may drop even further to 5.7. Tus, the damaged cell has not only
become an anaerobic cell, but it has also turned into a cell with a
highly acidic internal environment.
3. In the acid medium of the anaerobic cell, the genetic blueprint of the
cell (DNA and RNA) can be easily damaged, resulting in impair-
ment to the cells control mechanism. With the control mechanism
for growth now impaired, the cell rapidly duplicates and grows out
of control as a cancer cell.
4. Various cell enzymes are also completely changed in the acid medium
of the anaerobic cell. Liposomal enzymes are changed into toxic com-
pounds, which kill the cells in the main body of the tumor mass. (A
tumor therefore often consists of a thin layer of rapidly growing cells
surrounding a dead mass.) Te acid toxins leak out from the tumor
mass and poison the host. Tis is also the source of much of the pain
associated with cancer. Tese acid toxins can then act as carcinogens
on other healthy cells, in part by lowering the extracellular pH of
normal healthy tissues to the point where that environment becomes
oxygen decient as well.
Te above sequence of steps is how Dr. Brewer theorized that a nor-
mal cell becomes a cancer cell. His concept of how cesium can then be
used therapeutically to treat cancer is based on the fact that cesium is the
most alkaline (and most alkalizing) of all elements. In fact, when taken
up by cancer cells, cesium is able to radically raise the intracellular pH
of the cancer cells to the very alkaline range of 8.0 to 9.0. In this range,
according to Dr. Brewer, the life of the cancer cell is shorta matter of
days at most. Te cancer cell soon dies and is absorbed by the body uids
and eliminated from the system.
It is important to realize that, when a cancer patient alkalizes his or her
body through diet changes and the use of supplements other than cesium
(or rubidium), the eect on the cancer cell is not nearly as profound. It is
259 Cesium High pH Therapy
widely accepted that cancer cells thrive best in acidic extracellular uids
and do not thrive as well when their uid environment is optimally alkaline.
(See Chapter I8 for more details.) However, in most alkalizing programs
that use diet and supplements, it is the extracellular environment of ones
cancer cells that is being inuenced the most. But what many people
dont realize is that tumors create their own local acidic environments
by their excretion of lactic acid as a by-product of anaerobic functioning
(glycolysis). Tus, many alkalizing programs will have a dicult time
fully alkalizing the area around a tumor, and the tumor will still be able
to thrive in its own little acidic environment even if a persons attempts
at alkalizing are having a positive eect on the rest of their body.
With the use of cesium or rubidium, a person is able to bypass the
external environment of their tumor or tumors and impact the internal
pH of their cancer cells so powerfully that the cancer cells quickly begin
to die o. And cesium is able to limit the transport of glucose across the
cancer cells membrane. Tis causes an immediate decrease in fermenta-
tion and a resultant decrease in lactic acid formation. Since a large part
of the pain associated with cancer is due to lactic acid build-up, cancer
patients using cesium often nd their pain subsiding within about I2 to
24 hours.
Dr. Brewer also determined that there were some other key nutrients
that, when administered in conjunction with high pH therapy, enhanced
the cellular uptake of the cesium. Tese are vitamin A, vitamin C, zinc,
and selenium. And he suspected that the administration of Laetrile would
also greatly enhance the uptake of cesium by the cancer cells. According
to Dr. Brewer:
Te therapy I am proposing is one of changing the pH of the cancer
cell from acid to alkaline. Tis is entirely possible since as already stated,
the cancer cells have lost their pH control mechanism. . . . Tere are areas
of the earth where the incidences of cancer are very low. An analysis of the
foods in these areas shows them to be very high in cesium and rubidium.
It is these elements, which are absent in modern commercial foods, that
prevent cancer growth. I am convinced that it is food that causes cancer,
but it is the food we dont eat and not the food we do eat.
Early Clinical Results
As mentioned earlier, Dr. Brewer reported on 30 cancer patients who
were treated with cesium in the early I980s. In his summary of these
260 oursxair \oui caxcii
cases, Dr. Brewer stated, In each case the tumor masses disappeared. Also
all pains and eects associated with cancer disappeared within I2 to 36
hours; the more chemotherapy and morphine the patient had taken, the
longer the withdrawal period.
Another group of 50 patients was studied over a three-year period with
similarly impressive results. Tese patients were treated by Dr. Sartori
and written about in his book CancerOrwellian or Utopian. All of the
50 subjects were terminal cancer patients with metastatic disease. Forty-
seven of the 50 had received maximal amounts of conventional treatment.
Tree of the subjects were comatose, and I4 were already suering from
previous treatment-related or cancer-related complications. After cesium
treatment was started, pain in all 50 subjects disappeared within one to
three days! Tirteen of the subjects died within the rst two weeks, which
was most likely due to the treatment simply coming too late for them. But,
over the next three years, 50 percent of the original 50 survived. Tis
was an incredible survival rate given that all the patients were very late
stage, had exhausted all conventional forms of treatment, and were all
originally expected to die within weeks. Moreover, post-mortem exami-
nations done on those subjects who died showed substantial shrinkage
of those patients tumor masses.
Well-known German cancer researcher and physician, Dr. Hans Nieper,
also conducted studies on cesium high pH therapy in Germany. Like the
U.S. studies, Dr. Niepers trials were extremely successful.
In Kathleen Deouls revealing book, Cancer Cover-Up, Deoul presents
the story of her husband, Neal Deoul, and his battle with the cancer indus-
trys eorts to suppress eective natural and non-toxic cancer therapies.
In I996, Neal Deoul had provided nancing which enabled a Maryland
company, T-Up, Inc., to become a primary distributor of cesium and
concentrated aloe vera, each sold as natural dietary supplements. (Te
form of aloe vera sold was found to have the ability to greatly stimulate
the immune system and had proven to be very benecial for both cancer
and AIDS patients.) Te cesium and aloe vera were obviously working
for people because T-UP, Inc. had hundreds of testimonies on le from
consumers who claimed life-changing benecial results. T-UP also never
received a single consumer complaint.
But big business was not interested in whether cesium or aloe vera
were benecial to T-UPs ailing customers. And even though Neal Deoul
was not receiving prots from the sale of T-UPs products, he was tar-
geted as a nancier of the company and taken to court for bogus reasons.
261 Cesium High pH Therapy
Ironically, in January I999 while Neal Deoul was battling his case
in court, he himself was diagnosed with prostate cancer. Believing in
T-UPs products, Deoul immediately started administering cesium high
pH therapy to himself along with the aloe vera concentrate. By October
of that same year, his PSA was down to normal levels and there were
no more indications of cancer. Neals complete story is presented in his
wifes book, Cancer Cover-Up.
In Cancer Cover-Up, Kathleen Deoul describes one of the cases that
Dr. Brewer reported in the following way:
Te patient [an individual suering from lymphoma who arrived
in a comatose state] had a massive tumor in his abdomen, as well as an
enlarged liver and spleen. After three months of the High pH therapy,
the tumor had been virtually eliminated, and the liver and spleen were
returned to near normal size. Tree years after the treatment the patient
was still alive.
Deoul states, Clearly, the tests had shown that the High pH therapy
kills cancer. But Big Medicine ignored and continues to ignore these
dramatic results.
Form of Treatment
Until recently, the cesium used to treat cancer was a powdered form
of cesium chloride, also referred to as cesium salts. (Which was the form
that Neal Deoul used to cure his prostate cancer.) Usually given to patients
in capsules, it was eective but somewhat risky to use. Tis was because
the powdered form could build up to toxic levels in the body if taken for
too long a period of time. It could only be safely administered under a
doctors care, and some doctors believed cesium in this form should not
be used for longer than one or two months.
Although some cancer patients continue to successfully use the pow-
dered form of cesium, the use of liquid ionic cesium is becoming more
and more popular. When cesium is administered in liquid ionic form, it
is thought to be more easily assimilated by the body and more quickly
processed out so that it does not build up inside the body. Also, some
experts believe that a smaller amount of the liquid ionic form of cesium
can be used to achieve the same results as larger amounts of the capsule
form.
An ionic mineral is an element that has a positive or negative electrical
262 oursxair \oui caxcii
charge, meaning it has either too many or too few electrons. In this
unstable state, the element bonds readily with water. Because the liquid
ionic version delivers cesium in a form that is bonded to water molecules,
it enters the bloodstream faster than the powdered form, which the body
would have to dissolve in the stomach rst. Te liquid ionic form of
cesium is also thought to penetrate cancer cell walls more easily, causing
it to be more completely absorbed by the cancer cells. As to toxicity, a
dose of 6 grams of liquid ionic cesium per day is only about 5 percent of
the minimum toxic level. (One must remember, though, that extremely
high doses of cesium could cause cancer die-o to occur too fast for the
body to process, thus causing a detoxication crisis.)
Te most important aspect about using cesium safely is making sure
that enough potassium is supplemented along with it. James A. Howen-
stine, M.D. is an expert on cesium high pH therapy and author of the
comprehensive book, A Physicians Guide to Natural Health Products Tat
Work. On page 409 of his book, Howenstine explains why potassium
must be supplemented along with cesium. He states:
Any alkali therapy changes the pH of the body toward a more alkalotic
state. Tis causes movement of potassium into cells, which may result
in low serum potassium values. Tis movement of potassium into cells
means that a person can become seriously depleted of potassium even if
there is no diarrhea or vomiting.
Tus, taking high doses of cesium causes a lowering of serum potassium
levels and a severe potassium deciency can result if sucient potassium
supplementation is not also taken. Te danger of potassium deciency
cannot be overstated, since severe potassium deciency can result in death.
Te prime cause of death from this sort of deciency is heart attack.
Any distributor selling liquid ionic cesium will also sell liquid ionic
potassium, and this is the form of potassium supplementation preferred
when using liquid ionic cesium. People using cesium (either in capsule or
liquid form) should always have their blood potassium level checked on a
regular basis to be sure they are getting enough potassium and not devel-
oping a potassium deciency. For optimal eectiveness, cancer patients
usually also make positive changes in their diets and take other supple-
ments as well to enhance their overall health and immune system.
Even though this therapy is non-toxic when used correctly, cesium
in the amounts required to kill cancer cells can cause stomach upset or
nausea if taken on an empty stomach. Te reason that cesium may cause
263 Cesium High pH Therapy
nausea is because, as natures most alkaline mineral, it reacts with anything
that is highly acidic, including stomach acids. Tis type of discomfort is
generally avoided by only taking cesium right after a meal.
Patients taking cesium may also experience some diarrhea and/or
temporary numbness of the lips and tip of the nose for about 20 minutes
after the intake of cesium. Te numbness or prickling sensations in the
skin on various parts of the body, however, are not indicative of long-term
damage. Tey are simply a result of cesium being a mild nerve stimulant.
Less common symptoms are vomiting, yellow vision, or a peculiar dark
hue to the skin accompanied by cold hands or feet. If these less common
symptoms occur, it is best to simply stop the therapy for 3 or 4 days or
until the side eects subside, then start back up at one-half the previous
dose for a while. People with high blood pressure or other heart condi-
tions should be sure they are under the supervision of a physician while
using cesium.
Te following six real-life cases were recorded for this book from people
who used cesium and potassium in the liquid ionic form.
Case Stories
Case Story #ILung Cancer Metastasized to Bones and Liver
In April 2003, at the age of 82, Olga was diagnosed with advanced
lung cancer. She had such a large tumor in her lung that it could be eas-
ily felt from the outside around her ribs. She underwent chemotherapy
and radiation. But these treatments were ineective, and by June 2003,
Olgas doctors proclaimed that her cancer had spread to every bone in
her body as well as to her liver. Te family was told she would be dead
by September.
Because of her age and advanced state of illness, Olga was too weak to
undergo any more conventional treatments. With no further treatment,
her cancer began to progress quickly. Soon, Olga was having so much
diculty breathing due to the cancer in her lungs, she had to be hooked
up to oxygen 24 hours a day, seven days a week. She was also on heavy
pain medication.
Since the diagnosis, Olgas daughter, Trish, had been trying to nd
something else that could be done for her mother. Luckily, in late August
2003, when Olgas doctors thought she had only a few more weeks to
live, Trish found out about cesium high pH therapy using liquid ionic
264 oursxair \oui caxcii
cesium and potassium. She contacted someone who had experience and
knowledge about how to use this approach safely and started her mother
on it immediately.
Because Olga did not want to take too many dierent supplements,
her treatment protocol was extremely simple. She just took I tablespoon
of liquid ionic cesium and I tablespoon of liquid ionic potassium every
morning right after breakfast and again every evening right after dinner.
She simply stirred the liquid minerals into juice and drank them down.
She also took a coral calcium supplement. Olga used no other treatments,
but she did drink chocolate whey protein mixed into whole milk on a
daily basis to make sure she was getting adequate protein and to help her
gain weight. She also ate red beets every day to help support her liver.
When Trish started helping her mother with the cesium and potas-
sium, she had to quickly lift the oxygen mask o her mothers mouth
and nose to give it to her, then quickly put the oxygen mask back on. It
was so dicult for Olga to breathe that she could barely get by without
the oxygen long enough to take the minerals. But after just a few days
of taking the cesium and potassium, Olga was not so desperate for the
oxygen and could breathe without it for a few extra minutes whenever she
took her minerals. Amazingly, only I0 days after starting the liquid ionic
cesium and liquid ionic potassium, Olga was able to go o the oxygen
altogether. Trish says, It was like a miracle!
Olga continued to feel better as she kept taking the cesium and potas-
sium. Soon, she was out of bed walking around. Within a few months,
Olga was back to being active and living her life almost normally. In
mid-December 2003, another MRI was done. Tis time, only three-
and-one-half months after starting on cesium high pH therapy, her MRI
showed a very dierent picture. Te cancer in Olgas lungs was gone, her
liver was clear, and almost all of the spots on her bones had disappeared.
It looked like her advanced, metastasized cancer was almost all gone, and
the only problem she was experiencing was some severe bone pain that
was either due to some bone fractures caused by the cancer or the fact
that she may have still had a small amount of cancer in her spine that
had not yet had enough time to go away.
Unfortunately, in February 2004, Olga contracted a bad case of the
u that quickly developed into pneumonia. She was rushed to a hospital
and put on intravenous antibiotic treatment along with respiratory therapy.
She showed signs of improvement, but after being sent home with oral
antibiotics, she began to decline again. Her body just could not withstand
265 Cesium High pH Therapy
the infection and she passed away. Olgas daughter, Trish, related the fol-
lowing, however, regarding her mothers cancer status when she passed.
Tey scanned Moms lungs at the hospital, and her lungs were free of
cancer and so was her brain.
Given that almost all of Olgas advanced metastatic cancer was gone,
if she could have avoided the pneumonia somehow and been able to stay
on the cesium therapy a little longer, it is reasonable to assume that she
would have achieved a full recovery.
Case Story #2Multiple Myeloma Metastasized to Bones
Jim was 57 years old when he went to a doctor because he was expe-
riencing terrible pain in his neck. Tests revealed that he had a tumor on
his C3 vertebra that had nearly destroyed the vertebra completely. More
scans showed that he also had tumors on his pelvis, thigh bone, and a few
other bones in his body. A bone marrow sample was then taken through
the hip into the pelvis. Tis was biopsied, and the ocial diagnosis came
back multiple myelomaIGG, stage III.
Multiple myeloma is a malignant cancer of the bone marrow, and this
was considered the primary location of Jims cancer, with metastases to
other bone locations. Te IGG is a particular type of multiple myeloma
that is determined through a blood test, and his IGG count was high
at 5,720. Jims oncologist recommended radiation, chemotherapy, thali-
domide, and a stem cell transplant. Te doctor also told Jim, We cant
save your life; we can only prolong it. You have from a few months to a
few years to live.
Understandably, Jim was not happy with his prognosis. He had already
looked into coral calcium for another condition hed had, so he knew
about the importance of alkalizing the body. However, he also knew that
taking the coral calcium had never been enough to keep his pH in the
optimal range unless he took about nine capsules a day. He found out
about cesium high pH therapy and was told that, as opposed to some of
the old powdered forms of minerals, liquid ionic minerals do not build
up to a toxic level in the body. Jim worked with someone who knew a
lot about liquid ionic minerals, and he started the therapy using liquid
ionic cesium and liquid ionic potassium. Te only conventional treatment
he did was one week of radiation right after his diagnosis. According to
Jim, when he turned down all conventional treatment and started on the
liquid minerals, it was much to the dismay of his oncologist.
266 oursxair \oui caxcii
Jim took the liquid ionic cesium and potassium three times a day.
Besides the cesium and potassium, his protocol included a variety of
other minerals in liquid ionic form such as germanium, sodium, silver,
zinc, boron, and iron. He also supplemented with coral calcium, vitamin
D, and a few other vitamins and enzymes. Before Jim was diagnosed, he
drank only a glass or two of water each week, a lot of soda and coee,
and rarely ate fresh fruits or vegetables. When he started cesium high
pH therapy, he cut out all soda and coee and drank lots of good water
instead. He avoided sugar and rened carbohydrates, and reduced his
intake of red meat while eating more sh and chicken. He also greatly
increased his intake of fresh fruit and vegetables and started juicing mostly
green vegetables.
Unbelievably, just 24 hours after starting on the cesium, Jims severe
neck pain was completely gone. About four days into his program, he felt
that he was already detoxifying dead cancer cells out his body. Some of
his detoxing symptoms included a tired, weak feeling, loose stools, night
sweats, and increased urination. But the symptoms were mild and not
even as bad as u symptoms.
Jim had started cesium high pH therapy in January 2003. Just two
months later, he went back to his oncologist to be tested again. A blood
test this time showed his IGG count to be down to I,520 (from 5,720),
which was actually in the normal range for a healthy person. His oncolo-
gist told Jim he was blown away by the test results. Jim told his doctor
all the things he had done. Te doctor said, Well, I dont know why its
working, but keep doing it.
About a year after his cancer diagnosis of incurable multiple myeloma,
Jim was back to living a normal life and his scans no longer revealed
any cancer! He continued to take the liquid minerals and to maintain a
healthy diet to keep the cancer from coming back.
Over the year that Jim was recovering through the use of cesium high
pH therapy, he only experienced minor aches and pains, which he attri-
butes to his bones rebuilding. He also felt a slight tingling in his neck
and hips at times in the places where his tumors were, and he sometimes
experienced a slight numbness in his lips and nose for about 20 minutes
after taking the cesium. But all of these symptoms were easy to go through
and simply a part of his healing process.
Jim says that, because he was going against the conventional establish-
ment, he had to have faith that he was doing the right thing by following
the alternative approach that he chose. He credits his ability to stay with
267 Cesium High pH Therapy
the approach to his belief that God was guiding him and putting him in
touch with the right method that could help him to fully heal!
Case Story #3Non-Hodgkins Lymphoma of the Stomach
LaVaughn had been a welder for an oil company for many years and
breathing a variety of toxic substances on the job may have had some-
thing to do with the cancer he was diagnosed with in April 2002, at age
47. Before consulting a doctor, LaVaughn had started having excruciating
pain in his stomach and was sometimes throwing up blood. LaVaughn
and his wife, Cindy, thought he probably had a bleeding ulcer.
When his condition worsened, LaVaughn went to a doctor. Nothing
abnormal showed up on the CT scan or the MRI, so an endoscope pro-
cedure was performed. With the endoscope, LaVaughns doctor could
visually see a huge tumor in his stomach. Right in the middle of the
tumor mass was a bleeding ulcerated area about the size of a silver dollar.
A sample of tissue was biopsied, and the diagnosis came back non-Hodg-
kins lymphoma of the stomach. It was considered to be of a medium
to aggressive variety.
LaVaughns doctors did not want to try to surgically remove the tumor
because it involved too many large blood vessels and there was too high
a risk that LaVaughn would bleed to death. He started himself on nutri-
tional therapy immediately and began juicing and taking some herbs to
strengthen and support his body. He felt better right away, as the pain left
and his energy returned. However, the tumor continued to grow until it
blocked the lower stomach. LaVaughn was now no longer able to eat and
had to be put on intravenous feeding. His doctors started him on chemo
in June, thinking that might cause the tumor to shrink enough so he
could begin eating again. He knew that if he could eat again, he would
then become more aggressive with the nutritional therapy.
Unfortunately, the chemo was not eective and on October I, 2002,
another endoscope procedure showed that the tumor was bigger than
ever. It had been ve weeks since the last chemo treatment, and LaVaughn
was too weak to undergo any more chemo at this point. He was in ter-
rible pain and had not been able to keep any food or drink down for I6
weeks. His oncologist suggested to LaVaughn that the only option was
to surgically remove his entire stomach, then have his intestines attached
to his esophagus.
LaVaughn did not want to undergo stomach removal surgery. Cindy
268 oursxair \oui caxcii
had been searching for alternative options throughout his battle and nally
found out about liquid ionic cesium and potassium. On September 29,
2002, just before the endoscope procedure, she had started LaVaughn
on cesium high pH therapy. He was extremely weak and lethargic at this
point, and his duodenum was completely blocked. Since nothing was
going through his stomach, Cindy decided to spray the liquid minerals
on his skin and let them absorb into his body that way. She sprayed the
liquid cesium on his chest and back and sprayed the liquid potassium and
some of the other minerals on his arms and legs. She did this four times a
day for two days. By the end of these two days, LaVaughns stomach had
started gurgling and his vomiting had stopped. On the third day, Cindy
was able to start carefully giving the liquid minerals to LaVaughn orally
in juice, along with spraying them on him. It seemed like, each day after
that, his stomach was able to handle more and more food and drink, and
he gradually gained his strength back.
LaVaughns treatment was focused around using liquid ionic cesium
and liquid ionic potassium, as well as other liquid ionic minerals. After
a while, Cindy also started him on Dr. Kelleys enzymes, Essiac tea, and
a variety of other supplements. But he never stopped taking the liquid
ionic cesium, potassium, and other minerals.
Incredibly, about six weeks after beginning cesium high pH therapy,
LaVaughn felt well again. Two weeks after that, at the eight-week point,
another endoscope procedure was done. It was the day before Tanksgiving,
2002. Tis time, the endoscope showed that the tumor was completely
gone and the central ulcer part had shrunk down to the size of a pencil
eraser. A biopsy accompanied the scoping, and the resulting pathology
report stated that the cancer was now benign and no helicobacter pylori
bacteria were present.
LaVaughn has not had any more endoscope procedures done, but he
has continued to take the liquid ionic minerals and has continued to feel
great. In fact, he now says he feels I5 years younger than he did before
his diagnosis. In October 2003, he had a general physical and his doctor
could not nd anything wrong with him or any signs of cancer. Even the
hernias that had developed because of the chemo were gone.
LaVaughns treatment approach involved a three-to-one ratio of potas-
sium to cesium at rst. But he eventually switched to an even higher
ratio of potassium to cesium to be sure he did not suer any potassium
deciency. Although not everyone does this, LaVaughn also decided to
follow the practice of taking the cesium for ve days, then skipping it
269 Cesium High pH Therapy
for two days every week. During the two days of not taking the cesium,
however, LaVaughn would still take all his other minerals, including the
potassium.
LaVaughn and Cindy believe that when a person is on cesium high pH
therapy and starts to experience numbness or tingling in the mouth and
nose, or a general disoriented, dizzy, or shaky feeling, its an indication of
low potassium. Tey believe that using the cesium ve days on, two days
o helps to avoid potassium deciency and also gives the body time to
detoxify or ush out the dead cancer cells. Tis may be a helpful dosing
tip to others, though some people may decide not to incorporate the two
days o per week until their cancer has been signicantly reduced.
As of February 2004, LaVaughn is still feeling great, and as far as
anyone can tell, is completely cancer-free. His wife, Cindy, is now a
distributor of liquid minerals, and her contact information is listed at
the end of this chapter.
Case Story #4Non-Hodgkins Lymphoma, Grade III
Cheddy is the nickname for a woman who was also diagnosed with
a form of non-Hodgkins lymphoma. Her diagnosis came in Febru-
ary 2002, when she was 70 years old. Cheddy had gone to her doctor
because of a lump on her arm that had appeared and was about the size
of a nickel. Te lump was removed and biopsied. Te resulting diagno-
sis was non-Hodgkins lymphoma, grade II. Cheddy was immediately
referred to an oncologist who did more scans and tested her bone marrow
to see if her cancer had metastasized. Luckily, these tests indicated that
the cancer in her lymph system had not metastasized to other parts of
her body. She was advised to have a small amount of radiation done on
her arm for one month, which she did. After this, her doctor pronounced
her clear of cancer.
Just three days later, however, the cancer reared its ugly head again
as three new lumps appeared on her neck. Needle biopsies proved these
to be the lymphoma, and it was obvious that the radiation had not fully
gotten rid of Cheddys cancer. Her oncologist wanted her to do che-
motherapy. But Cheddy did not want to do chemo and told her doctor
that she wanted to look into a nutritional approach instead. Her doctor
gruy replied, I dont know anything about nutrition, and I dont want
to know anything about it.
Cheddy pursued nutritional support on her own for about a year. She
270 oursxair \oui caxcii
made major changes in her diet and took lots of supplements including
liver capsules, CoQ, and garlic. Troughout the year, her approach
seemed to be successful at keeping the cancer stable, but wasnt making
it go away. She still had tumors on her neck and one inside her throat.
In mid-March 2003, Cheddy found out about liquid ionic cesium
and potassium and started taking those. She also took other minerals
in liquid ionic form, including germanium, trace minerals and selenium,
plus an immune support supplement. After about six months of doing
this, Cheddys lumps started going down, so she patiently kept doing her
program. Her persistence paid o as she saw the tumors go away, and
she says she experienced very little in the way of side eects. She had no
nausea, no numbness or tingling in the mouth or nose, was simply a little
more tired initially, and had bowel movements that were a little looser.
By September 2003, all the lumps on her neck and in her throat were
completely gone and she had no indication of cancer whatsoever. As of
February 2004, she continues to feel great and show no further signs of
cancer.
Case Story #5Prostate Cancer
At age 56, Gerry was feeling so tired and depressed all the time, that
he was contemplating early retirement. But he knew that if he gave up
his job, he would need to get health insurance coverage from another
source. So he decided to see if he could get medical coverage from a
VA hospital. Te application for coverage required a thorough medical
exam. Gerry was checked for polyps and given an ultrasound to check
his prostate gland. Unfortunately, the ultrasound showed a mass on his
prostate, and Gerry was tentatively diagnosed with prostate cancer. Tis
was in mid-November of 2002. About a month later, a needle-biopsy
was performed on the tumor and Gerrys cancer was ocially veried
and classied as 7 on the Gleason scale. (However, even though Gerry
denitely had prostate cancer, his PSA count was only 0.9, which shows
that not all prostate cancer will cause a high PSA score. See Chapter 20
for more information on this issue.)
Gerrys oncologist suggested that they perform surgery to remove his
entire prostate gland and to also remove any surrounding lymph nodes
during the surgery, if it appeared necessary. But just about everyone in
Gerrys family had died of cancer after going through conventional treat-
ment, so he was extremely reluctant to go through it himself. Instead,
271 Cesium High pH Therapy
Gerry declined surgery and searched for alternative options. He found
out about liquid ionic cesium and potassium and started taking those
in January of 2003. When he told his oncologist about cesium high pH
therapy, the doctor was appalled and actually mailed Gerry a letter urg-
ing him not to do it. In the letter, the doctor warned, You are making
a big mistake.
But Gerry was steadfast in his decision to decline conventional treat-
ment. Along with the liquid ionic cesium and potassium that he began
to take, he also took other liquid ionic minerals, including calcium, mag-
nesium, germanium, sulfur, and vanadium. Plus, he used a rebounder,
which is a mini-trampoline that can be used for mild exercise indoors, and
he started walking a lot outdoors. Gerry radically improved his diet and
cut his bread and sugar intake to almost zero. He also bought a magnetic
mattress pad for his bed.
About four months later, Gerry went back for another ultrasound, and
this time no tumor showed up at all. As far as diagnostic tests were con-
cerned, no cancer could be found. Gerry continued to eat well, exercise,
and take liquid ionic minerals. After about six months, he was able to cut
back on the amounts of the liquid minerals, continuing them at lower
dosages. Gerry would have liked to continue to get ultrasounds and PSA
tests to monitor his progress, but his doctors refused to do these tests on
him anymore. Tey seemed to believe Gerry still had cancer and that more
ultrasounds or PSA tests would not change their minds about this.
Gerry now realizes that the extreme tiredness and depression that
had made him want to retire from his job early had been partly due to
the cancer. About a month or two into his cesium high pH therapy, he
began to feel a lot of energy and felt the depression go away. Now, at the
beginning of 2004, he has so much energy that he jogs between 6 and 9
miles every day and is scheduled to run in this years New York Marathon.
He thinks his positive attitude and diet changes were very important to
his healing, but he credits the bulk of his recovery to cesium high pH
therapy and liquid ionic minerals.
Case Story #6Ovarian Cancer
Sixty-one-year-old Merille (pronounced Marilee) had not been feeling
well for some time when she went to her doctor in January 2002. A CT
scan showed uid in her lungs, and since one of the causes of this could
be cancer, she was referred to a specialist at the Mayo Clinic. More tests
272 oursxair \oui caxcii
at the Mayo Clinic revealed tumors on both of Merilles ovaries as well as
in her lymph system. A blood test for the ovarian cancer marker CA-I25
showed her to have a count of almost 800. (Te normal, healthy range
for the CA-I25 is a count of around 34 or less.)
Merille was rushed into surgery to have her uterus and ovaries removed.
After the surgery, biopsies were done on the tumors and the diagnosis
came back ovarian cancer, stage IIIC. At this point, Merilles oncolo-
gist recommended chemotherapy for the cancer in her lymph system, but
told her there was no cure for her type of cancer. Te implication was
that conventional medicine would only be able to manage her cancer for
a while, but they would not be able to cure it and she would eventually
die from it. Merille did not know of any other option but to go with her
doctors recommendation, so she followed her surgery with six rounds
of chemotherapy.
When the chemotherapy was completed, Merilles CA-I25 had gone
down to a count of 9 and she was pronounced in remission. But as often
happens soon after chemotherapy, her count immediately started going
back up. By March 2003, her CA-I25 was up to 84 and her cancer
was obviously still there and growing. Merille now had new tumors
in her abdomen and also in her neck area around her collar bone. Her
Mayo Clinic oncologist pronounced that the chemo had failed. At this
point, the doctors performed more surgery on Merille, but they could
not remove all her cancer. Tey recommended more rounds of chemo,
but at the same time told Merille that there was a signicant risk that
further chemo would damage her heart. Merille was forced to make a
dicult decision and she decided to decline further chemo and to look
into alternatives instead.
Merilles daughter found out about cesium high pH therapy and Merille
was able to contact an experienced consultant and start on liquid ionic
cesium and liquid ionic potassium immediately. She also began to take
other supportive liquid minerals and supplements. Within three months,
all her tumors disappeared and her cancer marker test had gone from 84
down to 23. Now her CA-I25 was back in the normal range. Merilles
doctor at the Mayo Clinic was amazed and wondered what she was doing.
When she told him, he just said, Keep doing what youre doing!
Merille reduced her dosage of liquid minerals at this point, but her
next CA-I25 test three months later showed her marker results to be
up another I0 points. So she went back on the full dose of cesium and
other minerals and her marker numbers began to go back down again.
273 Cesium High pH Therapy
By January 2004, her CA-I25 marker was all the way down to I2, and
she had no clinical signs of cancer at all. Te latest CA-I25 test, taken
in April 2004, was 6.4the lowest it has ever been.
Merille did nothing other than the cesium high pH therapy while
she was recovering from her metastasized ovarian cancer. To ensure that
she stayed free of cancer, she continued to take the liquid minerals and
supportive supplements. Merille says she took the cesium ve days out of
each week, followed by two days o. (During those two days, she con-
tinued the liquid ionic potassium and other supplements, though.) She
took potassium four times a day and cesium twice a day with the overall
ratio of potassium to cesium being ve to one so that she could be sure
to avoid potassium deciency.
Merille also says that she felt very good during her treatment, with only
mild detoxing symptoms and sporadic diarrhea. And she only experienced
a little tingling and numbness around the nose and mouth at times. All
in all, it was a truly easy and miraculous recovery!
Variations on Dosing
It appears that dierent practitioners or consultants suggest dierent
dosing amounts. According to Dr. Brewer, the most common cesium
dosing that Dr. Nieper and Dr. Sartori used on their cancer patients was
2 grams of cesium chloride three times a day after eating for a total of
6 grams of cesium each day. Along with the cesium, 5 to I0 grams of
vitamin C and I00,000 units of vitamin A, along with 50 to I00 mg of
zinc were also administered to each patient.
It is also known that Dr. Sartori signicantly increased the amount
of cesium he gave to some of his extremely late-stage cancer patients
particularly those who only had been given two weeks to live. In some
cases, Sartori administered up to 27 grams of cesium per day. Te most
common cesium dosing he administered, however, was from 6 to 9 grams
daily, divided into three equal doses each day, given intravenously. Dr. Sar-
tori also intravenously administered high doses of vitamin A, vitamin C,
zinc, selenium, and Laetrile to his patients, but it was not clear how much
potassium was given. Dr. Brewer also thought that the use of Laetrile
could reduce problems with diarrhea in some patients.
But of course Dr. Sartori and other physicians Dr. Brewer consulted
with were using the powdered form of cesium. Some people believe that
the liquid ionic form, which was used in the case stories of this chapter,
274 oursxair \oui caxcii
is actually more eective and easier for the body to assimilate as well as
process out. Even so, various sources recommend variations on dosing.
Dr. Jim Howenstine regularly recommended a I:I ratio using 3 grams
per day of cesium and 3 grams of potassium divided into 2 equal doses
of I grams each twice a day. (He did not recommend taking the 2
days o from the cesium each week, but simply suggested taking a few
days to a week o if strong symptoms of potassium deciency occurred.)
Olga in Case Story #I also used a I:I ratio, but only 2 grams of cesium
and potassium each day. LaVaughn in Case Story #3, on the other hand,
started with a 3:I ratio of potassium to cesium, then increased to a 5:I
ratio later on.
Te tricky thing about trying to gure out dosing ratios is that some
people will compare grams to grams, while others may compare the num-
ber of tablespoons or ounces of the liquid they use. Tis is a problem since
the number of grams of liquid cesium in a tablespoon may be dierent
than the number of grams of liquid potassium in a tablespoon. Tus, for
clarity, it is best to only compare the number of grams of cesium used
per day to the number of grams of potassium used per day. Most liquid
ionic cesium products provide I grams of cesium per tablespoon, and
a common way of dosing is one tablespoon of the liquid cesium in the
morning and one tablespoon in the evening. Tat comes to a total of 3
grams per day. But the number of grams of potassium per tablespoon may
be dierent. So, comparing grams to grams to understand your dosage
ratio is important.
Also, at least one liquid ionic product provides both cesium and potas-
sium in the same liquid. Tis type of product can work out well and be
easier for some people, but the downside is that the ratio of potassium to
cesium cannot be altered when needed. So, those who are trying a com-
bination cesium/potassium product for the rst time may want to have
some extra liquid ionic potassium on hand in case they feel they need
more potassium at any point.
Dr. Brewer also wrote that, while dealing with active tumors, a person
should never take less than 3 grams of cesium per day.
0
His reasoning for
this was that several physicians observed that the administration of 0.5
grams per day (half a gram) will actually enhance the growth of the can-
cer. According to Brewer, Tis is to be expected, since this low amount
is sucient only to raise the cell pH into the high mitosis range. He
felt, however, that clinical ndings proved a quantity of 3 grams or more
per day to be eective against cancer. On the other hand, it is fairly well
275 Cesium High pH Therapy
accepted that once a cancer patient is in remission (no more tumors or
diagnostic evidence of cancer) then a daily dose of half a gram of cesium
per day can be used as a maintenance amount.
Brewer also stated, Te material comprising the tumors is secreted as
uric acid in the urine; the uric acid content of the urine increases many
fold. Tus, people testing their urine pH may nd it more acidic as
their tumors are breaking down. Measuring the uric acid content in urine
might also be an area for future research as a way to measure how much
cancer breakdown is occurring.
Unfortunately, the FDA is making it more and more dicult for
companies to sell cesium. And cesium distributors cannot legally give
out advice for using cesium to treat cancer. Tey can only legally give out
advice for using cesium to alkalize the body and support overall health.
(NOTE: If you come across a cesium distributor advertizing that
cesium does not kill cancer, keep in mind they are probably saying that
to avoid being shut down by the FDA/FTC for claiming cesium as a
cancer treatment.)
Many people obtain their cesium, potassium, and other liquid miner-
als from www.essense-of-life.com. It may be that the use of some other
liquid minerals, such as germanium and selenium, can aid in the success
of cesium high pH therapy and, as Dr. Brewer hypothesized, it may be
that B also can aid in the success of cesium high pH therapy.
It is very dicult to nd practitioners who administer cesium intra-
venously these days. However, one clinic in Reno, Nevada, is currently
providing intravenous cesium for cancer patients who are able to attend
their clinic for the rst 3 weeks of their treatment. Ten, they give them
supervision on self-administering the cesium and potassium at home until
the patients body becomes saturated. (See Reno Integrative Medical
Center in the Resources section at the end of this chapter.)
Te Reno Integrative Medical Center has a long and successful his-
tory of treating cancer through alternative methods and they have many
modalities at their disposal. For instance, Mistletoe, B and DMSO are
also given intravenously along with the cesium. Potassium blood levels are
monitored and German New Medicine is oered as well for resolving any
possible emotional roots of the cancer. Tis clinic is highly recommended
and worth looking into for anyone interested in cesium who wants to be
supervised by a physician.
Te real-life experiences of people who have used cesium high pH
therapy show that, when administered correctly, it is safe and non-toxic.
276 oursxair \oui caxcii
But like other alternative, non-toxic approaches, it is not approved by the
FDA as a cancer treatment. Tus, it cannot be legally prescribed by most
physicians. Also, distributors of cesium are not legally allowed to advise
people of its use as a cancer treatment. However, they can advise people
as to how to use cesium and other minerals for raising ones pH levels.
For those people who choose to use cesium high pH therapy, seeking
the guidance of a qualied practitioner or consultant to nd out how to
use it safely and eectively is advised. Taking precautions to not become
potassium decient is the only serious concern and because of that, it is
always advised to get regular blood tests to check your potassium blood
serum levels. If you have any type of heart condition, you should be under
a doctors supervision while using cesium.
As long as one is getting adequate guidance, this is an easy and extremely
eective approach to self-administer at home. Overall, it is certainly one
of the most impressive approaches for outsmarting cancer available
today.
Resources:
Distributors of Liquid Ionic Cesium and Potassium:
(888) 336-4972. Knowledgeable distributors of liquid ionic minerals
and other supplements. Ask for Cindy, or email Cindy at: Lcyordy@
swbell.net
(800) 642-9670. www.rainbowminerals.net (Distributor of liquid
ionic minerals.)
Cost of self-administered cesium high pH therapy: Tis varies, depending
on how many other liquid minerals or supportive supplements are used
along with the cesium and potassium. Te cost ranges from approximately
$200 per month for just cesium and potassium, to up to about $650
per month when a variety of other minerals and supplements are added.
For cost of intravenous treatments or guidance by a medical professional,
contact that clinic or practitioner.
277 Cesium High pH Therapy
For Intravenous Cesium Treatment:
Reno Integrative Medical Center (775) 829-1009
6110 Plumas, Suite B www.renointegrative.com
Reno, NV 89509
Books
Kathleen Deoul. Cancer Cover-Up. Baltimore: Cassandra Books, 2001.
H. E. Sartori, M.D. Cancer Orwellian or Utopian? Life Science Universal
Inc., 1985.
Booklets Written by Dr. A. Keith Brewer (available from the Brewer
Library listed below):
High pH Cancer Terapy with Cesium
Cancer: Its Nature and a Proposed Treatment
A. Keith Brewer International Science Library (608) 647-6513
325 N. Central Avenue
Richland Center, WI 53581
Websites
www.mwt.net/~drbrewer/brew_art.htm
www.cancer-coverup.com
www.essense-of-life.com
www.advancedhealthplan.com/2cesiumchlorideforcancer2.html
www.thewolfeclinic.com/cesium.html
http://cesium.alternative.cancer.cure.googlepages.com/home
279
I7
Ten More Treatment Options
T
his chapter highlights ten more excellent options for treating cancer
that are safe and non-toxic. Tough discussed more briey than pre-
vious approaches in this book, that does not mean they are less eective.
In fact, for some people, one of the methods presented here could be their
best option for a complete cureor, when used adjunctively with another
compatible approach, may help to bring about recovery. Tey are:
I. Poly-MVA Liquid Formulation
2. Te CAAT Protocol Controlled Amino Acid Terapy
3. LifeOne Formula Liquid Formulation
4. German New Medicine New Paradigm for Cancer
5. Low Dose Naltrexone Non-Toxic Pill by Prescription
6. Lapacho/Pau D'Arco/Taheebo Rainforest Herb in Tea or Capsules
7. N-Tense Graviola-Based Herbs in Capsules
8. Mexican Cancer Clinics Multiple Combined Approaches
9. German Cancer Clinics Multiple Combined Approaches
I0. Ellagic Acid Compound from Red Raspberries
280 oursxair \oui caxcii
I. POLYMVA
Tough it only became available to the public in the late I990s, Poly-
MVA has quickly become one of the more widely used alternative cancer
treatments in the U.S. today. Unlike some of the more obscure alternative
methods, Poly-MVA has ample information in print and on the Inter-
net about it, and many medical practitioners are recommending it. Like
Protocel
.)
Ellagic acid is yet another great cancer-ghting compound that is rela-
tively inexpensive and easy to take. Anyone dealing with cancer should
know about it, whether they are using alternative or conventional treat-
ment methods.
Websites
www.RaspberryGold.com
For pure ellagic acid products and bulk powder (928) 758-3091
www.HopeforCancer.com
For Ellagic Insurance Formula (866) 294-1119
(Also can order from www.GreenwoodHealth.com)
Section Tree
Key Cancer Recovery Issues
315
I8
To Alkalize or Not to Alkalize
I
f you have cancer, you will probably hear from many sources that you
should try to alkalize your body. Tis is because it is known that cancer
cells thrive best in acidic environments. It is also known that, in general,
cancer patients are much more acidic than non-cancer patientseven to
the point of being I,000 times more acidic.
Do cancer patients start out with more acidic bodies in the rst place?
Often they doespecially when cancer develops in adults. When can-
cer develops in children, however, this is often not the case. I have come
across cases of brain tumors, for instance, that occurred in children with
perfectly optimal pH and I suspect that many other pediatric cancers, as
well as many adult cancers, also occur under perfect pH conditions. Tus,
acidic bodies are not the only cause of cancer, but simply one of many
possible triggers (as in the forest re analogy.)
In general, though, it is widely thought that overly acidic body tissues
are prone to developing cancer. Ten, once a person has cancer, the body
may become even more skewed toward the acidic end of the scale due to
the cancer cells themselves producing lactic acidand this allows the
cancer cells to thrive in their own little acidic environment which they
have created.
Of course, the reason that overly acidic bodies are good environments
for cancer is because acidic tissues carry less oxygen than optimally
alkaline tissues (the extracellular and intracellular uids of tissues, to be
316 oursxair \oui caxcii
more exact), and cancer prefers to be in low oxygen environments. In this
chapter, well look at what the acid/alkaline balance is, talk about how
to alkalize the body, and clarify some common misconceptions about
alkalizing and cancer.
Cells and Homeostasis
Most of us could go our whole lives without wondering how our
extracellular and intracellular uids are doing. Normally, we shouldnt
have to worry about them because these uids are usually well-main-
tained by the body through a process called homeostasis. But if we
want to understand cancer, we have to get down to the cellular level
and understand what our cells need and want from their immediate
environment. To do this, it helps to look at how multicellular organ-
isms developed in the rst place and Id like to present the scientic
evolutionary viewpoint on this. (If this does not agree with your own
belief system about how life developed on earth, remember that this is
just a theory. It does, however, give us one way of understanding cells
that seems to make sense.)
From a scientic evolutionary viewpoint, life on Earth rst evolved
in the primordial waters of our planet, which became our oceans. Tis
ocean environment was perfect for fragile, single-celled organisms to
develop in because it was constant in temperature, pressure, and nutrient
availability. Living in the ocean was like being in a womb for these early
single cells. Chaotic characteristics of the dry land environment, such as
weather uctuations, landslides, earthquakes, oods, and so forth, were
not felt in the ocean womb. Tus, in this ideal environment, single-celled
organisms thrived, and the entire surface area of each cell could happily
interact with the outside watery environment to allow food in from the
ocean as well as to expel waste back out into the ocean.
Being in such a good situation, these early single-celled forms of life
evolved and progressed into more complex life forms. Tey eventually
became multicellular organisms. But amassing more than a few cells
together risked cutting some cells o from their watery environment which
each cell desperately needed to survive. In essence, multicellular organ-
isms solved this problem by developing an inner uid environment for all
the cells to interact withan inner ocean, so-to-speak, that they could
carry around with them. In fact, this inner ocean probably mimicked the
317 To Alkalize or Not to Alkalize
original pH, osmotic pressure, ionizing capabilities, mineral composition,
and other features of the outside ocean of primordial days.
Since those primordial days, some of the characteristics of Earths
oceans have changed. Evaporation, erosion of land into the water, and
climate changes causing large portions of water to be frozen into polar ice
caps, have all contributed to the oceans of today being saltier than they
used to be when single-celled organisms were evolving. But the original
inner ocean that multicellular organisms developed is still a part of our
physiology today and still allows each individual cell to gain its nourish-
ment from and excrete its wastes into the uid around it. It is called the
extracellular uid of our bodies. Our cells depend on it to survive. Tis
uid is maintained by the body at constant conditions through a process
called homeostasis. Homeostasis is carried out in other ways as well. Six
overall examples of homeostasis in the body are:
I. Keeping the body temperature constantly around 98.6F
2. Keeping blood acidity/alkalinity levels constant
3. Keeping certain chemical concentrations in body uids constant
4. Keeping the glucose level of the blood constant
5. Keeping the levels of oxygen and carbon dioxide constant
6. Keeping the volume of blood and body uids constant
From the evolutionary viewpoint, all of the above processes of homeo-
stasis could be said to be the bodys way of mimicking the constant condi-
tions of earths primordial waters wherein life rst developed.
Te Bodys Acid/Alkaline Balancing Act
Of course, all of the above constant conditions are important to the
functioning of a healthy body. But many believe that the acid/alkaline
balance of the extracellular uids is of particular importance to whether
or not normal cells turn into cancer cells, as well as to whether cancer
cells, once established, rage out of control.
Te body has a variety of ways that it maintains proper pH levels, but
the primary way that it does this is through the use of minerals from the
diet. Contrary to what some people might believe, it is not the acidity
318 oursxair \oui caxcii
or alkalinity of the foods we eat that keeps us in balance. In fact, it is a
common misconception that eating or drinking something acidic will
make the body acidicand that eating or drinking something alkaline
will make the body alkaline.
In reality, whether a food is acidic or alkaline before it goes into our
bodies is not necessarily an indication of whether it will make us more
acidic or alkaline once that food (or drink) is digested. For example, cit-
rus fruits such as limes and lemons are very acidic outside the body, but
they promote alkalinity when they are broken down and digested inside
the body. Tis is because certain minerals, such as calcium, magnesium,
potassium and iron, among others, are very alkalizing to the bodys inner
environment and many fruits and vegetables (including limes and lemons)
tend to be high in these alkalizing minerals. Tus, the digestion of fruits
and vegetables tends to have an overall alkalizing eect on the body, even
though some of them may be quite acidic before we ingest them. Another
example is apple cider vinegar, which is extremely acidic in itself but aids
in alkalizing the body once digested.
What a food breaks down into when digested, or how a food aids
digestion or the assimilation of nutrients are key factors when it comes
to inuencing body pH. Terefore, it is best to forget about whether a
food is acidic or alkaline itself, and instead, look at which foods are acid-
forming or alkaline-forming in the body.
Unfortunately, typical dietary habits in the modern industrialized world
generally include high quantities of rened and processed foods. Tese
foods tend to be robbed of their natural minerals, vitamins, and enzymes.
Very rened foods, such as white sugar and white our, are so severely
stripped of their mineral content, they are virtually all acid-forming in the
body. In contrast to rened sugars, raw fruits (which are also very sweet
due to their fructose content) contain such an abundance of alkalizing
minerals that the total fruit is alkaline-forming in the body.
Also, when people no longer had to work hard to hunt down their
meat and could buy it instead from a grocery store or fast-food restau-
rant, the consumption of meat became easier and more frequent. Animal
foods such as meat, sh, poultry, and eggs are acid-forming in the body,
primarily because of the extremely acidic byproducts that are produced
during digestion. Tese byproducts, such as sulfuric acid, phosphoric acid,
and uric acid, tend to overwhelm the alkalizing eects of the minerals
contained in these foods.
319 To Alkalize or Not to Alkalize
A brief look at some common acid-forming and alkaline-forming foods
and beverages can give us a quick understanding of how a persons acid/
alkaline balance can get skewed to the acidic end of the scale over many
years of modern eating habits. Te current tendency toward acidity as a
result of diet is then compounded by the fact that chronic stress also con-
tributes to acidity in the body, as do many prescription medications.
Lists of acid-forming versus alkaline-forming foods may vary slightly
from source to source, but most foods and beverages are commonly listed
in the following way:
Acid-Forming Food
all meats most nuts and seeds
sh peanut butter
poultry lentils
eggs most legumes
margarine soft drinks
most commercial cheese coee
pasteurized milk commercial teas
most processed grains most alcoholic beverages
pastas ice cream
crackers chocolate and cocoa
noodles tobacco
rened sugar NutraSweet, Equal, SweetN Low
pastries and candies most prescription drugs
Alkaline-Forming Food
most raw vegetables olive oil
most ripe, raw fruits goat cheese
sprouts raw milk
sprouted whole grains honey
wheatgrass molasses
sauerkraut maple syrup
apple cider vinegar stevia
algaes and sea vegetables spices
miso herbs and herbal teas
soy sauce green tea
320 oursxair \oui caxcii
Almost Neutral (slightly alkaline-forming)
soured dairy products (yogurt)
butter
almonds
buckwheat
millet
Optimally, peoples diets should be made up of approximately three-
quarters alkaline-forming foods, and approximately one-quarter acid-
forming foods to maintain a healthy pH balance. Yet, looking at the
above lists, it is clear that most Americans ingest way too many acid-
forming foods and beverages, and not nearly enough alkaline-forming
foods and beverages. Just think about how many people eat sugary cereal
or rened wheat toast with coee and maybe eggs for breakfast, a meat
sandwich with rened wheat bread and a soda for lunch (maybe along
with a little salad). Ten, for dinner, there is often a main course of meat,
sh, or pasta, possibly followed by a sugary dessert. Not to mention the
common extra cup of coee or soda in the afternoon with a candy bar
as a pick-me-up!
In general, understanding which foods tend to be acid-forming and
which tend to be alkaline-forming is important. But these types of lists
can only give us a partial understanding of how the acid/alkaline balance
in the body can become skewed. For instance, if a deciency of certain
key nutrients builds up over time, then some important alkalizing fea-
tures in the body may not be able to do their job no matter how many
alkalizing foods you ingest. A good example of this is illuminated by the
research of Dr. Johanna Budwig and her axseed oil and cottage cheese
approach (see Chapter I3). Her ndings showed that people who become
severely decient in omega-3 and omega-6 essential fatty acids (EFAs) can
develop low oxygen cellular environments because their cell membranes
cannot attract as much oxygen when they dont have enough of these
vital, electron-rich EFAs. In other words, sh for instance, is considered
acid-forming in general, but prolonged dietary intake of certain kinds
of sh that are high in essential fatty acids and vitamin D may promote
alkalinity in the body over time.
Tus, another common misconception is that people should only eat
alkaline-forming foods. Tere are important health benets to some of
the acid-forming foods, too. If not careful, those who eat only alkaline-
forming foods and cut out all animal products may suer from a deciency
321 To Alkalize or Not to Alkalize
of complete proteins, essential fatty acids, or iron. So, when it comes to
diet, moderation and balance are often the key and optimum health may
result from a diet made up of about 75 percent alkaline-forming foods
and 25 percent acid-forming foods.
Of course, diet is not the only contributor to over-acidity in our bod-
ies. Chronic stress, caeine, and dehydration (which are all rampant in
modern living) also contribute. Stress triggers the sympathetic nervous
system, which increases cellular metabolism, which in turn increases
acidity. Also, chronic dehydration is an increasingly common problem
of modern living where people are rushing around between work, tak-
ing the kids to school, talking on the cell phone, making dinner, etc.,
while keeping themselves going with caeinated drinks that are diuretics.
Chronic dehydration can promote acidity in the body in various ways
and certain toxins in our bodies can too. One easy way to help maintain
a good acid/alkaline balance is to drink plenty of good clean water every
day. Tis reduces dehydration and ushes out toxins.
A Detailed Look at pH, Oxygen and the Heart
So why is it that an overly acid environment in the body is also a low
oxygen environment? Te answer to this question is somewhat detailed
on a biochemistry level, but basically it is because all acidic conditions
consist of excess hydrogen ions. In the absence of sucient minerals to
neutralize this acidity, the body must combine these excess hydrogen ions
with any oxygen that is available, thereby creating water as a harmless
byproduct. Tus, if a person is continually creating an acidic inner envi-
ronment and they dont have enough alkalizing minerals in reserve from
their diet, then their body is constantly having to neutralize their overly
acidic state by depleting the bodys oxygen. However, if there are enough
alkalizing minerals available for the body to use rst, such as calcium,
magnesium, or potassium, then it is not necessary for the oxygen of the
body to be used up in order to neutralize the excess hydrogen ions.
According to Robert Barefoot and Carl J. Reich, M.D., authors of
Te Calcium Factor: Te Scientic Secret of Health and Youth, calcium is
the most important of all the alkalizing minerals we assimilate from our
diets. Tey claim that calcium to acid is like water to a re,
and well
be talking about calcium shortly.
A body pH of 7 is considered neutral on a scale of 0 to I4. Te more
you go down the scale from 7 (toward 0), the more acidic you are. Te
322 oursxair \oui caxcii
more you go up the scale from 7 (toward I4), the more alkaline you are.
Our bodies like to be slightly alkaline to function optimally. All of our
cells and enzymes function best in slightly alkaline environments.
Te pH level of our blood, however, is the most important for our bodies
to maintain and the blood is always kept at a constant level of about 7.4.
Tis is partly because it is critical that the blood be able to maintain suf-
cient oxygen in order to circulate oxygen to all of our cells. If the blood
becomes too acidic, the heart might relax to the point where it could cease
to beat. If the blood becomes too alkaline, on the other hand, the heart
might contract to the point where it could also cease to beat. Tus, the
blood pH has to be given priority over pH anywhere else in the body if
the person is to survive.
Tere are numerous ways that our bodies maintain a virtually con-
stant blood pH of about 7.4. (It literally must be maintained at the very
narrow pH range of 7.35 to 7.45.) If necessary, the pH of the rest of the
body will be sacriced so that the pH of the blood can be maintained
at this critical level. Our bodies do this by using up reserves of alkalizing
minerals from other parts of the body. Tese alkalizing minerals may come
from body tissues such as the bones, teeth, cartilage, muscles, kidneys,
and liver, among other places. Tus, a persons tissues and extra-cellular
uids can become way too acidic for good health throughout many areas
of the body, even though the blood remains at a constant optimum alka-
line/acid balance.
Te constant optimum pH level of the blood, along with the constant
optimum oxygen level of the blood, may be why cancer of the heart is
virtually unknown. Tis is helped by the fact that blood owing into the
heart comes directly from the lungs and has the highest pH and oxygen
levels of any blood within the body.
But all of our bodies cells are highly sensitive to proper pH levels of
the uid environment around them, and they will not function well if
this environment becomes overly acidic. Robert Barefoot and Dr. Carl
Reich explain the above concepts in the following passage from their
book Te Calcium Factor:
In chemistry, alkali solutions (pH over 7.0) tend to absorb oxygen,
while acids (pH under 7.0) tend to expel oxygen. For example, a mild
alkali can absorb over I00 times as much oxygen as a mild acid. Tere-
fore, when the body becomes acidic by dropping below pH 7.0 (note:
all body uids, except for stomach and urine, are supposed to be mildly
alkaline at pH 7.4), oxygen is driven out of the body thereby, according
323 To Alkalize or Not to Alkalize
to Nobel Prize winner Otto Warburg, inducing cancer. Stomach uids
must remain acidic to digest food and urine must remain acidic to remove
wastes from the body. Blood is the exception. Blood must always remain
at an alkaline pH 7.4 so that it can retain its oxygen. When adequate
mineral consumption is in the diet, the blood is supplied the crucial
minerals required to maintain an alkaline pH of 7.4. However when
insucient mineral consumption is in the diet, the body is forced to rob
Peter (other body uids) to pay Paul (the blood). In doing so, it removes
crucial minerals, such as calcium, from the saliva, spinal uids, kidneys,
liver, etc., in order to maintain the blood at pH 7.4. Tis causes the de-
mineralized uids and organs to become acidic and therefore anaerobic,
thus inducing not only cancer, but a host of other degenerative diseases,
such as heart disease, diabetes, arthritis, lupus, etc.
As mentioned above, there are certain systems of the body that have
dierent acid/alkaline ranges. Here is an overview of all the bodys pH
ranges:
Common pH Ranges
Blood 7.357.45
Saliva 6.507.50
Urine 4.508.40
Liver bile 7.108.50
Stomach uids 1.003.50
Over-Acidity and Cancer
Te Nobel Prize winner, Dr. Otto Warburg, believed that cancer cells
are normal cells which have been forced to adapt to a low oxygen envi-
ronment in order to survive. Could it be that, by switching to anaerobic
functioning, these normal cells are simply remembering how they
once functioned in the primordial oceans when they were single-celled
organisms? Tis might be the case since, according to current scientic
theory, all the cells that existed at that time were living in a largely anaero-
bic environment.
We dont generally think about this, but oxygen did not become preva-
lent in the earths atmosphere until after plants evolved. So, all single-
celled life before plants had to function anaerobically. It may be that every
cell in our body retains the ability (a memory, if you will) to function
anaerobically if it needs to in order to survive. Tis concept is supported
324 oursxair \oui caxcii
by the fact that normal healthy muscle cells frequently revert to anaerobic
functioning under adverse conditions. In other words, when we exercise so
strenuously that the supply of oxygen to our muscles is not sucient for
normal functioning, then our muscle cells switch to anaerobic functioning.
Tis involves utilizing glucose for energy, instead of oxygen, and it results
in the production of lactic acidjust as with cancer cells. It is largely this
production of lactic acid in the muscles that causes muscle soreness after
strenuous exercise. Luckily, muscle cells have the capacity to switch back
to normal aerobic functioning once the strenuous exercize has stopped
and oxygen delivery to the muscle cells has been restored. (Cancer cells,
on the other hand, are generally damaged cells that no longer have the
capacity to switch back to aerobic functioning.)
Another problem that over-acidity may cause is related to the fact
that enzymes of the body do not function well in acidic environments.
Tus, some of the bodys best defenses against cancer are neutralized.
And yet another problem may be related to micro-organisms. Tere are
some researchers who believe that, when the pH balance of the body is
skewed, certain harmless micro-organisms can then change form, become
pathogenic and thrive. We saw in the chapters on Royal Rife and Gaston
Naessens that some micro-organisms can change form and become cancer-
causing micro-organisms when conditions are unhealthy in the body.
It is interesting to note that how fast-growing or slow-growing a tumor
is may be directly related to the rate at which it uses anaerobic function-
ing. Some cancer cells rely more on anaerobic functioning than others.
Decades ago, two researchers at the National Cancer Institute performed
some experiments where they actually measured the fermentation rate
of dierent cancers known to grow at dierent speeds. What they found
was that the more aggressive (fast-growing) a cancer was, the higher its
glucose fermentation rate was, and that the slower-growing a cancer was,
the lower its fermentation rate was.
Tough over-acidity is not the only cause of cancer, it is generally
accepted that a poor acid/alkaline balance can contribute to the develop-
ment of the disease and that maintaining optimum alkalinity can go a
long way toward helping a person avoid a cancer diagnosis. For people who
already have cancer, alkalizing the body through diet and supplements
may help slow down cancer growth and help the rest of the body function
better as well, but it should not be relied upon as a curative measure.
325 To Alkalize or Not to Alkalize
Alkalizing Minerals
An understanding of the health benets of alkalizing minerals, and in
particular of calcium, was rst developed by Carl Reich, M.D. Dr. Reich
was a medical maverick who, in the early I950s, suspected that most of
the diseases of his patients could be related to overly acidic bodies and
calcium deciency. In fact, Reich worked together with the Nobel Prize
winner, Otto Warburg, for many years to formulate an understanding
of the role of ionic calcium and cancer.
Dr. Reich started his medical practice in I950 in Calgary, Canada.
When he suspected calcium deciency in his patients, he began to experi-
ment with prescribing several times the RDA of calcium to his patients
along with magnesium and vitamin D which helped the assimilation of
the calcium. Reich was immediately rewarded with a high percentage of
his patients (who were suering from a variety of chronic degenerative
diseases) getting better. By the I980s, Dr. Reich had cured thousands of
suering patients. He did not specialize in cancer, so most of his patients
received treatment for conditions such as asthma, arthritis, colitis, der-
matitis, rheumatism, migraine, fatigue, and depression. But his ndings
on calcium deciency applied to cancer as well.
In the early I970s, Dr. Reich discovered that the pH level of saliva is
an outstanding indicator of ionic calcium levels in the body. And he was
able to validate clinically that a simple three-second test of the saliva using
litmus paper strips could indicate whether a person was functionally de-
cient in calcium or not. He found that the pH of saliva for healthy people
is generally 7.07.5. On the other hand, when a person was decient in
ionic calcium, he found their saliva pH would be around 4.66.4 (much
more acidic). Reich was able to prove that a few weeks to a few months
of supplementation, along with dietary changes, would produce a gradual
increase in saliva alkalinity and a corresponding increase in wellness.
For anyone wanting to nd out what their own pH level is and whether
they are overly acidic or not, pH strip testing is easy to do. Saliva strips are
inexpensive and generally available in health food stores as well as from a
number of sites on the Internet. Strips usually come with a color-coded
chart. According to Barefoot and Reich, a healthy person with sucient
alkalinity and ionic calcium levels will generally show a result of dark
green to blue on the pH strip. (Remember to give at least I5 seconds
for the color to develop.) Most children test blue. But over 50 percent
of adults are green-yellow, indicating a pH of 6.5 or lower and calcium
326 oursxair \oui caxcii
deciency. Amazingly, according to Barefoot and Reich, terminal cancer
patients are usually a bright yellow, a pH of 4.5. Tis is more than I,000
times the acidity level of a normal healthy individual at pH 7.5, causing
the body to self-digest.
Te Importance of Vitamin D
Dr. Reich also reasoned that the minimum daily requirements of vita-
mins and minerals were way too low and he was the rst doctor in North
America to prescribe mega doses of vitamin and mineral supplements.
He gured out that a big factor behind why so many people showed signs
of calcium deciency was not having enough vitamin D in their bod-
ies. Even though calcium is one of the most important bioelements, it is
also one of the more dicult elements for the body to assimilate. Tis is
because, once calcium has been fully dissolved in the stomach, its absorp-
tion into the body is completely dependent on adequate levels of vitamin
D in the intestinal tract. No matter how much dietary calcium a person
ingests, without adequate vitamin D to aid in its absorption, most of this
calcium will just pass through the body. Dr. Reich made the important
discovery that many people who had enough calcium in their diets were
actually not assimilating the calcium they were ingesting due to insuf-
cient levels of vitamin D.
Unfortunately, vitamin D is quite rare in most foods. Te only com-
mon food source with signicant amounts of vitamin D is sh (and sh
oils). Possibly one of the richest food sources of vitamin D is eel, a delicacy
found in many sushi bars. A less common food source with signicant
amounts of vitamin D is Shiitake mushrooms, which may account for
some of this type of mushrooms healing action. But, in general, food
sources of vitamin D are rare. Luckily, Mother Nature has made up for
this by providing our bodies with the ability to manufacture vitamin D at
the surface of our skin when exposed to sunlight. Tis sunlight-induced
vitamin D then gets relayed to our intestinal tracts. If the vitamin D
receptors of the small intestine are saturated, a persons body can increase
its absorption of calcium by a factor of 20.
0
Vitamin D deciency could be considered yet another nutritional
deciency of modern living because, before modern times, humans spent
much more of their time outdoors exposed to sunlight. If they lived in
cold climates, such as in the northern latitudes, and couldnt be exposed
to a lot of sunlight, then they tended to subsist on large amounts of sh.
327 To Alkalize or Not to Alkalize
(Mainly because very cold climates do not support agriculture or even
sucient game hunting.) In the old days, when people lived in warm cli-
mates, they generally had minimal clothing covering their skin and spent
many hours every day exposed to sunlight while they did their hunting,
gathering, farming, preparing of tools, and so forth.
Nowadays, many people spend most of their time indoors in articial
lighting, which does not provide the spectrum of light needed to produce
vitamin D. And when people today are outdoors, they often have clothing
covering most of their skin. For people wearing loincloths and spending
most of their time outdoors, their bodies could produce between I mil-
lion and 3 million IUs of vitamin D every day. Tis is quite a contrast
to the ridiculously low recommended daily allowance (RDA) of vitamin
D which is 400 IUs. To put this RDA amount in perspective, 400 IUs
can easily be produced on the average persons skin surface in less than
I8 seconds if that persons body is in full exposure to sunlight!
So, cal-
cium is critical for maintaining optimum pH in the body, and vitamin
D is critical for assimilating calcium.
In Te Calcium Factor, Dr. Reich and Robert Barefoot make the fol-
lowing points:
No mineral is involved in as many biological functions in the body as
calcium.
Calcium is the key biological workhorse that brings nutrients into
all of our cells (helping to nourish all the cells of the body).
None of calciums jobs is more important than its role in helping to
maintain proper pH levels in the body.
One problem that can occur if the intracellular and extracellular
uids are too acid is that cell walls can begin to disintegrate. When
this happens, toxins and carcinogens are able to get inside the cell
and possibly bind with the DNAs nucleotides. Some of these toxins
and carcinogens can then cause the DNA to mutate with a result of
cancer.
In a sense, Dr. Reich actually considered cancer to be tailor made to
survive and to thrive in an ionic calcium decient environment.
It is interesting to look at the diet and lifestyles of the longest-lived and
healthiest people in the world, because doing so supports the importance of
328 oursxair \oui caxcii
a high assimilation of ionic calcium. For instance, the Hunzas in Pakistan;
the Armenians, Azerbaijanians, and Georgians in Russia; the Vilcabamba
Indians in Ecuador; the Titicacas Indians in Peru; the Bamas in China;
and the Tibetans are all mountain-residing people who drink highly min-
eralized water from glaciers. Tis water is so full of minerals, including
high levels of calcium, that it is milky color and is called milk of the
mountains. According to Barefoot and Reich, these long-lived people may
ingest on any given day I00,000 milligrams of calcium. Te Okinawans
are another group of people who are incredibly healthy and long-lived and
though they live at sea level, they do just as well by drinking water full
of coral calcium. Tis is a result of dissolved coral reefs and the water is
also milky white in color and called milk of the oceans.
All of the above groups of people are virtually disease-free and are not
limited to our required daily amounts, or RDAs, of minerals. In fact,
they consume about 70 times the RDA of calcium, 22 times the RDA
of magnesium, and I8 times the RDA of potassium, to name just a few
of their abundant dietary nutrients. All of these minerals are highly
alkalizing to the body and are therefore preventive to disease.
Barefoot and Reich suggest that a change in diet alone can, over time,
bring a persons body back into correct pH balance. But if a person has
cancer, they suggest that the person will want to bring about their pH re-
balancing as quickly as possibleand that requires high doses of certain
supplements. Calcium, magnesium, and vitamin D are very important for
regaining pH balance, and in particular, many people nd that supple-
menting with a coral calcium product helps immensely. Of the various
coral calcium products on the market today, the marine harvested and
high-grade versions are probably the best. Vitamin D is added to coral
calcium products, but people who are starting out acidic should also
either get a lot of skin exposure to sunshine every day or supplement
with extra vitamin D.
Alkalizing Once You Have Cancer
Reich and Barefoot made it clear in their book that cancer cannot
survive in an optimally alkaline environment. Tough this is true, it
has also sparked a common misunderstanding that can be dangerous
to the cancer patient. What has been proven scientically is that cancer
cells in articial environments, such as petri dishes, cannot survive if the
329 To Alkalize or Not to Alkalize
environment is alkaline enough. Tis has caused many people to assume
that if they are able to raise their body pH to the point where saliva test-
ing shows it to be in the optimally alkaline range (a pH of 7.07.5), then
all the cancer in their body will necessarily die o.
What people dont take into account is that active tumors within the
body are very dierent from a small number of microscopic cells in a petri
dish. Since a tumor is made up of millions of cancer cells, all thriving
and producing energy for themselves through the anaerobic respiration
process called glycolysis, the environment immediately around the tumor
will generally become quite acidic as a result of glycolysis producing lactic
acid as a byproduct. Tus, the area immediately surrounding the tumor
may remain acidic even when the rest of the body is optimally alkaline!
So, it is critical that people do not think that all they need to do is bring
their alkalinity up to get rid of their cancer. (Te exception to this rule
is Cesium High pH Terapy as described in Chapter I6. Cesium is not
an everyday supplement and not sold at most health food stores. It is
also only a trace mineral in our foods. While normal alkalizing supple-
ments like calcium, magnesium, potassium, and vitamin D alkalize the
extracellular environment of the body, Cesium High pH Terapy is a
specic treatment method that is capable of alkalizing the intracellular
environment of cancer cells. In other words, cesium is readily absorbed
into cancer cells, where it then alkalizes them to death from the inside.)
Having said that, it does appear that bringing ones general body pH up
to a healthy slightly alkaline level should be able to help slow the growth
of cancer and improve the bodys functioning and overall health. To this
end, many cancer patients take signicant doses of calcium, magnesium
and vitamin D. In general, it is best to consult with your physician, nutri-
tionist, or alternative cancer specialist about how to alkalize your body
when you have cancer. Tis is to ensure that the alkalizing supplements
and/or diet changes you choose are compatible with your cancer treat-
ment approach and support your optimum recovery.
Also, it is important to understand that many alternative treatments
for cancer have historically worked without the person alkalizing his or
her body at the same time. Two very powerful approaches that come
to mind, for instance, which dont require alkalizing are Protocel
and
Dr. Burzynskis Antineoplaston Terapy.
330 oursxair \oui caxcii
Resources:
Books
Robert R. Barefoot and Carl J. Reich, M.D. Te Calcium Factor: Te
Scientic Secret of Health and Youth. Wickenburg, Arizona: Deonna
Enterprises Publishing, 2001. (Can be ordered from Exxel Audio by
calling: 800-443-9935.)
Herman Aihara. Acid and Alkaline. Oroville, California: George Ohsawa
Macrobiotic Foundation, 1986.
Websites
www.superior-coral.com (also can call 877-287-3263)
www.healthtreasures.com
www.cureamerica.net
www.hopeforcancer.com/OxyPlus.htm (Also contains information about
Warburgs Oxygen Boosting and alkalizing formula, Oxy Plus.)
www.alkalizeforhealth.net
www.cocoonnutrition.org
www.gethealthyagain.com
331
I9
What Women Must Know
About Hormones
T
here can be many contributing factors to the development of cancer.
But one particularly important factor for women is hormone imbal-
ance. Many important hormones in our bodies work together and, when
in balance, contribute to our overall health and well-being. Some of these
important hormones are thyroid, DHEA, testosterone and cortisol. How-
ever, for women with cancer, the most important hormones to monitor
closely are estrogen and progesterone, and those are the hormones we will
be focusing on in this chapter.
Estrogen, Progesterone, and Hormone Imbalance
Generally, hormone imbalance in women occurs when there is too
much estrogen and too little progesterone in their bodies. In our discus-
sion of womens hormones and cancer, two concepts need to be clari-
ed up front. Te rst concept is that estrogen is really a group name
because every woman actually makes three dierent estrogen hormones
in her body. Tese three types of estrogen are called: estradiol, estrone,
and estriol. Whenever hormones are discussed, these three versions of
estrogen tend to be collectively referred to as estrogen.
Te second concept is that, in discussing hormone imbalance, it is the
332 oursxair \oui caxcii
natural estrogen and natural progesterone to which I am referring. So, if
you are a woman and thinking something like, Well, I am getting my
hormones balanced right now because I am on hormone replacement
therapy, then you may need to think again. Te hormones provided in
conventional hormone replacement therapy, such as those in Premarin
and Provera, are not natural in the sense that they are not bioidentical to
the hormones we produce in our bodies. Tus, they do not rectify hormone
imbalance in the body. Actually, most hormone replacement therapies
prescribed by conventional doctors involve non-bioidentical hormones and
the hormones in birth control pills are also non-bioidentical. Te func-
tional dierences between bioidentical and non-bioidentical hormones
will be discussed soon, but remember, it is only the bioidentical forms of
hormones that can bring about true hormone balance in a woman.
All hormones perform very important physiological functions. In
doing so, hormones can be so powerful that nature has created checks and
balances for them. Te way that our bodies naturally keep the estrogen
levels in check, for instance, is by producing the hormone progesterone to
oppose the estrogens. Te opposing eects of progesterone keep the eects
of the estrogens in balance, and this balance is necessary if a womans
body is to function normally and stay healthy. If a healthy balance is not
maintained, and a woman has too much estrogen and too little proges-
terone functioning in her body over a signicant period of time, then
she is prone to many serious health problems. Tese health problems can
even be life-threatening, and include stroke, heart attack, osteoporosis
(or brittle bones), and yes, even cancer. Te types of cancer in women
that are most frequently caused by an estrogen/progesterone imbalance
are the cancers of the sex organs. Tus, these tend to be breast cancer,
endometrial (uterine) cancer, and ovarian cancer. But other cancers can
result, in part, from hormone imbalance as well.
Estrogen/progesterone imbalances can also play a role in the develop-
ment of cancer for men. Te type of cancer most frequently caused by
this type of hormone imbalance in men is prostate cancer. But there are
reasons why an imbalance between estrogen and progesterone can often
be a much bigger cancer factor for women than for men. One reason is
that a womans natural life cycle includes big changes in her hormone
levels during her mid-life years, before and during her transition into
menopause, that can throw her into imbalance.
In general, a womans progesterone production will begin to decrease
I0 to I5 years before menopause begins, then will continue to drop even
333 What Women Must Know About Hormones
lower for several years afterward. Her estrogen levels, on the other hand,
will not decrease much during her premenopausal years. Just before
menopause her estrogen levels will, however, become more variable, with
up and down surges. It is not until a woman is actually experiencing
menopause and no longer having menstrual cycles that her estrogen levels
have nally decreased a signicant amount. Tus, hormone imbalance
in women occurs partly because, during the pre-menopause phase, their
estrogen and progesterone levels do not drop equally.
Tis gap between estrogen and progesterone is then widened even
more by environmental and dietary factors that contribute to increases in a
womans estrogenic activity. (Tese other factors will be discussed in more
detail when we look at the causes of estrogen dominance.) Women in the
modern western world suer from these added environmental and dietary
factors the most. Tis is why they tend to suer more from menopausal
symptoms than many women in third world or Asian countries.
Another major reason women are much more likely than men to suer
serious hormone imbalance is that they are so often recipients of some form
of prescribed, synthetic hormones. Tese synthetic hormones are most
often in the form of: (I) birth control pills, or (2) hormone replacement
therapy (HRT). HRT is usually prescribed for symptoms of menopause,
including the frequently occurring surgically induced menopause that
is a result of hysterectomy. Tese two sources of prescribed hormones can
cause many women to actually spend decades of their lives on a hormone
regimen that can cause a very unhealthy imbalance in their bodies. And
many of them are not told, and are thus not aware, that this imbalance
can signicantly increase their chance of developing cancer and other
life-threatening conditions.
Estrogen Dominance
When women develop an imbalance between estrogen and progesterone,
it is almost always the estrogen levels that are too high and the proges-
terone levels that are too low. It very rarely happens the other way. John
R. Lee, M.D., spent many years researching and writing books about the
dangers of hormone imbalances in modern women. In discussing what
causes these imbalances, Dr. Lee coined the term estrogen dominance.
Estrogen dominance refers to the ratio of estrogen to progesterone. In
other words, before, during and after menopause, a woman may suer
from various menopause symptoms as a result of her estrogen levels being
334 oursxair \oui caxcii
low. Tese symptoms of low estrogen might be hot ashes, depression,
foggy thinking, dry skin, vaginal dryness, low sex drive, and insomnia.
But even with low estrogen levels, she may still be estrogen dominant.
Tis is because her progesterone level most likely is even lower than her
estrogen, and the ratio of estrogen to progesterone in her body is still
imbalanced in the direction of too much estrogen.
Breast cancer, which is one of the second leading causes of cancer death
among women, is linked to this type of hormone imbalance. Luckily,
the good news is that the correction of hormone imbalance can not only
help to prevent cancer in women, especially breast cancer, but may also
improve a womans chances of recovery from cancer.
To understand how estrogen dominance contributes to cancer, we
must rst understand estrogen and progesterone a little better. Te estro-
gens perform many functions in our bodies. But for women, one of the
most important functions of the estrogens could be described in this
simplied way: Te estrogens prepare a woman for reproduction. (Te
word estrogen was coined originally when researchers rst discovered
its estrus-producing capabilities.) In other words, the estrogens bring
on menses in teenage girls (or stimulate the proliferation of endometrial
cells in preparation for pregnancy), and they stimulate the development of
breast tissue in young women to prepare them for breast-feeding. Both of
these important functions involve the stimulation of new cell growth.
On the other hand, one of the most important functions of progesterone
in women could be described in this simplied way: Progesterone protects
pregnancy once pregnancy has been initiated. (Te word progesterone
was coined originally to mean pro-gestation.) In other words, there are
many health benets to the body that progesterone provides throughout
the life of every woman, but it has a particularly important job during
pregnancy. During pregnancy, a womans progesterone production shoots
sky high. Tis high level of progesterone in her body then protects the
developing fetus by preventing ovulation and the ensuing sloughing o
of the endometrial lining. In fact, women who have low levels of pro-
gesterone will sometimes experience repeated miscarriages because their
bodies are not producing enough natural progesterone to safeguard the
normal process of gestation.
Another thing to keep in mind is that estrogen is dominant in a womans
body throughout the rst week of her menstruation, and progesterone is
the dominant hormone in a womans body right after ovulation and for
the two weeks preceding her menstrual period. When a woman does not
335 What Women Must Know About Hormones
produce enough progesterone she will often experience symptoms of PMS.
Tis is because the progesterone hormone is supposed to be dominant the
two weeks before menstruation, and if there is insucient progesterone
at this time, a woman will feel noticeable symptoms. Tus, many women
have reported great relief from their PMS symptoms after they started
supplementing their bodies with natural progesterone.
So, it is a direct result of women being the child-bearing sex that ini-
tially sets them up for a roller-coaster ride with their hormones. Womens
bodies must be able to switch between two drastically dierent modes
gestation and non-gestationand these dierent modes require dif-
ferent hormones being dominant at dierent times. Men dont have to
switch between these dierent modes, and so their hormone balance is
easier for their bodies to maintain. But normally, this roller-coaster ride
should not be too dicult. Womens bodies have evolved to handle the
changes in their hormones. It is largely because of modern living that
these changes have resulted in far more out-of-balance states in women
than ever before.
Estrogen Dominance and Cancer
Te cancer risk from estrogen dominance results from the fact that
the estrogens tend to stimulate cell growth. Because of this simple factor,
estrogen dominance puts a woman at serious risk for developing cancer.
And if a woman already has cancer, the state of estrogen dominance can
make it more dicult for her to achieve recovery. Tis cancer-promoting
factor of estrogen is widely accepted by the medical community and is
the reason most doctors will refuse to prescribe estrogen for menopausal
symptoms to a woman who has cancer.
Exactly how does estrogen promote cancerous cell growth? It does
this by activating an oncogene, or cancer-stimulating gene, in cells.
Te cancer-stimulating gene that responds to estrogen is called Bcl-2.
Progesterone, on the other hand, down-regulates this very same Bcl-2
gene, and up-regulates a tumor-suppressor gene in the same cells. Tis
tumor-suppressor gene is called p53. When p53 is activated, it slows
cell reproduction and restores proper programmed cell death. Tis pro-
grammed cell death is called apoptosis (pronounced with the second
p silent), and is an integral function of all normal, healthy cells. Tus,
estrogen tends to stimulate uncontrolled cell growth by activating the
Bcl-2 gene, and progesterone tends to stop uncontrolled cell growth by
336 oursxair \oui caxcii
activating the p53 gene, which slows cellular reproduction and restores
proper programmed cell death.
As we have seen so many times before, nature tends to provide checks
and balances for all physiological processes. As long as a womans estro-
gen and progesterone levels are balanced, she will not experience out-of-
control cell growth. But once her estrogen level is dominant, then the
many dierent eects of her estrogen can go unchecked.
So far, we have been discussing the type of estrogen dominance that
can occur in a womans body with her own natural hormones. But even
more of a cancer risk is when a woman is prescribed estrogen for meno-
pause symptoms and is not prescribed natural progesterone along with it.
Tis is referred to as prescribing unopposed estrogen, and it rarely hap-
pens anymore because doctors are now very aware that they should not
prescribe unopposed estrogen. Te dangers of doing this became all too
clear after mainstream medical doctors had been prescribing unopposed
estrogen for about 20 years to menopausal women and then found out that
a high number of these women were developing endometrial cancer.
But what conventional doctors have not yet fully admitted is that
this practice of prescribing unopposed estrogen for two decades not only
caused uterine cancer, but it also caused many women to develop and
die of breast cancer. In his book, What Your Doctor May Not Tell You
About Breast Cancer, Dr. Lee comments on the rapid rise in breast cancer
during the middle of the twentieth century:
Te probable cause of the rise in breast cancer deaths was the pre-
scription of unopposed estrogen (not balanced with progesterone) to
menopausal women, a common practice from the early I950s to the
mid-I970s. While the medical community acknowledged that this
practice caused endometrial (uterine) cancer, it never admitted that it
also caused breast cancer.
Tus, using prescribed estrogen without also supplementing with natu-
ral progesterone is a huge cancer risk to women. As Dr. Lee stated, this
practice not only can cause fatal breast cancer and uterine cancer, but as
we shall see later on, it can also cause fatal ovarian cancer.
Natural Progesterone and Breast Cancer
Over the last decade, the mainstream medical community has focused
a lot on genetic predisposition factors for breast cancer. Some conventional
337 What Women Must Know About Hormones
doctors are pushing the genetic origins of breast cancer so much that
some women who do not even have cancer are actually deciding to get
preemptive mastectomies just because there is a history of breast cancer
in their family. But according to Dr. Lee and his colleagues, only about
I0 percent of all breast cancer cases in this country can be attributed to
inherited genetic causes. And these genetic causes only predispose some
women to breast cancerthey dont guarantee that cancer will develop.
On the other hand, Dr. Lee believes that something as controllable as
estrogen dominance can be a powerful contributing factor to cancer in
women.
Support for the link between estrogen dominance and breast cancer
comes from a study that was done back in the early I980s by L. D. Cowan
and colleagues at Johns Hopkins University. Tese researchers discovered
that women who had low levels of progesterone in their bodies ended up
having a 540 percent higher incidence of cancer than women who had
good progesterone levels.
An even more interesting study was carried out from I975 to the mid-
I990s (over an I8-year period) in England. Tis study was conducted by
P. E. Mohr, M.D., a British physician, and the results were published in
a I996 issue of the British Journal of Cancer. Dr. Mohr and his colleagues
went to the top three surgical hospitals in London and asked them to
measure a variety of hormone levels in women at the time of breast sur-
gery for all breast cancer patients in those hospitals. Tis was done, and
the results were fascinating. (Incidentally, all of the women in this study
were node-positive cases, meaning their breast cancer had already metasta-
sized.) What Dr. Mohrs study showed was that those women whose breast
cancer surgery was performed in the second half of their menstrual cycle
(which is when their own production of progesterone was at its highest)
were much less likely to have their breast cancer recur later on.
Tis study showed that, of the women who had higher levels of proges-
terone in their bodies at the time of surgery, about 65 percent were still
alive I8 years later. But of those women who had low levels of progesterone
on the day of their surgery, only about 35 percent were still alive I8 years
later. In other words, if you are a woman preparing to undergo breast
cancer surgery, Dr. Lee says, You double your survival rate just by having
your progesterone level satisfactory on the day of your surgery!
Dr. Mohrs study looked at women whose progesterone levels were
high or low on the day of surgery simply due to the part of their men-
strual cycle they were in. Dr. Lee believes that if these women had been
338 oursxair \oui caxcii
supplementing with natural progesterone at ages when their own levels
began to drop, it is possible that they would have done even better. One
of the reasons he believes this is that, since I978, Dr. Lee has put many
of his own female patients on natural progesterone for osteoporosis. In
cases where the woman had a history of cancer, no estrogen was pre-
scribed along with the progesterone because of the cancer stimulating
eects of estrogen. Over the next 20 years, Dr. Lee made a point of
following these women who had a history of cancer that he had put on
natural progesterone. Amazingly, he found that not one of them died of
cancer in those 20 years.
Tus, both the I8-year study done by Dr. Mohr and Dr. Lees own
experience with his female patients showed that supplementing with
therapeutic levels of natural progesterone can signicantly decrease the
likelihood that a woman will have a recurrence of her breast cancer.
Natural Versus Synthetic Hormones
Unfortunately, when the medical community was nally forced to
accept that they could not safely prescribe unopposed estrogen to women,
rather than add natural (bioidentical) progesterone to their prescriptions,
they chose to add synthetic (non-bioidentical) progesterone. Tere are vari-
ous forms of synthetic progesterone, and they are all technically referred
to as progestins. (Te most commonly prescribed progestin today is
Provera.) Most likely, this practice came about because pharmaceutical
companies could not patent and make high prots from selling natural
progesterone, but they could make high prots from selling synthetic pro-
gesterone. Many hormones are synthesized in laboratories, and natural
progesterone is synthesized from various plant sources. However, the end
result is bioidentical to what we make in our bodies, thus the end result
is natural progesterone. Progestins, on the other hand, like Provera, are
called synthetic because they never become bioidentical to what we
make in our bodies.
Because they are not bioidentical, synthetic progestins do not protect
against cancer as natural progesterone does. After years of prescribing
synthetic progestins along with estrogen, the medical community nally
began to see evidence that progestins did not control the cancer risk of
unopposed estrogen. In fact, it made it worse.
Te problem is that doctors do not tend to be aware of the very impor-
tant dierences between synthetic progestins and natural progesterone.
339 What Women Must Know About Hormones
Since they know that estrogen and progestins can contribute to cancer,
doctors often wrongly assume that natural progesterone will contribute
to cancer as well. If you have cancer, and your doctor is leery of supple-
menting you with natural progesterone, keep this in mind: Synthetic
progestins contribute to cancer. Natural progesterone protects against
cancer. It is terribly unfortunate for women that many doctors still do
not understand this functional dierence.
Understanding the structural dierence between natural hormones
and synthetic hormones is simple. In a nutshell, natural hormones are
those hormones that occur naturally in our bodies, or are produced in a
laboratory to have exactly the same biochemical structure as those in our
bodies. Each hormone in our bodies has a specic chemical structure
that is unique to that hormone. For example, there is only one specic
molecule that is estradiol, one specic molecule that is estrone, one spe-
cic molecule that is estriol and one specic molecule that is progesterone.
Because pharmaceutical companies cannot patent and thereby cannot
make exorbitant prots on any natural substance, they prefer to modify
the hormones they sell. Tey do this by changing the natural hormone
molecule in some way so that it is no longer the exact same molecule (or
hormone) that occurs naturally. Ten, they have a substance they can
patent. Whenever a hormone molecule is even one atom dierent from
the natural hormone found in nature, it is referred to as synthetic.
However, natural hormones can also be synthesized in laboratories.
For example, natural progesterone is produced by our bodies, but it can
also be synthesized in a laboratory from plant sources to be completely
bioidentical to the progesterone we make in our bodies. Tese plant
sources tend to be either wild yam extract or soy, and contain diosgenin,
which is similar to our own natural progesterone. In laboratories, dios-
genin can easily be altered just a little bit to become exactly bioidentical
to the progesterone found in our bodies. Tus, in the eld of hormone
research and prescription, the synthesized result is called natural proges-
terone. It is synthesized from something that is natural to plants, and it
only requires a minimal change to turn it into something that is natural
to humans.
One way to look at this terminology is the following: to synthesize
something just means putting something together from parts. But syn-
thetic refers to any substance not found in nature.
As long as the natural progesterone, which is synthesized in laboratories
to put into natural progesterone creams and pills, is exactly bioidentical
340 oursxair \oui caxcii
to the progesterone in our bodies, then it is completely safe and will carry
out all the same functions in our bodies as the progesterone we naturally
produce. Synthetic hormones, on the other hand, are produced to have
almost the same, but not exactly the same, chemical structure as those
hormones that occur naturally in our bodies. Tus, they carry out some
of the same functions in our bodies as our own natural hormones, but
not all of them. Tis is not a good thing for women because all of the
functions of our natural hormones are there for a reason. Also, synthetic
hormones can bind to receptor sites for much longer periods of time
than their corresponding natural hormones would, which means they
can block the action of a womans own natural hormones that her body
may still be producing.
In the case of progesterone, the synthetic forms (called progestins)
denitely do not have many of the protective and benecial eects on
the body as the natural, bioidentical form of progesterone. Progestins do
not provide the protective eects against stroke, heart disease, osteopo-
rosis, and cancer that natural progesterone does. And because they block
a womans own natural progesterone from binding to cell receptor sites,
they actually make estrogen dominance worse. Plus, one of the key ways
that natural progesterone helps to prevent cancer is by activating the p53
gene in cellsthe tumor-suppressor gene that slows cell proliferation and
stimulates normal cell death. However, according to Dr. Lee, most syn-
thetic progestins do not activate the p53 gene. In fact, because progestins
are so dangerous and promote so many serious health risks, Dr. Lee states,
Prescribing a progestin to a menopausal woman should be considered
medical malpractice. Yet, synthetic progestins are the progesterone-like
hormones in all birth control pills as well as in conventional hormone
replacement therapy for menopause!
Te fact that synthetic hormones are not exactly the same in molecu-
lar structure as those hormones naturally found in our bodies turns out
to be a huge distinction. In the world of chemical molecules, changing
just one atom can sometimes turn a molecule into a completely dierent
thingsuch as a completely dierent hormone. Nowhere is the dier-
ence between natural and synthetic hormones so clear as in diagrams of
their chemical structures. For example, here is a graphic representation
of three dierent molecules. Te rst shows the chemical structure of the
hormone testosterone, the second shows the chemical structure of the
hormone progesterone, and the third shows the chemical structure of
the synthetic progestin Provera.
341 What Women Must Know About Hormones
As you can see, the two hormones, testosterone and progesterone, are
extremely similar in chemical structure. Yet, virtually everybody knows
there is a big dierence in how these two hormones function in the body.
Tus, a very small change in chemical structure can produce a large change
in how the molecule functions in the body. Look at the drug Provera. It
is obvious this molecule has quite a few dierences in its chemical struc-
ture from that of natural progesterone. In fact, natural progesterone is
actually more similar in structure to testosterone, a completely dierent
hormone, than it is to Provera, its synthetic counterpart.
Te most common hormone replacement therapy regimen being pre-
scribed to menopausal women today is a combination of the two drugs
Provera and Premarin. Tis is the regimen that is supposed to replace
their insucient levels of progesterone and estrogen. We have already
seen how dierent Provera is from the natural progesterone women need.
Now, lets look at Premarin to see how similar it is to the natural estrogen
women need.
Plain and simple, Premarin is a strange form of estrogen for women
because it is made up of horse hormones. Yes, thats right. Premarin is
synthesized from horse urine taken from pregnant mares. Because horses
are a dierent species and their hormones are thus dierent from ours,
this drug puts estrogen hormones into women that may be natural to
horses but are not natural to humans. Premarin, therefore, is considered
a prescription drug that provides synthetic estrogen for women because
the estrogen is not bioidentical to what human women produce in their
bodies. Moreover, the process of creating the Premarin drug is very cruel
to the horses that are used. Pregnant horses are kept in inhumane condi-
tions so their urine can be used to create this very protable drug. If you
342 oursxair \oui caxcii
have any doubt as to whether this is where the drug Premarin comes from,
just look at the name: Premarin is short for pregnant mares urine. In
technical publications, Premarin is sometimes referred to as conjugated
equine estrogen.
Te point to remember is that all synthetic estrogens and all synthetic
progestins are un-natural hormones. And they all create an imbalanced
situation in a womans body that can contribute to stroke, heart disease,
brittle bones, and cancer. Yet, how many reasons are there for women to
be prescribed synthetic hormones? Here are six common ones:
I. To alleviate menopause symptoms.
2. To supply hormones depleted by hysterectomy.
3. To avoid pregnancy through use of the pill.
4. To treat osteoporosis.
5. To alleviate painful or irregular menstruation.
6. To reduce acne.
Te cruel reality is that, ever since the development of synthetic hor-
mones, modern women have been turning into stroke, heart disease, and
cancer casualties in alarming numbers.
In its January 26, 2000, issue, the Journal of the American Medical
Association published a study that was done on a whopping 46,000 women.
Tis huge study concluded that the most commonly prescribed form of
HRT (Premarin and Provera) produced a 40 percent higher risk of breast
cancer in women who used it for ve years as compared to women not
using conventional HRT. Tis breast cancer risk factor was deemed to
increase by 8 percent for each year of use. So, women on Premarin and
Provera for I0 years could be assumed to have an 80 percent higher risk
of developing breast cancer, women on Premarin and Provera for 20 years
could be assumed to have a I60 percent higher risk, and so forth. Yet, a
combination of Premarin and Provera is still the most common form of
hormone replacement therapy prescribed to women today.
Unfortunately, the truth of the above study has still not completely
reached the public. Tis is partly because, when the above study results
came out, newspapers and other media around the country (such as
medical writers and TV commentators) reported the study inaccurately.
343 What Women Must Know About Hormones
Tey mistakenly used the term progesterone when they were referring
to the synthetic progestins used in the study.
Te same thing happened with an even more recent study that cap-
tured a lot of media attentionthe now famous Womens Health Ini-
tiative (WHI) Study. Tis study followed over I6,000 women and was
originally scheduled to run from I997 to 2005. But it was halted pre-
maturely in 2002 because of the high rate of life-threatening side eects
women receiving the HRT were experiencing. Tis study caused countless
women to give up their hormone replacement therapy. It is important to
understand that bioidentical hormones were not used anywhere in the
above studies. Tey both focused only on the use of Premarin and Pro-
vera. Provera appears to have been the most damaging of the two drugs,
probably because it replaced the use of natural progesterone which has
so many protective eects that progestins dont have.
Tus, it is critical that the public and doctors distinguish between
progesterone and progestins. And it is critical that people realize there
are many results from studies and statistics showing that progesterone in
its natural form carries a protective eect against cancer and other health
problems. For instance, its cancer-protective eect is evidenced by the
fact that the most common age for women to start showing the begin-
ning stages of breast cancer is about ve years before menopause. Tis is
exactly when a womans own progesterone level has dropped dramatically,
yet well before her estrogen levels have fallen.
Te cancer-protective eects of natural progesterone are also evidenced
by the statistic that going through a full-term pregnancy by age 24 can
reduce the risk of breast cancer for a woman by more than half. During
pregnancy, a woman goes through many months where her progesterone
level is extremely high as compared to those times when she is not preg-
nant. Tis high level of progesterone contributes to normal dierentiation
of breast tissue and can have a long-term protective eect against cancer
developing later on in the breasts.
Since birth control pills are made with synthetic progestins, the use of
birth control pills at young ages can contribute to breast cancer as well
as synthetic HRT. Dr. Lee states,
It has been well established that when girls between the ages of I3
and I8and to a lesser but still signicant eect, women up to the age
of 2Iuse birth control pills, their risk of breast cancer can increase by
as much as 60 percent. Te younger a girl begins to use contraceptive
hormones, the greater her risk of breast cancer.
344 oursxair \oui caxcii
Dr. Lee and his colleagues believe that this predisposition to breast
cancer caused by birth control pill usage happens in two ways: (I) the
synthetic progestins in the birth control pills block the benecial and
cancer-protecting activity of a womans natural progesterone; and
(2) because the pill blocks ovulation, it thereby blocks a certain amount
of a womans own supply of natural progesterone from being produced
in the rst place.
It is extremely unfortunate that the medical community has resorted to
using Big Pharma studies such as those mentioned above to warn women
against any use of hormoneseven bioidentical ones. In fact, the mis-
understanding has gone so far as to terrify women if their breast cancer
cells are not only estrogen receptor positive, but also progesterone receptor
positive. Once again, conventional medicine has now adopted the erro-
neous idea that natural progesterone is bad, when the studies that have
been scaring them have only been done on non-bioidentical progestins.
Given that natural progesterone promotes apoptosis and down-regulates
the Bcl-2 gene, it would appear to be a good thing if a womans cancer
cells are progesterone receptor positive. If your doctor tells you there is
no dierence between progesterone and progestins, just show him or her
a picture of how dierent the two molecules look.
Other Causes of Estrogen Dominance
If hormone imbalance only occurred as a result of conventional HRT
or birth control pills, then many women who had never taken either of
these would be able to rest easy. However, this is not the case. Tere are
other causes of hormone imbalance and estrogen dominance in modern
women as well that do not involve prescribed hormones. For those women
who have never undergone prescribed synthetic hormone use, the main
factors contributing to estrogen dominance are: environmental xenoestro-
gens, diets high in rened carbohydrates and low in phytochemicals, and
excess body fat.
Xenoestrogens
Xenoestrogens are petrochemically derived compounds that are
estrogen-like, which most people are exposed to on a regular basis. (Te
x in xenoestrogens is pronounced like a z, as in xylophone.) Te prex
xeno means foreign and indicates that xenoestrogens are not normally
345 What Women Must Know About Hormones
found in nature. Tese unnatural compounds are considered estrogenic
because they produce estrogen activity in our bodies.
We are exposed to xenoestrogens in a variety of ways:
We ingest xenoestrogens from pesticides used on crops whenever we
eat nonorganic supermarket fruits and vegetables.
We absorb xenoestrogens into our bodies through our skin whenever
we come in contact with common lawn and garden sprays, as well as
indoor insect sprays.
We breathe in xenoestrogens from car exhaust and smog.
We drink in xenoestrogens in areas where industrial waste dumps have
contaminated the ground water supply.
We eat xenoestrogens when we ingest eat meat or dairy products from
livestock fed estrogenic drugs to fatten them up.
We are exposed to xenoestrogens through the use of common solvents,
soaps, and plastics.
Xenoestrogens are everywhere. Tey are nonbiodegradable and accu-
mulate in our bodies over time. Because they build up in our bodies and
mimic our own estrogen, they dangerously contribute to the condition
of estrogen dominance. According to Dr. Lee, all xenoestrogens (as well
as other xenohormones) should be considered toxic.
Tere are two main ways that environmental xenoestrogens contrib-
ute to estrogen dominance. Te rst way is that they bind to estrogen
receptors in our bodies and produce an increase in estrogenic activity.
Te second way that xenoestrogens contribute to estrogen dominance in
women is that they can damage a womans egg follicles and cause ovarian
dysfunction. Ovarian dysfunction can then result in the decrease of a
womans own progesterone production. Chronic xenohormone exposure
to adult women can bring about this ovarian dysfunction and result in
reduced progesterone production, but it can happen much earlier, too. It
is now known that exposure to xenohormones as early as during embryo
development can cause this functional loss of ovarian follicles. Tis means
that estrogen dominance for many of us women may be partly caused by
the environmental xenohormones our mothers were exposed to when they
were pregnant with us.
346 oursxair \oui caxcii
It is imperative that the public at large become more aware of the
dangers of xenoestrogens in our environment. Tese dangerous, nonbio-
degradable chemicals are already reducing the populations of many other
species on our planet, and are seriously contributing to reduced fertility
in women and men as well. In general, men in industrialized countries
are already showing greatly reduced sperm counts (compared to their
grandfathers) as a result of these xenohormones. Some researchers believe
that humans may, at some point, become an endangered species because
of the multitude of xenohormones in our environment.
Diet
It is well known that eating lots of fresh fruits and vegetables on a
regular basis can protect against all kinds of cancer. Tis is in large part
due to the cancer-ghting vitamins and minerals, as well as the natural
ber that these healthful foods provide. However, few people know that
diets high in fresh fruits and vegetables also protect against the cancer-
prone condition of estrogen dominance. One of the ways they do this is
by providing our bodies with what are called phytoestrogens.
Phytoestrogens, or plant estrogens, are natural compounds found in
plants that have weak estrogen-like activity in humans. Tey are part
of the larger family of compounds known as phytochemicals, and are
a natural and important part of any healthy diet. Tere are presently
I8 dierent phytochemicals known to be estrogenic in humans. Tese
phytoestrogens bind to estrogen receptors in the body and convey many
of the health benets of human estrogen to men and women alike. And
because they bind to estrogen receptors, they compete with our own
estrogen hormones for the same receptors.
Tis is particularly helpful for women battling estrogen dominance
because the weaker plant estrogens block some of the activity of the excess,
stronger human estrogens. Tey do not cling to the receptors for long
and are easily processed out of the body.
Te seven subgroups of phytoestrogens are: isoavones, coumestans,
avanones, avones, avanols, lignans, and chalcones. Te isoavones
and coumestans are the most powerful of the phytoestrogens, with about
a I0-fold stronger estrogenic eect than the others. Virtually all plants,
including vegetables, fruits, seeds, legumes, and grains, have some form
of phytoestrogen in them. Flavanones are primarily concentrated in citrus
347 What Women Must Know About Hormones
fruits, lignans are found in all fruits, vegetables, and cereals, and the
stronger isoavones and coumestans are mostly found in legumes.
Because of so much processed food in our diets, Americans generally
dont eat as many whole foods as people in other countries do. Tere
are many other populations around the world where a higher percent-
age of the daily diet consists of various forms of whole vegetables, grains,
seeds, legumes and fruits than in the United States. In those populations,
women generally dont have to deal with as much estrogen dominance
because they havent spent a lifetime eating processed and rened foods
virtually devoid of phytochemicals.
Te isoavones are some of the most potent phytoestrogens to humans,
yet, ironically, they are the most lacking in the modern western diet. Tis
is because when most westerners eat a phytochemical-containing plant, it
is usually in the form of a piece of fruit or a salad vegetable. It is not usu-
ally in the form of some type of legume (or bean). Yet, in countries where
women suer the least from symptoms of PMS and menopause, legumes
are part of their staple diet. In the orient, this staple legume tends to be
the soybean, and in Central and South America, this staple tends to be
made up of more than one legume, including chickpeas and lentils.
Te important isoavone category of phytoestrogens can be broken
down into four specic isoavones. Tese are: genistein, biochanin, daid-
zein, and formononetin. Every time we eat a legume, we are consuming at
least one of these four benecial isoavones. A great deal of research has
been done on the eects of isoavones. Besides helping to alleviate the
many uncomfortable symptoms of estrogen dominance, isoavones have
also been shown to have potent anti-cancer properties. Tey ght cancer
in a variety of ways, including by inducing apoptosis (normal cell death)
and inhibiting angiogenesis (new blood vessel growth to cancer cells). In
addition to their direct anti-cancer properties, isoavones are also known
to be diuretics, have anti-inammatory properties, are antioxidants, and
can stimulate the immune system and improve cardiovascular health.
Tus, women who have diets low in fresh fruits, vegetables, and legumes,
are deprived of many of the hormone-balancing nutrients these foods can
supply. Soy products are becoming a more and more common way for
women to naturally treat their health issues, but there is some controversy
around soy as well. Unfermented soy products actually contain some
anti-nutritive agents in them that are somewhat harmful to the body.
Terefore, the healthiest way to get isoavones is by eating fermented soy
348 oursxair \oui caxcii
products, such as miso, tofu, and tempeh, as well as a variety of other
legumes, such as various beans, chickpeas, and lentils.
In this discussion of diet, it is also important to note that the consump-
tion of excess alcohol can contribute to estrogen dominance. Tis is because
estrogen is processed out of our bodies through the liver. If a woman
regularly consumes alcohol, she may be compromising the functioning
of her liver and thereby not be as able to process out the excess estrogen
from her body as well as she should.
0
Excess ingestion of prescription
drugs can also have the same eect on the liver as alcohol. Over time,
the continued excess intake of alcoholic drinks and/or prescription drugs
can compromise the functioning of a persons liver, which compromises
the processing out of excess estrogen and thereby contributes to excess
buildup of estrogen in the body and to estrogen dominance.
Body Fat
Yet another reason women in the modern western world have more
problems with hormone imbalance than others is that they tend to be
more overweight. Easy access to highly processed and fast foods, overly
generous restaurant meal proportions, abundant candy and snacks, and
less than optimum exercise levels have all taken a toll on both men and
women. Little do most women know, however, that fat cells produce estro-
gen. In general, the more fat a woman has, the more estrogen she is likely
to be making in her body, even after menopause. Tese extra fat cells,
each making estrogen, complicate the problem by being storage cells for
xenoestrogens as well. It is no wonder that a largely overweight country
like the United States is also a largely estrogen-dominant country.
So, when it comes to estrogen dominance, there are four main
causes:
I. Synthetic hormones from HRT and birth control pills
2. Xenoestrogens from pesticides and other environmental sources
3. Diets low in phytochemicals and high in rened carbohydrates
4. Excess body fat
For more information on estrogen dominance, and how to correct
female hormone imbalance, I highly recommend any of Dr. John R. Lees
349 What Women Must Know About Hormones
books, videos, and audiotapes. According to Dr. Lee, one of the quickest
and easiest ways to start correcting this imbalance, if you have it, is by
using natural progesterone.
Pesticides and Breast Cancer
In examining direct causes of breast cancer, xenoestrogens and other
toxins from pesticides also need to be looked at closely. Tese dangerous
chemicals may promote a high risk of developing breast cancer in women
for two main reasons. One reason is that toxins from pesticides and
industrial waste tend to be stored in the body in fatty tissues and womens
breast tissue is made up of about one-third fat. As long as these toxins sit
in the fatty tissue, they pose a risk of genetic damage to cells. Moreover,
these and other toxins can accumulate in breast tissue over time, posing a
greater and greater threat to each woman as she grows older. Corporations
that cause pollution often refer to the small amount of toxins that people
are exposed to at any given time as being safe, without ever addressing the
fact that these toxins can accumulate and concentrate in the body and
have a cumulative eect over time. Tis is an example of how science
can be misused and facts can be presented in a misleading way.
If you think that pesticides are safely controlled by laws, you may not
know that many of the pesticide chemicals used today are exempt from
current laws. For instance, in I970 the EPA set certain safe pesticide
limits. But within this legislation, congress allowed the continued use
of all pesticides approved before I970. (Tis is a curious way to enforce
environmental protection regulations.) Similarly, in I978, more accurate
measures of testing pesticides for safety were enacted, but this legisla-
tion once again exempted all pesticides that had been approved prior to
I978.
One of the most telling studies about the relationship between pesti-
cides and breast cancer involved the entire country of Israel. After breast
cancer deaths had been rising in Israel for about 25 years, they dropped
sharply between the years of I976 and I986. Te only apparent reason
was a strict ban of three organochlorine pesticides that had been enacted
in the early I970s. (Tese pesticides were DDT, BHC, and lindane).
Organochlorines are considered to be complete carcinogens, which
means that they both initiate cancer as well as promote cancer once it has
gotten started. Moreover, along with the decrease in breast cancer cases
350 oursxair \oui caxcii
in women after this ban, it was noted that there was also a corresponding
decrease of these pesticides in cows milk and in Israeli womens breast
milk. Breast milk, therefore, is one way that infants can receive concentrated
doses of pesticide xenohormones.
It is important that we, the public, exercise more control over what
pesticides we are exposed to. And it is not just those pesticides that are
used on crops that we must think about, but also those used in public
buildings, on lawns, gardens, and in our own homes.
Breast Cancer Statistics
Te number of women getting breast cancer has been steadily increas-
ing over the past century, and this increase appears to be accelerating.
According to the National Cancer Institute, the incidence of breast cancer
rose by a whopping 40 percent between I973 and I988. Breast cancer is
now the most common cause of death from cancer in women between
the ages of I8 and 54, and the leading cause of death for any reason in
women aged 45 to 50.
It is not easy to come across accurate gures of what the cure rates for
breast cancer through conventional medicine really are. Tis is because
all ocial statistics are based on the denition of cure as being alive
ve years after diagnosis. Keeping a woman with breast cancer alive for
ve years is often achievable through surgery, radiation, and chemother-
apy. But it also often involves the woman going in and out of remission,
feeling frequently ill, being surgically mutilated, and never becoming
cancer-free.
Tis bogus way of dening cure is one of the biggest ways that ocial
statistics are misleading and directly give women false hope.
Tere is another way organized medicine has made ocial breast cancer
cure rates misleading. It is by including something called DCIS in their
breast cancer statistics. DCIS stands for ductal carcinoma in situ, and
is classied as a form of breast cancer within the duct. But many experts
debate whether DCIS should even be classied as a cancer at all. When
a woman is diagnosed with DCIS, it means she has abnormal cells scat-
tered here and there, not clustered together into a tumor, which are con-
tained within the duct and are not penetrating or inltrating the deeper
layer of cells in the breast. Te bottom line is that DCIS is essentially
known to be a benign condition. If the abnormal cells begin to invade the
351 What Women Must Know About Hormones
deeper tissue, then it is no longer considered DCIS. Te critical thing
to understand is that only a very small fraction of DCIS cases go on to
become actual malignant cancer, and therefore DCIS is really more of
a pre-cancerous state.
According to many experts, DCIS is 99 percent curable. Tis makes
it similar to many skin cancers in that it is not generally a life-threatening
condition. But the cancer industry includes this easily curable, mostly
benign condition in their ocial breast cancer cure-rate statistics, and
thereby makes the overall cure rate for all breast cancers look consider-
ably better. Over the past 20 years, DCIS diagnoses have comprised
approximately 30 percent of all breast cancer diagnoses.
Conventional Breast Cancer Treatments
Surgery
For virtually all breast cancer cases, surgery is the primary treatment
used. Following that, radiation, chemotherapy and hormone-blocking
drugs are the treatments of choice. Whether a lumpectomy (removal of the
lump and surrounding tissue) or a mastectomy (removal of the entire breast
and surrounding tissue) is recommended, depends on the type and stage
of the breast cancer. For women whose cancer has not yet metastasized, so
that they only need surgery with no follow-up radiation or chemo, their
chances of long-term recovery are the greatest in conventional medicine.
In fact, Ralph Moss reports in his book Questioning Chemotherapy that
for cases of non-metastasized breast cancer (lymph node-negative), surgery
alone will cause about 90 percent of these cases to not have a recurrence of
the disease. Many women have survived their breast cancer under these
conditions and gone on to live long, normal lives.
But surgery for breast cancer is generally only curative when the can-
cer has not yet metastasized. Once metastasis has occurred to any other
location, including the lymph glands, the surgery may be considered only
palliative, or simply a procedure that is not expected to bring about
long-term cure but merely to buy the patient time.
Unfortunately, when metastasis has occurred and follow-up treatments
after surgery are required, long-term life expectancy drops dramatically
for a woman with breast cancer using conventional approaches. Here are
some comments on those follow-up treatments.
352 oursxair \oui caxcii
Radiation
Te benets of radiation treatment for breast cancer are questionable,
yet radiation is still the most commonly used treatment for breast cancer
after surgery. A recent article in the British medical journal, Te Lancet,
showed that, according to one study, the use of radiation on breast cancer
patients did reduce deaths from breast cancer by I3.2 percent. However,
these same radiation treatments increased deaths from other causes by
2I.2 percent. Tese other cause deaths were largely from heart disease
as a result of the radiation administered right around the heart area. As
Dr. Lee puts it, the only conclusion that can be made from this study on
the use of radiation for breast cancer is that the treatment was a success
but the patient died.
Chemotherapy
After surgery and radiation, chemotherapy is the next most often pre-
scribed treatment for breast cancer. However, it is also debatable as to how
eective this type of treatment for breast cancer is. Ralph Moss reports
that there is literally no evidence that chemotherapy can bring about long-
term survival in cases of breast cancers that have already metastasized.
Yet, over two dozen chemotherapy drugs have been approved for use in
metastasized breast cancer. In these cases, it is apparently hoped that the
chemotherapy treatments may be able to extend the life of the patient
somewhat. Once again, we are looking at a palliative treatment, with
the doctor hoping to buy the patient time but not necessarily expecting
a cure.
As mentioned earlier, surgery alone can prevent recurrence for about
90 percent of the women surgically treated for non-metastasized breast
cancer. Of those I0 percent who do have a recurrence, it has been esti-
mated that only about 3 percent could benet in any long-term way from
chemotherapy. If Ralph Mosss research and the above statistics are
accurate, we must conclude that no patient with metastasized breast can-
cer will benet in a long-term way by the use of chemotherapy, and only
about 3 percent of those patients with very early stage, non-metastasized
breast cancer will benet in a long-term way from chemotherapy.
By the early I980s, the medical community was so discouraged with
their lack of long-term success in treating breast cancer, that they tried
something radical. For a period of about I0 years, from the mid-I980s to
353 What Women Must Know About Hormones
the mid-I990s, a new regimen of extremely high doses of chemotherapy
(about I0 times the normal amount) followed by a bone marrow trans-
plant was tried. For a while, this highly risky combination treatment
was thought by many doctors to be a womans best chance of surviving
advanced breast cancer. Te high-dose chemotherapy was the cancer
treatment. Te bone marrow transplant was the follow-up treatment used
to save the womans life after the chemo had destroyed her bone marrow
and her bodys ability to produce new red blood cells.
Before the mid-I980s, about a hundred of these treatments each year
were performed for breast cancer. By I994, this number had grown con-
siderably with about 4,000 high-dose chemotherapy/bone marrow trans-
plant procedures being performed each year in the United States for breast
cancer. Tis type of combination treatment is truly barbaric. It might not
be out of line to say that it is the most horrendous type of treatment for
any patient to undergo. Te high-dose chemotherapy seriously damages
the intestinal lining from mouth to anus, causing patients to endure great
pain whenever they swallow or defecate. Making this unbearable are the
alternating bouts of nausea, vomiting, and diarrhea the chemo causes. On
top of this, the patient has to undergo extreme loneliness by being kept
in an isolation room for weeks while their bone marrow recovers. Tis
isolation is necessary because their immune system has been so damaged
that they are highly susceptible to infection at this time. Tus, it is too
risky for even their family members to approach them.
In the early years, one out of every ve women died directly from this
treatment. In later years, after the procedure had been perfected consider-
ably, the death rate directly caused by this treatment improved to one
out of every I0 women it was used on. Tose who survived the treatment
often sustained permanent damage to their heart, kidneys, lungs, liver,
and nerves.
Finally, after many years, the medical community realized that the
long-term survival gain for patients who received this type of treatment
for breast cancer was debatable. One revealing article in the August 2002
issue of Discover magazine summed it up as follows:
Most oncologists now agree that high-dose chemotherapy is simply
the wrong treatment for breast cancer. Chemotherapy works by killing
cells when theyre dividing, so the faster cancer cells divide, the harder
theyre hit. Blood cancerssome leukemias and lymphomasgrow
rapidly and so are acutely vulnerable. But breast cancer cells reproduce
more slowly and tend to be far more resistant to cancer drugs. No matter
354 oursxair \oui caxcii
how many breast cancer cells are killed, at least a few survive, and they
keep dividing after the chemotherapy ends.
Te slow pace of most breast cancers also helps explain why trans-
planters were so optimistic. Breast tumors can take years to reappear after
treatment, but the transplanters were used to leukemia, which tends to
come roaring back in a matter of months. If they found no evidence of
breast cancer after a year and a halfthe usual waiting period for blood
cancersthey assumed a patient was cured, or at least in long-term remis-
sion. Yet the cancer was often lurking in the background, gathering its
forces for another, more devastating appearance.
From the moment [Dr.] Peters rst administered high-dose chemo-
therapy until the rst clinical trials were concluded, nearly 20 years
passed. During that time, hundreds of physicians practiced the unproven
treatment. An estimated 30,000 breast cancer patients suered through
high-dose chemotherapy, only a fraction of them as part of a clinical
trial. All told, the nation spent around $3 billion paying for it, while an
estimated 4,000 to 9,000 women died not from their cancer but from
the treatment.
According to the above article, doctors initially talked about high-dose
chemotherapy/bone marrow transplant procedures as the long-sought
cure for breast cancer they had been waiting for. Even many insurance
companies were nally persuaded to pay for this expensive treatment.
But after longer-term studies were concluded, the medical community
was forced to realize that any survival advantage the treatment may have
provided for patients was actually wiped out by the fact that so many
patients died from the treatment itself. One of these long-term studies was
performed by the National Cancer Institute over almost I0 years and the
results were presented to the public in I999. Tis randomized NCI study
only included patients whose breast cancer had not yet metastasized, but
even in these cases of early breast cancer the survival benets of high-
dose chemotherapy followed by bone marrow transplant were negated
by the number of women who died from the treatment. Tus, even for
breast cancer that had been caught early, the high-dose chemotherapy/
bone marrow transplant procedure was deemed ineective.
It seems that if normal doses of chemotherapy had been saving the lives
of women with breast cancer and having worthwhile long-term results,
then the medical community would never have spent so much time and
money on such a risky procedureone where the treatment itself killed
from I0 to 20 percent of the patients it was used on.
355 What Women Must Know About Hormones
Tamoxifen
Tamoxifen is a nonsteroidal, estrogen-blocking drug that has become
the most common conventional treatment for breast cancer after surgery,
radiation, and chemotherapy. Te reasoning behind the use of this drug is
that Tamoxifen is actually a synthetic form of estrogen, but it is a weaker
estrogen than estradiol (every womans strongest natural estrogen in her
body). By binding to the estrogen receptors of the breast, Tamoxifen
blocks a womans own more powerful estrogen from binding to those
same sites and doing their work. Tus, in breast tissue, Tamoxifen is
considered an anti-estrogen.
However, what doctors dont generally tell their female patients is
that Tamoxifen acts as a stronger estrogen in the uterus and is actually
classied as a cancer-causing drug because it can cause endometrial
cancer. Moreover, according to Dr. Lee, the endometrial cancer caused
by Tamoxifen is far more aggressive and more lethal than endometrial
cancer caused by unopposed estradiol.
Te following are ve major downsides to using Tamoxifen:
I. About 20 to 30 percent of all breast cancers are not estrogen-driven,
and therefore are not aected by Tamoxifen at all.
2. Even for estrogen-driven breast cancers, there is evidence that Tamox-
ifen is not eective once the cancer has metastasized to the lymph
nodes.
3. Research has now shown that Tamoxifen does not permanently stop
cancer cells from growing, but rather puts them into a sort of deep
sleep. Once the Tamoxifen is removed from the body and a womans
own estrogen is again allowed access to those receptors, the cancer cells,
if still there, will begin to grow again. For this reason, Tamoxifen is
called a cytostatic drug rather than a cytotoxic one.
4. Tere are many serious side eects that may accompany the use of
Tamoxifen, some of which can be life-threatening. For instance, a
womans risk of developing a potentially fatal blood clot in the lung
is tripled on Tamoxifen, and her risks of suering a stroke, blindness,
and liver dysfunction are also signicantly increased. Less serious
side eects that this drug can induce are hot ashes, night sweats,
depression, nausea, and vomiting.
356 oursxair \oui caxcii
5. As already mentioned, Tamoxifen can actually cause aggressive endo-
metrial cancer in the very women who are taking it to recover from
their breast cancer.
Short-term studies on the use of Tamoxifen for breast cancer in the
United States have made the drug look a lot more successful than the
long-term studies that have been performed in Europe on the same drug.
For instance, Dr. Lee comments,
Te only large U.S. study was cut short, supposedly because the inci-
dence of breast cancer dropped so much in the Tamoxifen group that
they couldnt justify withholding this treatment from the placebo group.
Its worth noting, however, that the trial was stopped at about the same
time that breast cancer began to reappear, despite the Tamoxifen, in the
two European studies.
Tus, it appears that a number of European studies have concluded
there is no long-term life extension gain for women with breast cancer
who use Tamoxifen. One article in the Lancet suggested that the dif-
ferent conclusions from the American versus the European studies may
have resulted from the fact that Tamoxifen only temporarily suppresses
tumors, and that if the American studies had followed the women for a
longer period of time, their conclusions would have been more like the
European conclusions.
0
Yet, despite the fact that European studies showed no long-term life
extension through the use of Tamoxifen, despite the fact that Tamox-
ifen is not eective for lymph-node positive cases of breast cancer, and
despite the life-threatening side eects that may be caused by this drug,
approximately 60 percent of the women with breast cancer in the United
States are being treated with Tamoxifen right now. Surely, if women
were made fully aware of all Tamoxifens drawbacks, there would be a
lot fewer women willing to use it.
Another estrogen-blocking drug currently being considered by the FDA
for use on breast cancer is Raloxifene. It apparently does not tend to
cause uterine cancer the way Tamoxifen does; however, it does also carry
with it some very dangerous side eects. Like Tamoxifen, Raloxifene tends
to cause blood clots in the veins, and if one of these blood clots travels to
the lungs, it can threaten the life of the patient.
357 What Women Must Know About Hormones
It seems odd that most conventional doctors are so willing to prescribe
very expensive, very dangerous, and not very eective estrogen-blocking
drugs to women with breast cancer, yet they so rarely consider prescribing
low-cost, entirely safe natural progesterone. Natural progesterone safely
opposes the eects of estrogen in the body, including normalizing cell
growth, while at the same time providing other great health benets to
the body as well.
Estrogen Dominance and Other Cancers
Earlier, I referred to a study done at Johns Hopkins that showed women
with low progesterone levels (estrogen dominance) to have a 540 percent
greater risk of developing breast cancer. But that same study also showed
that women with low progesterone levels had a I0-fold higher incidence of
all types of cancer compared to women with good progesterone levels. In
other words, women with insucient progesterone carry a I,000 percent
higher risk of developing cancer of any type when compared to women with
good progesterone levels. Tis study clearly indicated that breast cancer is
not the only type of cancer that can result from estrogen dominance.
Evidence has been available for many years that proves the prescription
of unopposed estrogen can cause uterine cancer. Tere is also evidence
that the prescription of unopposed estrogen can cause ovarian cancer.
One large study, done at Emory University, looked at 249,000 women
over a period of seven years to nd out more about which factors might
be linked to fatal ovarian cancer. (Te researchers had to study such a
large group of women in order to be able to have a signicant number of
cases of fatal ovarian cancer naturally occur.) A computer was then used
to analyze and compare common characteristics of those women who
developed fatal ovarian cancer. What it came up with was this: every one
of the women in this very large group who developed fatal ovarian cancer
was on prescribed, unopposed estrogen.
Also, Dr. Lee believes that estrogen dominance may be a contributing
factor to prostate cancer in men. As we have discussed, estrogen domi-
nance is not usually as serious a problem for men as it is for women, but
mens progesterone levels do decline as they get older, and men are also
subjected to many xenoestrogens from the environment which can make
them estrogen dominant. Dr. Lee claims he has also had very good results
supplementing his prostate cancer patients with natural progesterone.
358 oursxair \oui caxcii
Testing for HormonesBlood or Saliva Test?
Lets say you are a woman who wants to know whether or not you
are balanced or imbalanced in your estrogen and progesterone. Most
conventional doctors will have you do a blood test to nd out, and most
alternative doctors will recommend a saliva test. What is the dierence
and which type of test is more accurate?
Te answer to this question is somewhat controversial, but Dr. Lee
makes a very good case for why the saliva test for these particular hormones
is much more accurate and reliable than the blood test. His reasoning is
that saliva testing is much more useful because it measures the amounts
of bioavailable (or free) hormones in the blood, whereas blood testing
measures a lot of bound up hormones that will never be available to
the cells in the body. According to Dr. Lee:
Saliva tests are more useful than blood tests because they measure
the bioavailable (free) hormone in the blood. After steroid hormones
(progesterone, cortisols, estrogens, DHEA, testosterone) are manufac-
tured by the ovaries, adrenal glands, or testes, theyre released into the
bloodstream, where they attach or bind to very specic hormone carrier
proteins and, to a lesser extent, to red blood cells. Progesterone and cor-
tisol bind to cortisol binding globulin (CBG). Te estrogens (estradiol,
estrone, estriol) and testosterone bind to sex hormone binding globulin
(SHBG). All of the steroids also bind to albumin, which is a protein
present in very high concentrations in the blood. For every I00 steroid
molecules bound to these carrier proteins, only about I to 5 percent
escape the binding proteins and make it into the cells during circulation
through the blood. Te small I to 5 percent of steroids that escape the
binding proteins are considered the free or bioavailable hormones, and
these are what you want to measure, because they represent the amount
of hormone that the tissue actually receives and responds to.
Some of the steroids also bind to red blood cells. Te more fat-loving
a steroid hormone is, the more likely it is to hitch a ride on a red blood
cell. Steroids hang on less tightly to red blood cells than they do to car-
rier proteins. Tis means that steroids bound to red blood cells will dis-
sociate more easily and therefore are more bioavailable for use by your
cells. Studies have shown that when red blood cells pass through the
capillaries of tissues, the steroids bound to them can dissociate and enter
tissues within milliseconds.
Te two problems associated with using blood tests to measure estrogen
and progesterone levels are: (I) blood tests measure hormones that are
359 What Women Must Know About Hormones
bound to carrier proteins, only a small percentage of which will be avail-
able for use by the body; and (2) because blood tests generally measure
the serum or plasma of the blood (meaning the blood cells have been
removed), these tests are not able to measure those hormones bound to
the fatty membranes of red blood cells which are largely available to the
body because they tend to dissociate from the blood cells when they pass
through the capillaries.
Progesterone is more likely to bind to red blood cells than other hor-
mones. Dr. Lee refers to the research of one of his colleagues when he
explains:
According to hormone researcher David Zava, Ph.D., progesterone
is by far the most lipophilic, or fat loving, of the steroid hormones. It
circulates in the blood, carried by fat-soluble substances such as red blood
cell membranes. Some 70 to 80 percent of ovary-made progesterone is
carried on red blood cells and thus is not measured by serum or plasma
blood tests. Tis progesterone is available to the body for use and read-
ily lters through the saliva glands into saliva where it can be measured
accurately. Te remaining 20 to 30 percent of progesterone in the body
is protein bound and is found in the watery blood plasma where it can
be measured by serum or plasma blood tests. However, only I to 9 per-
cent of this progesterone is available to the body for use. Tat is why
saliva testing is a far more accurate and relevant test than blood tests in
measuring bioavailable progesterone.
If you consult with a naturopathic or holistic physician who uses saliva
testing, they will generally have a laboratory with which they work. How-
ever, you can order your own saliva tests without a doctors prescription if
youd like to assess your hormone balance yourself. One very competent
laboratory you can contact to do this is:
ZRT Lab, (503) 466-2445, www.salivatest.com
If you live in any state of the United States other than California or
New York, you can order your own saliva test from ZRT Lab without a
doctors prescription. If you live in California, however, you will need a
doctors prescription, and if you live in New York, you will not be able
to order from this lab even with a prescription. You can also access more
detailed information about saliva tests and hormone balancing on ZRTs
website (www.salivatest.com).
360 oursxair \oui caxcii
Cream Versus Oral Progesterone
Once a woman has determined through testing that she needs to
supplement her body with natural progesterone, there are two main ways
she can do this. One way is by using a non-prescription natural proges-
terone cream that is rubbed onto various areas of the body. Another way
is by getting a doctors prescription for pharmaceutically compounded
natural progesterone in pill form and taking it orally.
Both ways can be successful, but evidence indicates that the cream,
or transdermal route, is the most ecient way. Since natural progester-
one is so lipophilic (fat-loving), it is easily absorbed through the skin.
When taken in pill form, on the other hand, as much as 90 percent of
the natural progesterone is destroyed in the gastrointestinal track within
I5 minutes, and thus no longer available to the body. Tis means that
a much higher dose of progesterone must be taken when used orally as
opposed to transdermally.
Te important thing to remember if you decide to use a cream, how-
ever, is that not all natural progesterone creams are alike. It is critical to
choose a cream with the correct amount of progesterone in it. Dr. Lee
states that women should always use a cream that has at least 400 mil-
ligrams of progesterone per ounce. Most of the good progesterone creams
provide about 480 milligrams of progesterone per ounce. Since the levels
of progesterone in creams are not regulated, some progesterone creams
on the market have carried as little as I0 mg of progesterone per ounce.
(What a dierence!) So looking into which creams have the right amount
of natural hormone in them and are best to use is very important.
Also, some creams are sold as hormone-balancing creams when they
only have wild yam extract in them. It is true that progesterone is often
synthesized from wild yam extract, but that does not mean that the wild-
yam extract itself is going to be the same as progesterone. If a cream boasts
its wild yam extract content, but does not claim to have progesterone in
it, then it will not do a woman any good.
Tere are many good natural progesterone creams on the market today,
and I do not wish to recommend any particular one. But as a general
help, I will mention some of the progesterone creams that I have heard
are good hormone balancing creams. Tese are just some of the creams
that have been independently tested and assessed as having about 400
to 600 milligrams of progesterone per ounce.
361 What Women Must Know About Hormones
Natural Progesterone Creams
ProGest by Emerita (800) 648-8211
www.progest.com
Natural Prog. Cream by Heartland Products (888) 772-2345
www.heartlandnatural.com
Awakening Woman by Alt. Med. Network (877) 753-5424
www.altmednetwork.com
Balance Cream by Vitality Lifechoice (800) 423-8365
Gentle Changes by Easy Way, Internatl. (800) 267-4522
Renewed Balance by AIM Internatl. (208) 465-5116
FemGest by Bio-Nutr. Formulas (800) 950-8484
Woman by Natures Garden (909) 898-1466
www.progesteronecreme.net
Eternal Woman by Mind/Body Solutions (818) 879-1203
www.eternalwoman.com
Natural Prog. Cream by Young Again Nutr. (877) 205-0040
www.youngagain.com
Kokoro Balance by Kokoro, LLC (800) 599-9412
www.kokorohealth.com
ProBalance by Springboard (866) 882-6868
www.springboard4health.com
Natural Prog. Cream by Source Naturals (800) 815-2333
www.sourcenaturals.com
Woman To Woman by Woman To Woman (888) 267-5032
www.womantowomanco.com
ProgestaCare by Life-o (888) 999-7440
www.life-o.com
Tere are many more good balancing creams on the market, and the
creams listed here should not be seen as the only ones to choose from. Tere
is a great deal of information on the Internet about natural progesterone
362 oursxair \oui caxcii
creams, and visiting various sites can give you more information about
each creams specic number of milligrams of natural progesterone, as
well as other ingredients that might be included.
For women who do not have cancer, or who are in remission from can-
cer, supplementing with natural progesterone is easy and safe. Instructions
on how and when to apply the cream are provided with each product, as
well as in Dr. Lees and other books on natural progesterone. However,
for women who are dealing with active cancer (especially those with
large and aggressive tumors), seeking the guidance of a physician or
holistic practitioner is recommended. Tis is because the rst few weeks
on natural progesterone may temporarily sensitize the estrogen receptors
in a womans body and initially cause mild symptoms of estrogen domi-
nance. Tus, depending on your particular case, your practitioner may
suggest you add natural progesterone supplementation very gradually, or
may even suggest that you wait until the alternative approach you are
using has your cancer growth under control rst, before adding natural
progesterone to your program.
Resources:
Books
John R. Lee, M.D., David Zava, Ph.D., and Virginia Hopkins. What
Your Doctor May Not Tell You About Breast Cancer. New York: Warner
Books, 2002.
John R. Lee, M.D., with Virginia Hopkins. What Your Doctor May Not
Tell You About Menopause. New York: Warner Books, 1996.
John R. Lee, M.D., Jesse Hanley, M.D. and Virginia Hopkins. What
Your Doctor May Not Tell You About Premenopause. New York: Warner
Books, 1999.
Websites
www.johnleemd.com ( All of Dr. Lees books, videotapes, and audiotapes
can be ordered from this site.)
www.salivatest.com (For saliva testing.)
363
20
What Men Must Know About
Prostate Cancer, the PSA
and Hormone-Blocking Drugs
W
omen are not the only ones who have to worry about a hormone link
to cancernor are they the only ones who must wonder whether
hormone-blocking drugs are safe or eective. With prostate cancer being
the second most common cause of cancer death in men (after lung can-
cer), and hormone-blocking drugs such as Lupron and Casodex being so
commonly prescribed, this is a very big issue for men, too.
For women with cancer, the hormone that is blocked is estrogen. For
men, the hormone that is blocked is testosterone. In Chapter I9, we saw
that blocking estrogen in women is fraught with negative side eects and
does nothing to help bring about a long-term cure. In fact, some women
die as a result of the estrogen-blocking drug given to them. Is there any
evidence that testosterone-blocking drugs are any more eective for men
who have cancer? Tis is what we will be exploring in this chapter. In the
process, well look at:
I. Diagnosing Prostate Cancer
2. Conventional Prostate Cancer Treatment
364 oursxair \oui caxcii
3. Te PSA Test and Its Limitations
4. What the PSA Really Does and Why the Body Produces It
5. Hormone-Blocking Drugs
6. Te Misunderstood Role of Testosterone
Diagnosing Prostate Cancer
Over the past century, prostate cancer occurred primarily in older men
and was known for being slow-growing in most casesso slow-growing,
in fact, that men over 65 could often simply live with their cancer without
getting any treatment at all. Tis was because they had a good chance of
dying of old age before dying from their cancer. However, according to
cancer treatment specialist Dr. Contreras of the Oasis of Hope Hospital,
recent years are showing more and more cases of aggressive (fast-growing)
prostate cancers being diagnosed. Plus, men of younger and younger ages
are developing prostate cancer and the younger cases tend to have a higher
incidence of aggressive forms.
Methods for diagnosing prostate cancer have improved over the years
and include digital rectal examination (DRE), transrectal ultrasound,
PSA testing, and needle biopsy. Digital rectal examination involves a
physician using a lubricated gloved nger to manually feel the prostate
gland through the rectum. Tis takes only a minute or less and is done
to detect a lump or unusual hardness on the back side of the prostate. It
is an easy, virtually painless procedure and a good diagnostic tool, but it
cannot detect tumors that are on the front or embedded in the middle
of the gland. Since approximately one-third of all men diagnosed with
prostate cancer have normal DREs, the digital exam is never conclusive
by itself.
Transrectal ultrasound (TRUS) is a 5 to I5-minute outpatient proce-
dure that involves an ultrasound wand inserted through the rectum up
toward the prostate. Tough not able to detect every mass I00 percent
of the time, this procedure will detect most masses and is also a valu-
able tool for ascertaining the size and shape of the gland. Together, the
DRE and TRUS are important diagnostic tools for detecting a mass or
a change in size or shape of the prostate gland.
Te PSA test is the easiest diagnostic tool, because it is a simple blood
test. Tis test is not able to detect cancer denitively, but it can often
365 What Men Must Know About Prostate Cancer, the PSA . . .
detect the likelihood of cancer at an early stage, before a mass is noticeable.
Te PSA blood test looks for levels of a compound in the blood called
Prostate Specic Antigen. Tough dierent clinics or doctors may vary
in how they evaluate PSA scores, the following are how PSA levels are
categorized in general:
0 to 2.5 is considered low
2.6 to I0 is considered slightly to moderately elevated
I0 to I9.9 is considered moderately elevated
20 or more is considered signicantly elevated
In the past, doctors considered any PSA count below 4.0 as normal.
Ten it was found that a small percentage of men with prostate cancer
had PSA counts below that, so 4.0 is no longer considered a denitive
number that indicates no cancer. Now, the normal PSA level for most
men is considered to be less than 4.0 and it is thought that men under
the age of 40, in general, should have a PSA count under 2.7. For older
men who have enlarged prostates or calcium deposits in their prostate
glands, a count of 6 to I0 may be considered normal.
Tus, there is no normal or abnormal PSA level which can apply
to everyone. Tis is because PSA levels are only an indirect measure of
something happening in the prostate gland. As we will see in the next
section, there are many reasons why a mans PSA count may be elevated,
and cancer is only one of those possible reasons. Te PSA level goes up in
response to enlargement of the prostate gland or because of pressure in
the prostate gland. Tis pressure may be caused by a tumor growing, but
there can be other sources of pressure, too. Since most men experience
enlargement of the prostate as a normal part of aging, the age of a man
as well as other factors must always be considered in order to understand
the meaning of a mans PSA count.
Keep in mind that PSA results alone do not conrm the existence of
cancer and that this diagnostic blood test simply helps to narrow down
the likelihood of cancer. For example, for a 40-year-old man with no
obvious infection or inammation in the prostate, an elevated PSA count
above 4 indicates a 2025 percent chance of prostate cancer and a PSA
count higher than I0 indicates about a 50 percent chance of cancer. As
the count goes up from there, the likelihood of prostate cancer increases.
366 oursxair \oui caxcii
PSA testing is an important early detection tool, but it is not a denitive
cancer marker test.
Te needle biopsy procedure, on the other hand, does give the deni-
tive answer as to whether a man has prostate cancer or not. It can also
indicate how fast-growing or slow-growing the cancer is. Tis rate of
growth is assigned a number between I and I0 and is referred to as the
Gleason score or the Gleason scale rating. 2 on the Gleason scale
indicates the slowest growing type of prostate cancer and I0 indicates
the fastest-growing type. Typical prostate cancer Gleason ratings might
be 3, 4, or 5. Ratings of 7, 8, 9 or I0 indicate aggressive (fast-growing)
forms of prostate cancer.
Tis way of determining the aggressiveness of prostate cancer was
developed in I966 by a pathologist named Dr. Donald Gleason. Actu-
ally, the Gleason score is really the sum of two preliminary scores from
two sitesa primary site and a secondary site. Each score is obtained by
needle biopsy and assigned a number from I to 5. Ten these two pre-
liminary scores are added together. For example, a score of 4 from the
primary site may be added to a score of 3 from the secondary site to
produce an overall Gleason score of 7.
It is not uncommon for between I2 and 24 needle biopsy sticks to be
required in order to get an accurate sampling of cancerous tissue. Te
down sides to this procedure are: It can be extremely painful; there is
a risk of secondary infection as a result of moving bacteria from the
rectum into other tissue or the bloodstream; and, worse, there is a seri-
ous risk of spreading a mans cancer by promoting metastasis down the
needle tracks into the rectum. Some clinics are using Doppler transrectal
ultrasound to pinpoint the tumor more accurately and thereby require
fewer than the usual number of needle sticks in their eorts to obtain
adequate prostate tissue sampling. So, anyone planning to get a needle
biopsy might want to search for a clinic that uses TRUS to guide their
needle biopsy procedure.
Conventional Prostate Cancer Treatment
Since men are being diagnosed with prostate cancer at younger and
younger ages and often face more aggressive forms of it today, they dont
have the luxury of being able to live with it as commonly as they did in
years past. Tus, there are many more men today who must receive eec-
tive treatment or their prostate cancer will kill them. Unfortunately, the
367 What Men Must Know About Prostate Cancer, the PSA . . .
types of treatment oered by conventional medicine are problematic. Te
four most commonly used treatment methods for prostate cancer are:
I. Surgery
2. Radiation
3. Chemotherapy
4. Hormonal Terapy
Surgery
Tis is the most eective treatment that conventional medicine has to
oer for prostate cancer that is caught very early and involves the complete
surgical removal of the prostate gland (radical prostatectomy). When the
cancer has not yet metastasized, prostatectomy may result in a long-term
cure. However, getting all the cancer is not guaranteed, and this type
of surgery is something most men would like to avoid if possible since it
is often an emasculating procedure with a high likelihood of some degree
of impotence and other dysfunction occurring as a result. (For instance,
besides impotence, some men experience incontinence for years after this
type of surgery.) If the cancer does recur at some point post-surgery, it
will then be considered metastasized prostate cancer and surgery will no
longer be a curative option.
Radiation
Once the cancer has metastasized to other areas of the body, such as
to the lymph system, liver or bones, surgery is no longer a curative option.
At that point, radiation and/or chemotherapy must be relied upon. Radia-
tion treatments can either be done through external beam radiation, or
through radioactive seed implants (called brachytherapy). Either form of
radiation can cause sexual dysfunction and damage to sensitive tissues
in nearby areas such as the bladder, urethra, and rectum that may cause
a man serious physical diculties for the rest of his life. Urinary and
rectal irritation can involve pain, burning, and bleeding, and increased
urinary frequency and urgency may occur. Sometimes these symptoms
dissipate over time, but according to a recent study published in the
Journal of Clinical Oncology, a signicant number of men report new
368 oursxair \oui caxcii
symptoms developing up to 6 years after radiation treatment. Men who
receive radioactive seed implants appear to suer the worst outcomes for
sexual dysfunction and incontinence. Moreover, radiation has also been
proven to sometimes cause prostate cancer cells to mutate into more
aggressive forms that may then be even more dicult to treat than the
original cancer was.
Chemotherapy
Chemotherapy comes with many possible negative side eects: hair loss,
nausea, exhaustion, liver, kidney, heart and nerve damage, to name just
the most common ones. And, like radiation, it rarely has any long-term
curative eect. Dont let ocial cure rates fool you. Tey do not reect
real long-term cures. Tey simply reect 5-year survival rates. Whether
a man continues to suer from cancer or even dies from his cancer after
the 5-year point is of no consequence to these statistics. Doctors will refer
to these statistics when they talk about your chances of being cured
because mainstream medicine has dened cured as being alive ve
years after diagnosis. But the truth is that toxic treatments (any form of
chemo or radiation) may be able to knock down the cancer for a while
and sometimes put a patient into remission, but they can rarely get rid
of all the cancer cells in a persons body. Terefore, chemo and radiation
are rarely able to make a person cancer-free.
Hormonal Terapy
To try to improve the ecacy of conventional treatment for prostate
cancer, mainstream medicine added Hormonal Terapy to their list of
recommended treatments. With this form of therapy, a hormone-blocking
drug is prescribed to block the mans production or use of testosterone.
Two of the most common hormone-blocking drugs for men are Lupron
and Casodex, however there are others as well. Te use of these drugs is
based on the conventionally-accepted idea that testosterone feeds cancer
growth. Hormonal therapy is generally listed as palliative because it is
not even considered by mainstream medicine as a possible curative treat-
ment for a man with prostate cancer. In other words, hormonal therapy
is simply used in an eort to prolong a mans life. But whether it actually
does prolong mens lives, or shortens them, is in question. At the core
of this question lies the controversy around the testosterone-cancer link.
369 What Men Must Know About Prostate Cancer, the PSA . . .
According to Dr. John R. Lee, the current commonly accepted medical
concept that testosterone feeds cancer growth is a fallacy that should have
been corrected decades ago. (Well go into more detail about this issue
very soon and look at why the concept that testosterone feeds cancer does
not hold up to scientic scrutiny.)
Other less common conventional treatment methods for prostate can-
cer are orchiectomy and estrogen therapy. Orchiectomy involves surgical
castration through the removal of the testicles. About ninety-ve percent
of a mans testosterone is produced by the testicles, with the remainder
being produced by the adrenal glands. Orchiectomy is performed as an
attempt to stop as much testosterone production as possible which, of
course, is due to the widely-held belief that testosterone feeds cancer. Since
testosterone-blocking drugs were developed, however, the use of drugs
to block testosterone tends to be chosen as a more favorable approach
over surgical castrationespecially since it was found that the adrenal
glands in men who underwent orchiectomy would often step up and
produce more testosterone after the surgery to compensate for the loss of
production by the testicles. Tus, men who undergo orchiectomy often
have to take hormone-blocking drugs post-surgery, anyway, to block the
testosterone their adrenal glands are making. Tis is no longer a preferred
approach because it is irreversible and also since men still need to take
testosterone-blocking drugs afterward anyway.
Side eects of all hormone therapy methods used to block or reduce
a mans testosterone include impotence, hot ashes, weight gain, loss of
muscle mass, fatigue, loss of sexual drive, nausea, vomiting, and breast
swelling and tenderness.
Estrogen therapy is another hormone therapy that is sometimes used
in an attempt to block testosterone. Tough not one of the more common
protocols, administration of estrogen not only suppresses the production
of a mans testosterone, but it is thought to also have a negative eect on
prostate cancer cells. Historically, this type of treatment has been used
primarily in late-stage cases in patients who have developed hormone-
resistant prostate cancer and a synthetic estrogen called diethylstilbestrol
(DES) has been the estrogen of choice. However, this approach is only
used occasionally today and may carry with it some risk of developing a
blood clot, heart attack or stroke.
Even with all of the above treatment options to choose from, conven-
tional medicine has not had signicant success curing prostate cancer other
than through complete surgical removal of the prostate gland when the
370 oursxair \oui caxcii
cancer is caught early. Many alternative cancer treatments, on the other
hand, have shown excellent track records for curing prostate cancereven
after it has metastasized. Some of the most eective alternative methods
for bringing about long-term prostate cancer cures are: (I) Protocel
For-
mula 23, (2) the Flaxseed Oil and Cottage Cheese diet, (3) Essiac Tea and
(4) Low-Dose Naltrexone. Other alternative methods have been known
to work for prostate cancer as well. Tus, it is no surprise that more and
more men are turning to alternatives that dont involve surgical mutila-
tion or damage to the body through toxic treatments.
However, because drugs such as Lupron and Casodex can very quickly
lower a mans PSA count, men with prostate cancer are convinced they
should still take a hormone-blocking drug even though they choose to
rely primarily on an alternative non-toxic method to treat their cancer.
Te medical establishment seems to have everyone convinced that less
testosterone in the body is best for a man with prostate cancer and that
a lower PSA count means less cancer. But, as we will see, lowering the
PSA count through the use of testosterone-blocking drugs is simply an
articial way of reducing the PSA and does not correlate with a decrease
in cancer. Moreover, there is reason to believe that less testosterone in
the body may actually cause a hormone imbalance that can promote the
growth and spread of cancer! Terefore, the issue of whether a man with
prostate cancer should use a hormone-blocking drug or not is of utmost
importance. But, in order to fully understand this issue, we must rst
understand more about the PSA.
Te PSA Test and Its Limitations
Men choosing either conventional or alternative treatment will gener-
ally want to follow their progress by getting regular scans as well as by
checking their PSA levels. Te good news is that the PSA test can be used
as a valuable tool in the diagnostic process. Te bad news is that the PSA
test is not as accurate at measuring cancer as many doctors lead patients
to believe, and anyone using this test should be aware of its limitations.
As already mentioned, PSA stands for Prostate Specic Antigen,
which refers to a protein produced primarily within the prostate gland.
However, as Dr. Lee points out, calling this substance prostate specic
antigen is not completely accurate since it is not specic only to the
prostate glandin fact, PSA is also produced within breast tissue in
both men and women. Tat issue aside, it is normal for healthy men to
371 What Men Must Know About Prostate Cancer, the PSA . . .
have a small amount of PSA always leaking out into the bloodstream.
Te amount of PSA that is leaked, so-to-speak, is what the PSA test is
designed to detect.
When the prostate gland is enlarged, infected, or diseased, greater
than normal amounts of PSA are released. Because high elevations in
PSA tend to correlate with the growth of cancer in the prostate gland, the
PSA test was approved by the FDA in I986 for helping to monitor and
care for patients who had already been diagnosed with cancer. Ten, in
I994, the test was approved for the general public as an early detection
blood test for cancer. Since then, the PSA test has become more often
relied upon as a cancer diagnostic, and its limitations have become more
often ignored.
What surprises many men is that there are conditions besides prostate
cancer that can cause a mans PSA count to rise. For instance, prostatitis
and lower urinary tract problems can cause the PSA to rise and remain
elevated. BPH (benign prostate hypertrophy), which is simply enlarge-
ment of the prostate gland, can also cause the PSA to rise and remain
high. Temporary increases in PSA levels may be caused by ejaculation
within 24 hours before the test, digital rectal examination before the test,
or prostate biopsy. (In fact, prostate biopsy can cause such a dramatic rise
in the PSA that it can take up to a month for the PSA count to return
to normal after this procedure.)
In other words, a man with a high PSA count might have cancer, or he
might just have inammation in the prostate gland or some other reason
for an elevated PSA. Te truth is that a whopping two-thirds of men with
elevated PSA levels do not have prostate cancer!
Tus, the poorly-named Prostate Specic Antigen is not only not
specic to the prostate gland, it is also not specic to prostate cancer. Too
many men are being scared into thinking that a certain PSA level means
they must have cancer. And other men who are dealing with prostate
cancer are being scared into thinking that even a one-point rise in their
PSA count is an indication that their cancer is growing, when there could
be many reasons why their PSA count might go up one or more points
at any given time.
On the other hand, one might at least hope that if a man does have
prostate cancer, the PSA test will denitely ag it. Not necessarily. In about
20 percent of the cases where men are known to have early prostate cancer,
the PSA level is normal! For example, this will generally be the case when
a malignant tumor is occultmeaning it occurs on the outside of the
372 oursxair \oui caxcii
prostate gland rather than inside it. Doctors even classify some prostate
cancers as low-PSA producing cancers. Frank Critz, M.D. is founder
and medical director of Radiotherapy Clinics of Georgia (RCOG) and
has treated 8,000 men with prostate cancer over 25 years. In a question
and answer posting on his website, Dr. Critz made some very illuminat-
ing statements. He wrote:
Some prostate cancers will not make very much PSA and are called
low-PSA producing cancers. Low-PSA producing cancers can be very
advanced and fool doctors. For example, the worst cancer we have treated
at RCOG in the past I0 years was in a man whose highest PSA was
only 0.5 ng/ml. However, he had a Gleason score of I0 and the cancer
had already spread (metastasized) into his bones and he was incurable.
Te PSA is usually a good indication of the amount of cancer you have,
but it is far from foolproof.
So what is this all about? Havent men been led to believe that a PSA
test can tell them whether they have prostate cancer or not? For the next
level of understanding, we must look at what the PSA does in the body
and why it is produced in the rst place.
What the PSA Really Does and Why the Body Produces It
Te clearest explanation of the real functioning of the PSA comes from
a 28-page booklet called Hormone Balance for Men, by Dr. John R. Lee.
Dr. Lee produced this booklet in 2003, and in it he challenges common
misconceptions about the PSA and the role of testosterone and cancer.
Troughout the rest of this chapter, Ill refer to the main points Dr. Lee
makes, but readers should get his booklet for a more in-depth technical
understanding. It can be ordered online for just $I4.95 at www.johnlee
md.com/store/books_booklets.html, or by calling (877) 375-3363.
In Hormone Balance for Men, Dr. Lee explains that the PSA has only
recently begun to be understood in medicine. First of all, the PSA is not
something that only cancerous cells produce. In fact, PSA is produced
in large part by normal healthy cells of the prostate gland. Te most
important concept that Dr. Lee explains is that normal healthy cells of
the prostate gland produce PSA simply in response to crowding (or pressure).
Tis is why an infection or any type of inammation in the prostate gland
will generally cause a rise in a mans PSA productionthe inammation
causes swelling, and the swelling causes pressure against the surrounding
373 What Men Must Know About Prostate Cancer, the PSA . . .
normal cells. It is also why benign calcium deposits in the prostate gland
can cause general irritation and result in a rise in the PSA as well. Even
manually applying pressure by massaging the prostate gland will often
cause an elevation in PSA production. Basically any signicant or sus-
tained pressure against normal healthy cells of the prostate gland will
tend to cause those cells to produce more PSA, and this will show up as
a rise in a mans PSA count.
In the same way, when a mans PSA count rises due to prostate cancer it
is because a tumor developing inside the gland presses on the surrounding
healthy cells as it growsthereby crowding them. Te crowded healthy
cells of the prostate then respond by producing higher amounts of PSA.
Tis is why there is a general correlation between higher PSA levels and
prostate cancer.
Te concept that increased PSA production is caused by cells being
crowded is not generally accepted throughout mainstream medicine,
but it elegantly explains why so many dierent types of situations can
cause a rise in a mans PSAand it is also supported by the fact that an
occult tumor on the outside of the prostate gland will not cause a rise in
PSA. (Since a tumor on the outside grows outward and away from the
prostate, it does not crowd the healthy cells of the gland.) In his booklet
Hormone Balance for Men, Dr. Lee has, in essence, explained a new way
of undrstanding what causes the PSA production in a mans body to rise.
And he points out that there is ample scientic support for this new way
of looking at the PSA.
So, if we accept that a mans body responds to increased pressure
against normal healthy prostate cells by having those cells that are being
crowded produce more PSA, then the obvious question to follow is, Why
do those cells produce more PSA when they are crowded? Nature gen-
erally has a very good reason for any physiological action that repeatedly
takes placeand this is no exception. According to Dr. Lee, the answer
is that the healthy prostate cells produce more PSA when they are crowded
because the PSA has anti-angiogenic properties. Voila! Tis is the key bit
of information that allows everything else to make sense!
Anti-angiogenesis is a very interesting process. It is well-known that
malignant tumors of virtually all types are able to stimulate the growth
of new blood vessels to themselves. Tis is called angiogenesis, and it
occurs when a tumor is quickly outgrowing its food source and needs
new blood vessels to feed itself. In other words, the tumor feeds its own
374 oursxair \oui caxcii
abnormal growth by triggering the growth of new blood vessels to itself
through angiogenesis. Anti-angiogenesis, therefore, refers to the process
of inhibiting new blood vessel growth to a tumor and there are a number
of dierent substances in nature that are known to be naturally anti-
angiogenic. For instance, the use of shark cartilage by cancer patients
was introduced decades ago because shark cartilage has anti-angiogenic
properties. A number of dierent herbs also have anti-angiogenic prop-
erties and have successfully been used to help control cancer growth in
many cases. (One such herb is called Bindweed.) Since anti-angiogenesis
slows down a malignant tumors ability to feed itself and thereby slows
the tumors growth, it is always a good thing for a person with cancer to
have this occurring.
So, now our understanding of the functioning of the PSA is complete,
and it is really quite simple. Normal healthy prostate cells are crowded when
a tumor inside the prostate gland starts growing. Te crowded healthy cells
produce higher amounts of PSA than they normally would and that PSA
has angiogenesis inhibiting (or anti-angiogenesis) properties. Tus, the
crowded surrounding healthy tissue is simply responding to the pressure
from a tumor by producing more PSA to slow the growth of the tumor.
Tis is the common sense that nature so often exhibits and is the bodys
way of allowing the prostate gland to protect itself against the spread of
cancer. Apparently, a mans prostate is quite a smart gland!
At this point, it would be perfectly reasonable for a person to ask, Are
there any other sources of medical research that back up this concept that
the PSA has anti-angiogenic properties? Or is Dr. Lee the only one saying
this? As it happens, various scientic studies have already supported this
concept. For instance, the American Cancer Society summarized some
groundbreaking research in November of I999 in an article they posted
on one of their online news sites. Te title of the article was Does PSA
Fight Prostate Cancer? In it, the American Cancer Society stated:
When PSA levels rise above normal, it indicates prostate cancer may
be present or returning. For this reason, men have generally thought of
PSA itself as something undesirable. But this study from the Journal of
the National Cancer Institute (Vol. 9I, No I9) suggests PSA may not be
the enemy but only a messenger.
PSA may be ghting prostate cancer. It may be an angiogenesis
inhibitor, meaning it may work to slow or stop the growth of tumors by
shutting o the blood vessels that feed them.
375 What Men Must Know About Prostate Cancer, the PSA . . .
Tis ACS news article then went on to report some of the research
ndings from a Maryland biotech company called EntreMed that was
trying to develop some anti-angiogenic drugs. It appears that, as back-
ground research, the EntreMed scientists had performed some interesting
studies using human PSA. Tis is what the American Cancer Society
reported about EntreMeds research:
Te researchers were aware that PSA had been found in cancers other
than prostate cancer. For example, a study showed breast cancer patients
with high PSA levels had a better prognosis. Tey theorized higher PSA
levels in men with prostate cancer might reect PSA being produced to
ght growth of the tumors new blood vessels and decided to test their
theory with a series of experiments.
Te group rst introduced PSA into lab dishes containing endothelial
cells, the kind of cells that form blood vessels, and found that it did slow
their reproduction. PSA also reduced the cells ability to migrate, or to
come together in preparation for forming new blood vessels.
. . . Te researchers then injected PSA into mice with cancer and found
it reduced the number of new tumors in distant locations (metastases)
by 40 percent. Tey concluded PSA does, in fact, reduce tumors ability
to grow new blood vessels and suggested other researchers might want
to re-think the concepts behind anti-PSA prostate cancer vaccines and
other anti-PSA strategies now being developed.
If Dr. Lee and the EntreMed scientists are correct, then an increased
production of PSA in a man with prostate cancer is simply his own bodys
way of trying to stop or slow down the cancer growth. Clearly, no man
would want to articially reduce his bodys production of PSA with this
understanding. Unfortunately, this is exactly what hormone-blocking
drugs do.
Hormone-Blocking Drugs
Tere are a number of hormone-blocking drugs that are prescribed
to men with prostate cancerLupron and Casodex being two of the
most common. Tough various drugs have dierent mechanisms of
action, the overall result of these types of drugs is that they either block
the production of testosterone or they block the use of testosterone in a
mans body by blocking the testosterone receptors. When testosterone is
blocked either way, the PSA count goes down. Why? Because the body
376 oursxair \oui caxcii
needs testosterone to produce PSA. Tus, using a testosterone-blocking
drug is simply an articial way of lowering of a mans PSA count that
has nothing to do with reducing the amount of cancer in his body. In
eect, blocking testosterone and seeing a reduction in PSA is simply like
blocking the delivery of our to a bakery and seeing that the baker cant
make as many cakes as before!
So why do doctors love to prescribe testosterone-blocking drugs? One
reason is because they like to see a mans PSA count go down. Tey know
that higher PSA scores tend to correlate with more cancer and lower PSA
scores tend to correlate with less cancer. But they dont understand the
crowding issue or the anti-angiogenic property of the PSA, because those
things have not gotten any attention in the mainstream medical world. So
they tend to categorically think of any elevated PSA level as a bad thing.
But, Wait a minute, you might ask, When I use a testosterone-
blocking drug for my prostate cancer, my PSA count goes down dra-
matically and stays down. Doesnt that mean the drug is reducing my
cancer? Te answer is No, it doesnt mean that. Hormone-blocking
drugs for men articially reduce the PSA count simply because they block
testosterone and testosterone is needed by the cells of the prostate gland
in order to eciently produce PSA. Tis way of reducing the PSA count
has no correlation to a reduction in a mans cancer. In reality, articially
lowering a mans PSA count with a testosterone-blocking drug, then
thinking his cancer is going away, is like articially tampering with the
digital display on a weight scale so that it displays a signicantly lower
weight than it shouldthen standing on that scale and thinking youve
actually gotten thinner!
Tus, the only way for a man on a hormone-blocking drug to really
know if his cancer is receding or not is through some form of scan that
can actually detect tumors in the prostate and/or metastatic lesions in
distant locations. Te PSA test should denitely not be used as a diag-
nostic tool when testosterone is being articially blocked. At that point,
a mans digital display has been tampered with, so-to-speak.
Another reason that physicians like to prescribe testosterone-blocking
drugs is because there is a basic misunderstanding in the medical world
about the role of testosterone and prostate cancer. Tis misunderstanding
has been telling physicians that testosterone feeds cancera medical fallacy
that began more than six decades ago. Unfortunately, as we know from
womens hormone issues, medical misunderstandings are dicult to turn
around and can take many, many years before they are nally corrected.
377 What Men Must Know About Prostate Cancer, the PSA . . .
Te Misunderstood Role of Testosterone
According to Dr. Lee, the misunderstanding about testosterones role
in prostate cancer began back in I94I, when a well-known physician
named Dr. Charles Huggins carried out some ground-breaking medi-
cal research on men with prostate cancer. In Hormone Balance for Men,
Dr. Lee describes this historical event which he calls Te Testosterone
Fiasco in the following way:
In I94I, Dr. Charles Huggins showed that castration (orchiectomy)
slowed the progression of prostate cancer. Castration removes much of
ones testosterone production. He unfortunately assumed that the reduc-
tion of testosterone levels was the operative agent for his benecial results.
He failed to consider that castration also removes ones estrogen produc-
tion. Tus, it is likely that the estrogen reduction was the real operative
agent. Despite these faulty assumptions, Dr. Huggins was given the
Nobel Prize for his research. As a result, conventional medicine came to
believe that testosterone was the culprit in causing prostate cancer. Te
prevention and treatment of prostate cancer focused on either remov-
ing the prostate gland or reducing testosterone, or both. Techniques
were found to castrate men surgically or chemically, as in Lupron, for
example. Other doctors opted for radiation. In all of these treatments,
all sex hormone production by the testes is stopped or arrested, and
undesirable side eects are common. Te sad fact is that survival of men
with prostate cancer has not improved with these treatments. Further
drugs (e.g., Flutamide) were developed to block all testosterone recep-
tors (called total androgen blockade), thus eliminating the testosterone
eect completely. It is now conceded that survival time is not aected;
the men so treated instead developed depression, dementia, and diarrhea
before dying right on time.
Te fallacy that testosterone feeds cancer was probably then kept alive
by researchers who saw that blocking testosterone made mens PSA levels
go down and who drew the conclusion that the cancer was going away
because they did not have the understanding that testosterone is simply
needed to produce PSA.
A very eye-opening point that Dr. Lee makes is that the erroneous
testosterone feeds cancer concept still exists today despite the fact that
(I) it has always been known that prostate cancer occurs most frequently
in older men after their testosterone production has declined and that,
until recently, prostate cancer was virtually unheard of in young men
378 oursxair \oui caxcii
when testosterone production is highest, and despite the fact that (2) as
far back as the I950s, the University of Chicago was reporting on stud-
ies that showed pre-treating mice with testosterone prevented successful
implantation of prostate cancer in those mice. Moreover, when cancer
cells were implanted without testosterone and the cancer was allowed to
developthen testosterone was added at that pointthe prostate cancer
implants in the mice promptly stopped growing.
Te University of Chi-
cago studies are an example of how good science can be ignored if the
results dont t with the currently accepted medical paradigm.
So, if the PSA can slow down the growth and spread of prostate cancer
by inhibiting angiogenesis, and testosterone is needed by a mans body to
produce PSA, and if testosterone by itself has also been found to inhibit
prostate cancer growth in laboratory animals, then it is clear that men
should not be blocking their testosterone production if they have prostate
cancer. If thats not convincing enough, Dr. Lee makes two more impor-
tant points about testosterone which indicate that the more testosterone
a man with prostate cancer has, the better.
Te rst important point is that testosterone has the ability to oppose
estrogen. Mens bodies make estrogen, too, though not as much as wom-
ens bodies, and estrogen can fuel not only womens cancers of the breast,
uterus or ovaries, but it can also fuel mens cancer in the prostate gland.
Numerous studies have clearly shown that raised estrogen levels promote
prostate cancer. Tus, the more testosterone a man has, the less likely he
will be estrogen-dominant. Unfortunately, when a mans testosterone level
is articially reduced through the use of a testosterone-blocking drug, that
allows a dangerous shift in hormone balance to occura shift, accord-
ing to Dr. Lee, that always results in estrogen dominance. In fact, there
is no doubt that estrogen dominance occurs when testosterone-blocking
drugs are administered, because men can feel and see this shift happening.
When men take Lupron, Casodex, or other testosterone-blocking drugs,
they often experience enlarged or tender breasts and other symptoms that
indicate the estrogen in their body is having a more pronounced eect
than it was having before.
Te second important point that Dr. Lee makes about testosterone
and cancer is that, like progesterone, testosterone activates the p53 gene
in cancer cells. As we discovered in the last chapter, it is the p53 gene
that induces normal cell death, or apoptosis. In fact, Dr. Lee was so con-
vinced that testosterone is actually benecial to men with prostate cancer,
that he prescribed both testosterone and progesterone to his own prostate
379 What Men Must Know About Prostate Cancer, the PSA . . .
cancer patients. Over a decade and a half, the results he had with those
patients were excellent.
One of the reasons testosterone supplementation originally got labeled
as dangerous was because, back in the mid-I900s, some drug companies
produced and sold a synthetic and chemically altered testosterone called
methyltestosterone. Tey promoted it as if it were real testosterone even
though it was a form not naturally found in the human body. After several
years, some men using methyltestosterone developed liver cancer.
It is never a good idea to use a chemically altered hormone that is not
naturally found in the body, and even supplementing with bioidentical
hormones must be done carefully and in balance with other hormones.
Tus, when men supplement with testosterone for body-building or for
reduced libido due to normal aging, if they dont supplement in a balanced
way, they may put themselves at risk for various health problems. Dr. Lee
always looked at progesterone levels in men as well and prescribed bioi-
dentical progesterone when needed along with bioidentical testosterone.
When it comes to the role of testosterone and cancer, one of the prob-
lems we face today is that conicting studies keep coming out. Anyone
doing a quick online search today can nd recent scientic reports with
titles such as High Blood Testosterone Levels Associated With Increased
Prostate Cancer Risk, and Study Links High Testosterone and Prostate
Cancer Risk. In the same search, however, one can nd equally prestigious
medical institutions putting out scientic reports that say just the opposite.
Report title examples are Testosterone Doesnt Aect Prostate Cancer
Risk, and Testosterone Seen Unrelated to Prostate Cancer Risk. Tus,
if your doctor claims that scientic studies have proven that testosterone
promotes cancer, you can assert that there are equally prestigious scientic
studies that prove it doesnt. Obviously, the testosterone-cancer link is a
complicated issue that medical science has not yet gured out.
In fact, more and more holistically-oriented doctors are prescribing
bioidentical testosterone to men who are going through normal aging
changes as a way to improve their health and functioning. According to
a recent Life Extension Magazine article, A recent study found that men
with lower testosterone levels were more likely to die from cardiovascu-
lar disease and all causes compared with men who had higher levels. . . .
Another review from the Baylor College of Medicine reported that there
is a higher prevalence of depression, coronary heart disease, osteoporosis,
fracture rates, frailty, and even dementia with low testosterone states.
It is well-known that testosterone helps maintain strong muscles and
380 oursxair \oui caxcii
bones, and the risk of osteoporosis and increased fracture rates in men
with low testosterone is no small matter. In other words, suppressing ones
testosterone while dealing with prostate cancer could cause other serious
health threats that most men are not hearing about from their doctors.
In fact, one MSNBC news release posted in 2005 stated, Hormone-
suppressing drugs increasingly used to suppress prostate cancer make
men so prone to broken bones that the risks of the treatment may out-
weigh the benets in those whose cancer was caught early.
Te release
goes on to explain that, for the elderly, broken bones can be lethal due
to complications and that One-third of elderly men who break their hips
die of complications within a year.
All of the above brings us to the unhappy conclusion that, when a man
is given a testosterone-blocking drug for prostate cancer:
I. He is having his testosterone level articially reduced . . . even though
testosterone helps to control prostate cancer by opposing estrogen and by
activating the p53 gene to induce normal cell death,
2. He is having his PSA production articially reduced . . . even though
the PSA is his bodys own defense against prostate cancer through its ability
to inhibit angiogenesis and thereby slow a tumors ability to feed itself,
3. He is having his body thrown into an articially-induced estrogen
dominant state . . . even though estrogen dominance is known to promote
prostate cancer, and
4. He is having his body thrown into an extremely low-testosterone state
. . . even though low testosterone is known to cause depression, dementia,
and an increased likelihood of death from cardiovascular disease as well
as from bone fracture complications in the elderly.
Tese four situations are at a best, undesirable, and at worst, deadly.
Yet a majority of men with prostate cancer will be faced with their doctor
prescribing them a hormone-blocking drug. Tis is why it is so impor-
tant for men to understand the real testosterone connection to PSA and
prostate cancer and what PSA and testosterone really do in the body. As
mentioned earlier, there are a number of alternative non-toxic methods
that have excellent track records for prostate cancer. Specic approaches
381 What Men Must Know About Prostate Cancer, the PSA . . .
in this book to refer to would be Essiac Tea, Protocel
, Flaxseed Oil
and Cottage Cheese, Cesium High pH Terapy, Low Dose Naltrexone,
Pau D'Arco, and Ellagic Acid. (Remember, however, that when using
Protocel
the PSA count may rise dramatically for a while as the cancer
is breaking down.)
For those men who are still not convinced of the dangers of testoster-
one-blocking drugs and wish to use one while they pursue an alternative
treatment approach, virtually no scientic study has been done on the
associated impact that blocking testosterone may have on success with
alternative therapies. One medical expert, Dr. Bernard Bihari, found this
to be a serious issue with his own patients. In his work with non-toxic
Low Dose Naltrexone (LDN), Dr. Bihari had a high rate of success put-
ting prostate cancer patients into remission. (See Chapter I7.) However, he
discovered that this success only applied to men who were not currently
taking, or who had not previously used some form of hormone manipula-
tion treatment. According to Bihari, the prostate cancer patients who had
used a hormone manipulation treatment for their cancer did not respond
as well as other patients did to the Low Dose Naltrexone therapy. Tis
included men who had taken Lupron, Casodex, Eulexin, DES, or other
drugs designed to reduce testosterone.
It may not be clear at this point as to what all the ways are that a
testosterone-blocking drug could interfere with an alternative approach,
other than making a man estrogen-dominant and speeding up the spread
of his cancer. But it is particularly alarming that even men who were no
longer on a hormone-blocking drug, but had taken one before, still did not
respond well to Dr. Biharis treatment.
Hopefully, more and more men will decide to decline hormonal therapy
for their prostate cancer. If this is something you are considering, it may
not be easy. Your oncologist may not be sympathetic to your decision to
turn down what is considered an established medical approach. You may
even nd that your doctor will refuse to treat you or monitor your progress
if you do not take a hormone-blocking drug. In that case, you may want
to refer him or her to Dr. Lees booklet Hormone Balance for Men for the
scientic evidence that blocking testosterone in men with prostate cancer
is not a good idea and indeed may cause harm. You may even need to nd
a dierent doctor to work with. Te bottom line is that men have a right
to refuse any treatment they dont want, and it may be time for men with
prostate cancer to just say no to hormone-blocking drugs.
382 oursxair \oui caxcii
Resources:
Booklet
John R. Lee, M.D. Hormone Balance for Men. $14.95, 28 pages. To order,
call (877) 375-3363 or go to www.johnleemd.com and select Books
then Booklets and Reports.
Websites
www.johnleemd.com (All of Dr. Lees books, videotapes, and audiotapes
can be ordered from this site.)
www.zrtlabs.com (For hormone testing.)
383
2I
Toxic Teeth
S
ome of the most disturbing information about aspects of modern liv-
ing that can contribute to cancer involves common dental practices.
However, on the bright side, dealing with some of these dental issues can
be a very powerful step to overcoming cancer in certain cases. Although
not everyone with cancer has toxic teeth, the information in this chapter
may provide some people with an important key that could inuence
whether or not the treatment they use for outsmarting their cancer is
successful or not.
Tere are three main sources of toxic teeth in dental practice today that
can contribute to cancer. Tey are: (I) silver llings, (2) nickel-alloyed
porcelain crowns, and (3) root canals. People who have any of these in
their mouths may be carrying around an extra load of carcinogenic sub-
stances. Many people are healthy enough to be able to handle this extra
load without obvious problems. But others, especially those people who
are ghting serious illnesses, may not be.
Silver Fillings
First, lets look at the most common of these three practicesthat of
installing silver llings. Tis type of cavity-lling material is not quite as
prevalent today as it used to be, but is still being administered widely. For
those of us in our mid-life years, this was the only type of dental lling
384 oursxair \oui caxcii
that was ever oered to us as children or young adults. Te truth we
were not told, however, is that silver llings are only half silver. Techni-
cally, they are silver amalgams because they are always combined with
another material to make them more pliable. Tat pliable material, which
comprises the other half of the silver lling, is mercury.
Mercury is one of the most deadly substances found on earth, if ingested.
Even the vapor from mercury is extremely toxic. Most of us have heard
the term mad as a hatter, which was popularized with the mad hatter
character in Lewis Carrolls tale of Alice in Wonderland. Te mad hatter
syndrome was prevalent in the I800s and may have continued into the
early I900s because mercury was used extensively in the hat-making pro-
cess. A mercury compound called mercury nitrate was commonly used to
remove fur from pelts and to produce felt for hats more easily. (Abraham
Lincolns big stovepipe hat was made this way.) Te hat-makers themselves
were exposed to large amounts of vaporized mercury and began to dis-
play symptoms of brain damage. Doctors who did autopsies on hatters
sometimes reported seeing large holes inside their brains. Although the
use of mercury in hat-making has been banned, the use of mercury in
dental llings has not. Mercury still comprises about 50 percent of all
silver (amalgam) llings.
In some European countries, mercury amalgam llings have been
banned for decades. However, in the United States, they continue to be
standard practice, and many dentists are still telling their patients they
are completely safe. Te true toxic nature of silver-mercury amalgams
has been played down by the American Dental Association and most
dentists believe the standard line of the ADA. However, other American
dentists started wondering years ago how safe amalgams really could
be when the instructions they receive with the lling material include
some alarming directives. Tese instructions on how to handle mercury
amalgam llings are still given with the material, and include warnings
to dentists such as:
Dont ever touch it with your ngers.
Dont leave it lying around uncovered.
Leftover amalgam material, or an extracted tooth with an amalgam ll-
ing still in it, must be disposed of under strict toxic waste protocols.
In other words, dentists are warned that the mercury for silver amalgams
385 Toxic Teeth
is too toxic to touch, breathe, or to just throw into the waste basket. (Yet,
its okay to put it into someones mouth and leave it there for many years.)
As a result of instructions such as these, many clear-thinking dentists qui-
etly stopped using amalgam llings about 20 years ago and started using
other materials whenever possible. Tis had to be done quietly, because
dentists who were outspoken about the hazards of silver-mercury llings
often lost their license to practice.
One famous dentist who became probably the most outspoken against
amalgam llings was Dr. Hal Huggins. He wrote a controversial book
about this issue and reported many illnesses such as multiple sclerosis,
Parkinsons disease, and crippling arthritis that either cleared up or greatly
improved when his patients silver amalgam llings were safely removed.
Since so many of the side eects caused by silver amalgam llings have
been dismissed as psychosomatic complaints by doctors, Huggins aptly
named his book Its All in Your Head.
Although the ADA still seems to hang onto the idea that the mercury
in amalgams does not leak out once it is put into someones mouth, there
have been many scientic studies proving that it does indeed leak out into
the body. Included in these studies is proof that a signicant amount of
mercury can get into the brain and stay there. Some researchers believe
this is a contributing factor to Alzheimers disease, since it is known that
mercury in the brain can cause the sort of damage that is seen in the
brains of Alzheimers patients.
Tere are many ways that toxic mercury poisoning from dental work
can bring about a gamut of illnesses. One of the ways this can happen
is by weakening the immune system in general. Dr. David Eggleston of
the University of Southern California measured T-lymphocyte levels in
patients with mercury amalgam llings. As an important contributor to
health, T-lymphocytes normally comprise from 70 to 80 percent of the
lymphocyte population in a healthy persons immune system. In one case,
Eggleston found that a 2I-year-old woman with amalgam llings in her
mouth had a T-lymphocyte level at only 47 percent of her total lymphocyte
population. He removed her amalgams and replaced them with a plastic
type of temporary lling. At that point, her T-lymphocyte levels rose from
47 percent to 73 percent. Next, he removed the plastic llings and lled
the teeth again with amalgam, and her T-lymphocytes fell back down to
55 percent. Finally, Eggleston removed this second set of amalgam ll-
ings and lled the patients teeth with safe gold inlays. At this point, her
T-lymphocyte level went back up to a healthy 72 percent.
386 oursxair \oui caxcii
It is very likely that a depressed immune system from mercury poisoning
can predispose a person to cancer, not to mention the fact that mercury
is, itself, a carcinogenic substance. Tis means that it can also directly
cause cancer. One cancer story involving mercury amalgams was reported
by the son of a dentist named Dr. Pinto. Dr. Pinto rst learned about
the dangers of amalgams at a conference in the I920s. According to the
story, Dr. Pinto was asked to treat a child who was complaining that her
gums hurt. Te child was also dying of leukemia. To try to save the child,
Dr. Pinto quietly removed all of her amalgam llings. Tis childs condi-
tion dramatically responded in just of few days and her doctors actually
pronounced her leukemia as a case of spontaneous remission.
Dr. Pinto then told the physician that he had removed her amalgams,
but the physician and others in the medical profession wouldnt believe
that had anything to do with the remission. To try to get through to
them, Dr. Pinto re-inserted one amalgam lling in the little girls mouth
and told the doctor to look for a recurrence of the leukemia. Tere was a
recurrence of symptoms, and Dr. Pinto then removed the amalgam ll-
ing, which was followed again by the childs recovery.
Dr. Pinto did further research into the historical occurrences of certain
types of diseases and found that Hodgkins disease, another type of cancer,
was virtually unheard of until I832, shortly after amalgam llings had
been introduced into the very region where the rst case of Hodgkins
disease was discovered. Unfortunately, no one in the dental profession
would listen to Dr. Pinto.
However, recent research on amalgam llings has been conclusive
enough to cause some serious changes around the world. For instance, the
government of Sweden performed its own research and concluded that
250,000 Swedes had immune system and other health disorders related
to their amalgams. Te Swedish government then put amalgam use on
a schedule for complete phase-out. In I994, a German company called
Degussa, the worlds largest producer of metals for use in dentistry, shut
down its production of amalgam completely. Degussa apparently took
the stance that it would reinstate the production of amalgam after mer-
cury had been proved safe for the body. Tere are at least four European
countries that currently have either banned the use of amalgam llings
for children and women of child-bearing age, or have put amalgam use
on a schedule toward complete phase-out.
Even though the United States has not banned amalgam use, one survey
published in the December I989 issue of Dentist magazine reported that
387 Toxic Teeth
over one-third of the dentists polled did believe that all silver amalgam
llings should be removed and replaced with composite llings. Yet, den-
tists who feel this way in the United States are up against very powerful
opposing forces that appear to control the policies of the ADA. As of
I994, the ADA Code of Professional Conduct stated:
. . . the ADA has determined through the adoption of Resolution
42H-I986 that the removal of amalgam restoration from the non-allergic
patient for the alleged purpose of removing toxic substances from the
body, when such treatment is performed solely at the recommendation
or suggestion of the dentist, is improper and unethical.
A CBS 60 Minutes program aired a segment on the amalgam contro-
versy in December I990. Although it received one of the highest viewer
responses ever, this segment was not repeated. Moreover, the Washington
State Dental Associations response to this program was to immediately
inform its dentist members that their patients did not have a right to
know that their silver llings contained mercury.
Te diculty with this controversial issue is that not everybody with
amalgam llings has cancer or some other obvious illness. Tis is because
many peoples immune systems are strong enough to withstand the dam-
age that the mercury does to the body. However, if you are already dealing
with a serious illness, you may want to consider having your amalgam
llings safely replaced with another material.
What is critical to understand, however, is that there are safe ways to do
this and unsafe ways. If you rush out and have your amalgams removed
quickly by a dentist who does not understand the safety precautions
required, you may be risking even more damage to your health. Sloppy
removal of silver amalgam llings can release even more mercury into
your system than was leaking out before. You should denitely understand
this issue if you are ghting a terminal illness and you opt for amalgam
replacement. In fact, you may want to seek out the services of a biological
dentist. (Tis is a more and more common description of dentists who
specialize in understanding and working with toxic teeth issues.)
When planning to get your silver amalgams replaced, two safety pre-
cautions to discuss with your dentist are the following:
I. Request a rubber dam. Tis is a piece of rubber designed to stretch
between the lower right and left teeth with only the tooth being
worked on uncovered. Its purpose is to keep any small pieces of
388 oursxair \oui caxcii
amalgam lling from falling onto your tongue or down your
throat.
2. Request oxygen during the procedure. When amalgam llings
are removed, they must be drilled out. Tis can release mercury
vapor into the air. Te patients nose, being closest to this vapor,
can readily breathe it in. Your dentist should be able to provide
an oxygen tube directly to your nose so that you breathe in clean
oxygen rather than toxic vapor.
Once your amalgams are removed and replaced with a safe material,
you may also want to opt for chelation. Tis is not always necessary, but
is a way to get rid of any remaining mercury that may have gotten into
your body. Te most important thing to remember, however, is that the
amalgams need to be removed safely in the rst place.
If you are someone who is already dealing with cancer, unsafe removal
of amalgam llings may cause a worsening of your disease. In fact, if you
are currently using an alternative treatment that you believe is eectively
working on your cancer, you may not want to have your amalgams removed
until after you are cancer-free. But if you are nding that your alternative
cancer treatment is not working as eectively as you think it should, or if
you are a healthy person and just want to avoid a cancer diagnosis, then
seeking out a qualied dentist who knows how to safely remove silver
amalgam llings can be a great help to your health.
Nickel-Alloyed Porcelain Crowns
Although the toxicity of mercury in silver amalgam llings is becoming
more and more accepted, the toxicity of certain types of porcelain crowns
and their possible link to cancer is not so widely accepted. Yet, about 75
percent of all crowns, including porcelain crowns, contain nickel, which
is known to be an incredibly toxic substance and a powerful carcinogen.
Te way that porcelain crowns contain nickel is not in the white porcelain
covering itself, but in the stainless steel inner metal band that the porcelain
is bonded to for strength. What we arent generally told is that this stain-
less steel is usually alloyed with nickel. Te old-fashioned metal braces
(used for straightening teeth) were also generally a stainless steel nickel
alloy, and partial dentures often employ this form of alloy as well.
According to Dr. Eggleston, Nickel is not nearly as active as mercury,
however it corrodes and is far more carcinogenic. In fact, Dr. Eggleston
389 Toxic Teeth
states that the nickel alloys being used in dental practices today are actu-
ally quite similar to a form of nickel that is commonly used by cancer
research centers around the country to induce cancer in lab animals.
Two reported human cases involving nickel-alloyed porcelain crowns
are particularly disturbing. Te rst one involves kidney disease, and the
other involves breast cancer. Te rst story was a case of Dr. Egglestons
and is described by him. It involved a female patient who was admitted
to Long Beach Memorial Hospital with kidney disease. However, the
doctors attempting to treat her could not nd the cause of her kidney
problem. Her family physician then suggested special tests, which ended
up showing she was highly reactive to nickel. Te patients doctor then
asked her if shed had any dental work done in the past seven years. She
replied that she did have three porcelain crowns put in by her dentist. Te
doctor, knowing that porcelain crowns often have nickel-alloyed metal
jackets underneath, suggested she get the crowns removed right away. Te
patient did this, and all of her kidney failure symptoms went away.
Te other story involved breast cancer and was presented on one
Internet site as told by Dr. Hal Huggins. According to Dr. Huggins, he
came across a woman who had undergone a lumpectomy for breast can-
cer. While attending a support group for cancer in her area, she brought
up the subject of the possible link between nickel crowns and breast
cancer, since her husband had heard something about this from another
source. One of the other women in the group replied that she had gone
to a particular dentist down the street who had put nickel crowns in her
mouth, and a couple of years later she developed the same type of breast
tumor the rst woman had undergone a lumpectomy for. It turned out
that they both had gone to the same dentist, and both had gotten crowns
put in. Ten, these women found a third woman who had gone to the
same dentist, gotten a crown, and also developed the same type of breast
tumor. Amazingly, with a little more investigation, these women found a
fourth woman, a fth, and then a sixthall who had gone to the same
dentist, had one or more crowns put in, and who later came down with
the same type of breast tumor.
Coincidence? Possibly. It could also be that toxins or pesticides in that
geographical region were contributing to this type of breast cancer. But
the fact that there are thousands of articles that refer to nickel as a car-
cinogen make this sort of situation denitely worth investigating. How
many other women, or men, have paid dentists or orthodontists big money
to unknowingly promote cancer in their bodies?
390 oursxair \oui caxcii
As already pointed out, approximately 75 percent of the crowns placed
currently in peoples mouths in America contain nickel, which means that
about 25 percent of them dont contain nickel. Tis is partly because gold
alloys not containing nickel are also used sometimes as a metal base for
crowns. It is also partly because, in recent years, the hardening process for
porcelain used in dental applications has gotten better so that some crowns
now do not use any metal at all and, instead, are I00 percent porcelain.
So there is a chance that, if you have a porcelain crown in your mouth,
it might not contain nickel. But this could be worth calling your dental
oce about since, when nickel based crowns are used, the patient is gen-
erally not told this. And when asked directly, a common response from
your dentist or orthodontist might be that what youre getting is stainless
steel. Tis certainly sounds good, but if you want to be sure, you must
make it clear that you know stainless steel for dental work is generally
alloyed with some other metal and that you want to know specically if
the stainless steel in your mouth is alloyed with nickel.
If you are told that the crown in your mouth is gold-based, then
you are most likely better o. Gold in itself is not toxic or carcinogenic.
However, gold is way too soft to be used by itself in dental procedures
and is always alloyed with a stier metal for dental work. Terefore, you
must also be sure that you know what the gold in your mouth has been
alloyed with if you want to know whether it may be causing you illness
or not. As far as I know, gold alloyed with platinum is a common and
safe metal combination.
If you are unsure about the materials in your dental crown or crowns,
you might look into being tested for levels of nickel in your body as an indi-
cator. One way this can be done is through a hair analysis procedure.
Root Canals
So far, we have discussed silver-mercury amalgam llings and nickel-
alloyed crowns. Now, we come to the dental practice of administering
root canal procedures. Te very common practice of administering root
canals may unfortunately be one of the biggest dental problems today
because so many current dentists dont even know about the dangers
of this type of treatment. In other words, many intelligent dentists will
refuse to put mercury or nickel in peoples mouths, but they will go right
ahead and happily perform any number of root canals on their patients
without any idea of the damage these procedures can cause.
391 Toxic Teeth
Basically, a root canal is a procedure that is done when tooth decay or
infection has advanced so far that the nerve in the root area of the tooth
has become infected. Te root canal is a narrow canal that runs from
about the middle of the tooth down to the tips, or roots, of the tooth
which are rmly buried in the jawbone. Front teeth have a single root
into the jawbone and back teeth have two.
A healthy tooth contains a root canal that is lined with pink living
tissue lled with tiny blood vessels, all of which surround a main nerve
running down the center of the root and eventually connecting to other
nerves in the surrounding jaw. Once this nerve is infected, the patient
generally comes into the dentists oce in some degree of pain. Tis is in
contrast to the more common dental decay that is conned to the hard
shell of the tooth and is usually not painful because it does not involve
nerves. When the nerve area in the tooth is infected, the most common
procedure for the dentist to perform is called a root canal. In doing this,
the dentist removes the nerve and cleans out the entire root canal area,
which is usually infected as well to some degree. Ten, the inside of the
tooth is disinfected, lled with some form of lling material, and sealed
up again, usually with a crown on top.
Te positive side of the root canal procedure is that the tooth remains
in your mouth and does not have to be extracted. Tis allows the tooth
to remain functional for chewing purposes, as well as to look good
when you smile. On the negative side, the root canal-lled tooth is now
a dead tooth because the inside living tissue and the tiny blood vessels
that would normally bring nourishment to the tooth have been removed.
Almost all root canal procedures appear, on the surface, to be wonder-
ful solutions because rarely does the patient have any noticeable problem
with the tooth itself after the procedure is done. Most dentists enjoy the
fact that they rarely have a patient come back with complaints about a
root canal-lled tooth.
Te big problem, however, lies in the fact that the damage done by the
root canal procedure is almost never noticeable at the location of the tooth.
Tis of course is similar to the toxic eects of mercury from amalgams
and nickel from crowns. But at least we know that mercury and nickel
are extremely toxic substances, and we can test for those substances in
the body with hair analyses and other procedures. Side eects from a root
canal-lled tooth are much more dicult to pinpoint. Te irony of the
situation is that there may actually be more denitive research on the
dangers of the root canal procedure than there is on any other type of toxic
392 oursxair \oui caxcii
dental practice! But there is far less awareness of this research because it
has been largely ignored by the dental profession for over 75 years.
Te bulk of the research on root canal procedures was done between
about I900 to I925 by a respected dentist named Dr. Weston A. Price.
Dr. Price was a dedicated and thorough researcher who conducted meticu-
lous laboratory research with a 60-man team. Over a 25-year period he
conducted experiments on 5,000 lab animals after which he recorded
and published his results in a two-volume report totaling I,I74 pages.
Dr. Price also published 220 articles and two additional books, which
can be found in the dental and medical literature.
It is extremely unfortunate for all of us that few dentists today have
even heard of Dr. Weston Price and his research. In an eort to remedy
this lack of awareness a noted dentist, Dr. George E. Meinig, recently
undertook the mission of carefully reading all I,I74 pages of Dr. Prices
two-volume report. Dr. Meinig then condensed Prices ndings about
the dangers of root canals into a much smaller and easy-to-read con-
temporary book called, Te Root Canal Cover-Up. Dr. Meinig had the
perfect background and experience to do this because he, himself, had
practiced and taught root canal therapy, and was one of the founding
members of the American Association of Endodontists (root canal
practitioners).
According to Dr. Meinig, what Price and other researchers have been
able to prove is that there is an unavoidable problem with the root canal
procedure. Te problem is that, no matter how much a dentist tries to
disinfect the inside of the tooth after the root area has been cleaned out,
there is really no way that all of the infection can be reached. Tis is
because teeth contain microscopically small tubules that run through the
dentin like a huge lattice of caverns in a mountain. Te purpose of these
tubules when the tooth is alive is to transport nourishment-carrying uid
and oxygen throughout the tooth. Tus, a healthy tooth is very much
alive. To give you an idea of just how extensive this lattice of tubules is,
it is estimated that if you were able to string all the tubules from just one
average front tooth together, end-to-end, they would reach about 3 miles
long. And since back teeth are much larger than front teeth, their tubules
placed end-to-end would reach considerably farther.
Once infection has progressed into the depths of these microscopically
small tubules in any tooth, there will inevitably be a certain number of
bacteria that have roamed so deep that no disinfectant can reach them.
So there will invariably be some number of bacteria that are still left alive
393 Toxic Teeth
in the tubules of the dentin after the root canal procedure is done and
the tooth is lled and closed back up again.
But the root canal-lled tooth is now dead. Tere is no longer a supply
of nourishment going in and out of the tooth, and there is no longer any
uid owing into and out of the tubules. Without uid owing through
the tubules, there is no mechanism for transporting antibiotics to the
trapped bacteria. More importantly, there is no longer any transport of
oxygen throughout the intricate maze of tubules. So the bacteria, which
started out as normal aerobic bacteria, may now mutate to survive and
become anaerobic bacteria. Unfortunately, the anaerobic forms of these
bacteria can be much more dangerous than the aerobic form originally
was and Dr. Price discovered that the entombed anaerobic bacteria are
capable of creating powerful toxins that can then leak into the tissue sur-
rounding the tooth. Once these toxins leak out of the tooth, they can get
into a persons bloodstream and travel throughout the entire body.
Back in the early I900s, after suspecting that some of the chronic ill-
nesses of his patients were linked to root canal-lled teeth, Dr. Price started
extracting those teeth. Ten, by simply taking a piece of the extracted
root canal-lled tooth and embedding this piece of tooth under the skin
of a rabbit, he found that the rabbit would develop the same type of ill-
ness the person had!
For instance, Dr. Price found if he took a small piece of a root canal-
lled tooth that had been extracted from a person whod had a heart
attack and placed it under the skin of a rabbit, that rabbit would die of
a heart attack in about I0 days. He could then take that same piece of
tooth out of the dead rabbit and put it under the skin of another rabbit,
and in about I0 days, that rabbit would also die of a heart attack. Price
found he could do this over and over with the same piece of tooth and
get the same result for up to about 30 rabbits.
Moreover, heart disease only occurred in Prices lab animals when the
person the root canal-lled tooth had come from had suered from heart
disease. If the person had suered from another illness, that would be
the illness that would show up in the rabbit. For instance, if the patient
from whom the tooth was taken was suering from kidney disease, then
the rabbit with the piece of that persons tooth embedded in it would also
develop kidney disease.
Dr. Prices rst clinical case involved arthritis. In that case, he removed
a root canal-lled tooth from a woman with severe arthritis and implanted
the extracted tooth under the skin of a rabbit. Within 48 hours, the rabbit
394 oursxair \oui caxcii
had developed crippling arthritis. Furthermore, after extraction of this
tooth, the womans arthritis improved dramatically. Dr. Price performed
these types of experiments over and over, and kept getting the same results.
Very rarely, did the rabbit not come down with the very illness the human
patient was suering from.
Price was a thorough researcher and he, of course, tested the possibility
that just putting part of a human tooth into an animal was the problem.
But he found that if he did the same procedure using a perfectly healthy,
non-root-canal-lled tooth, then the rabbit would suer no ill eects
whatsoever. He also found that if he sterilized the piece of root canal-lled
tooth rst by using a powerful procedure involving steam heat, then the
rabbit would suer no ill eects, either.
Dr. Price found a high number of chronic degenerative diseases to be
linked to root canal-lled teeth. Te most common appeared to be vari-
ous forms of heart and circulatory diseases, presumably because the toxins
from anaerobic bacteria in the teeth leaked into and circulated through-
out the bloodstream. Other chronic conditions that his research linked
to root canal-lled teeth were various forms of arthritis, nervous system
disorders, and even digestive disorders. For more detailed information
about Prices discoveries regarding the toxic nature of root canal-lled
teeth, I highly recommend Meinigs book, Root Canal Cover-Up.
A poignant description of the root canal procedure was given by
Dr. Hal Huggins in a lecture he gave to the Cancer Control Society in
I993. Huggins stated, in his usual colorful way,
. . . Ten we get into the root canal business, and that is the most
tragic of all. Isnt there something you can put in the center of the canal
that is safe? Yeah, there probably is, but that is not where the problem is.
Te problem with a root canal is that it is dead. Lets equate that. Lets
say you have got a ruptured appendix, so you go to the phone book, and
who do you look up? Lets see, we have a surgeon and a taxidermist, who
do you call? You going to get it bronzed? Tat is all we do to a dead tooth.
We put a gold crown on it, looks like it has been bronzed. It doesnt really
matter what you embalm the dead tooth with, it is still dead, and within
that dead tooth we have bacteria, and these bacteria are in the absence of
oxygen. In the absence of oxygen most things die except bacteria. Tey
undergo something called a pleomorphic changelike a mutation. Tey
learn to live in the absence of oxygen (and) now produce thioethers, some
of the strongest poisons on the planet that are not radioactive.
395 Toxic Teeth
Huggins went on to say in this lecture that the thioethers do escape
into the bodys bloodstream and he points out a correlation between the
increase in the rate of heart attacks in the United States since the early
I900s, and the corresponding increase in the practice of performing
root canals. Tis would be consistent with what Dr. Price found in his
research, which was that the predominant damage caused by root canals
was to the cardiovascular system of the body since the mode of travel for
the toxins is through the bloodstream.
Te main problem in accepting the dangers of root canals over the years
has been expressed in a debate over the focal infection theory. Tis is
the theoretical idea that an infection focused in one part of the body can
have a detrimental eect on a distant part of the body. Even though this
debate continues, there are some transplant surgeons today who require
root canal-lled teeth to be extracted before they will perform an organ
transplant in a patient. Tis is because these surgeons believe there is a
risk that focal infections in teeth might aect the new organ.
Josef Issels, M.D., of Germany, a world-famous cancer specialist, took
the dangers of root-lled teeth very seriously. Dr. Issels was probably
the rst physician to require all of his cancer patients to have their dead
teeth extracted as a part of his normal cancer treatment protocol. Over a
40-year period of working with more than I6,000 cancer patients, Issels
had one of the highest total remission rates with late stage terminal can-
cer patients of any cancer practitioner. He also found that a survey of his
cancer patients showed over 90 percent of them to have between two
and I0 dead teeth in their mouths when they rst arrived at his clinic
for treatment.
In his well-written, in-depth book, CancerA Second Opinion, Dr. Issels
talks about his research with root canals. In Chapter 8, titled Focus on
Foci, Issels found that dead teeth left in the mouth can become toxin
factories and do, in fact, produce thioethers. Moreover, he presents very
convincing evidence that thioethers have all of the qualications of a
substance capable of causing spontaneous cancer in humans.
Dr. Isselss writing is highly technical, and he uses medical terminol-
ogy that is often dicult for the layperson to understand. But one simple
experiment he reports is quite clear and impressive. Issels found that he
could use an infrared-sensitive instrument to measure the level of infra-
red emission anywhere in a persons body. In doing so, he found that the
infrared emission on the outer skin next to a root canal-lled tooth was
396 oursxair \oui caxcii
elevated slightly higher than the area around healthy teeth. He could also
monitor the infrared emission around a cancerous tumor area.
What Dr. Issels found was that, when a dead tooth in a cancer patient
was treated (presumably by extraction), the corresponding infrared emis-
sion of that area of the mouth decreased, and the infrared emission of the
persons tumor area also decreased at the same time. Tus, he proved a
denite interrelationship between the dead tooth and the cancer.
Yet another possible relationship between root canal-lled teeth and
cancer may have to do with a dierent mechanism than toxins. Tis
mechanism involves acupuncture meridians. Although little research has
been done on this subject, one alternative cancer practitioner, Dr. John
Diamond of Reno, Nevada, has said, I have a number of patients with
breast cancer, all of whom had root canals on the tooth related to the
breast area on the associated energy meridian. Tis is certainly some-
thing to think about for anyone with any type of cancer.
Of course, we all know people who have root canal-lled teeth in their
mouths and appear to be perfectly healthy. Tis seems to confuse the issue.
One alternative doctor claried this issue in the following way. He said,
Root canals are like mortgages. As long as you can make enough money
to pay the payment every month, everything is ne. But once you cant
make the payment, then youre in big trouble! In other words, it is the
strength of the immune system and the body in general that determines
whether or not a root canal-lled tooth is going to bring about obvious
health problems in any individual. Tis could be applied to the eects of
mercury amalgam llings and nickel-alloyed crowns as well. With diet,
stress levels, and other factors varying greatly from person to person, the
eects of these dental practices are necessarily going to vary from person
to person also.
As with amalgam removal, having your root canal-lled teeth removed
safely is of utmost importance. If your dentist or oral surgeon does not
fully understand the issues of toxicity, there could be a danger that after
the dead tooth is removed, toxic infection still remains in the surrounding
bone socket. Once more, seeking out a competent biological dentist who
knows how to safely extract root canal-lled teeth is a good idea. On pages
I93I94 of his book, Root Canal Cover-Up, Dr. Meinig details how a root
canal-lled tooth should be removed to ensure that none of the infection
is left behind, and it might be a good idea to make sure your dentist or
oral surgeon is familiar with those instructions in Meinigs book.
Although it is common practice for endodontists to leave behind the
397 Toxic Teeth
periodontal ligament when a tooth is extracted, Dr. Meinig and Dr. Hal
Huggins both believe it is likely for root canal infections to have infected
this ligament as well. Tey both recommend total removal of this ligament
along with approximately I millimeter of surrounding jawbone following
extractions. Tis procedure usually causes any residual infection from the
root canal-lled tooth to be removed.
One last word of caution is warranted. Some alternative cancer spe-
cialists recommend that people who are in a weakened state from cancer
may not be strong enough to have all of their toxic teeth dealt with at
once. For some people, it might be best to have toxic teeth addressed
slowly, over time. Again, consulting with a knowledgeable alternative
cancer specialist, if possible, is a good idea.
Resources:
Books
Hal A. Huggins, D.D.S. Its All in Your Head: Te Link Between Mercury
Amalgams and Illness. Garden City Park, New York: Avery Publishing
Group, 1993.
George E. Meinig, D.D.S, F.A.C.D. Root-Canal Cover-Up. Ojai, Cali-
fornia: Bion Publishing, 1998.
Josef Issels, M.D. CancerA Second Opinion. Garden City Park, New
York: Avery Publishing Group, 1999.
Websites
www.curezone.com/dental/root_canal.html
www.price-pottenger.org
www.whale.to/d/cancer.html
www.yourhealthbase.com/amalgams.html
399
22
Evaluating Conventional Methods
A
re conventional cancer treatments ever warranted? Yes. For instance,
surgery alone may sometimes be a curative approach when a tumor
is localized and caught early. Other situations may warrant some amount
of conventional treatment as well. For instance, if a persons tumor is so
large that it is restricting a vital organ, or if the cancer is so advanced
that there is not enough time left for an alternative treatment to have
a chance to work, then immediate surgery, chemotherapy, or radiation,
may be used to ones advantage. However, this is often simply short-term
damage control. When it comes to long-term recovery, the ecacy of
toxic conventional treatments is a dierent story.
Te current medical establishment would like us to believe that most
cancers, if caught early, are curable with standard medical techniques.
Impressive-sounding conventional cure-rate statistics are advertised. But
these statistics are achievable only after gross statistical manipulations
have been done, and after key terms like cure have been re-dened.
To review from Chapter I, the following are six major ways that ocial
cancer cure-rate statistics are often fudged so that conventional methods
for treating cancer can look better than they really are:
I. By re-dening cure as alive ve years after diagnosis, instead of using
the words real meaning, which is cancer-free.
400 oursxair \oui caxcii
2. By simply omitting certain groups of people, such as African Ameri-
cans, or by omitting certain types of cancer, such as all lung cancer
patients, from the ocial statistical calculations.
3. By including types of cancer that are not life-threatening and are easily
curable, such as skin cancers and DCIS.
4. By allowing earlier detection to erroneously imply longer survival.
5. By deleting patients from cancer treatment studies who die too soon,
even if that is on day 89 of a 90-day chemotherapy protocol.
6. By using a questionable adjustment called relative survival rate.
Te problem is that if you are dealing with life-threatening cancer, the
misleading ocial statistics are the numbers that will be oered to you as
representative of your chances of survival, should you choose conventional
treatment. It is critical that you understand how to accurately evaluate
conventional cancer treatment methods because your life literally depends
on the treatment decisions you make.
Te Big TreeSurgery, Chemotherapy, and Radiation
What are the real statistics on conventional medicines big three
cancer treatments today? Unfortunately, nobody knows. Nobody can
know when there are no data in mainstream medicine that reect real
cures. Te only data we have to work with are gures that reect the
phony re-denition of the term cure, that talk about short-term results,
and that are recorded selectively in the rst place in ways that defy cor-
rect statistical methodology. Tus, trying to gure out the true cure-rate
statistics for conventional cancer treatments is a lot like trying to gure
out which cup the magicians red ball is under.
Having said that, there are a number of things you can learn about
conventional cancer treatment ecacy. For instance, out of all the con-
ventional cancer treatments available today, it is probably safe to say that
surgery alone has the best track record. Cancer researcher, Dr. Ralph
Moss, claims that most of the conventional cancer cures today can be
attributed to surgery alone. However, the types of cases where surgery
can be eective in a long-term way apply to only a small percentage of
cancer patients. For instance, everyone agrees that surgery is virtually
helpless as a curative procedure in any case where the cancer has already
401 Evaluating Conventional Methods
metastasized, and unfortunately, the majority of cancer patients are told
they have metastasized cancer at the time they are rst diagnosed.
Tus, for most people with cancer, surgery is no more than a palliative
treatment (meaning it cannot save the patient, but is merely performed
in the hope that it will buy the patient some time). For surgery to have
a chance at actually being curative, it must be performed at a very early
stage, before the cancer has spread past the primary site. Even for many
of these cases, surgery cannot guarantee recovery. Some medical experts
believe that there are early cancer situations where surgery may even cause
the cancer to spread throughout the body by releasing free-oating cancer
cells into the bloodstream or lymph system. But overall, the use of surgery
alone probably still accounts for the largest number of long-term survival
cases in conventional cancer treatment. And the best chance for long-term
recovery through surgery may be when an entire organ can be removed
(such as the thyroid gland, prostate gland, uterus, ovaries, etc.)
After surgery, we have radiation and chemotherapy. Unfortunately, the
true long-term eectiveness of these methods can only be seen as dismal.
Some studies have even produced evidence that cancer patients may be
able to live longer without these treatments. For example, a Science News
article, published August I, I998, presented a review of data about radia-
tion treatment after surgery for lung cancer. Te immense amount of
data, which was collected from nine studies over a 30-year period, actu-
ally showed the two-year survival rate after lung cancer surgery to be 48
percent for patients who got post-surgical radiation treatments, and 55
percent for patients who underwent surgery alone. In other words, more
patients who did not receive radiation treatments after surgery lived to
the two-year mark than those who did receive radiation after surgery.
When it comes to chemotherapy, which is prescribed to about four out
of ve people with cancer in the United States today, Ralph Moss states
in his book, Questioning Chemotherapy:
A close look at chemotherapy yields some major surprises. Few would
dispute its usefulness in acute lymphocytic leukemia, Hodgkins disease,
testicular and ovarian cancer, and a handful of rare tumors, mainly of
childhood. But evidence for the life-prolonging eect in other common
malignancies is weak, even for those cancers in which almost certainly
it has some marginal success. And proof is simply non-existent for the
majority of cancers, especially the advanced carcinomas.
Even for the common cancers in which chemotherapy works, such
as small-cell lung cancer, the actual survival benet is reckoned in weeks
402 oursxair \oui caxcii
or months, not in years. And during this time, the patient is likely to
experience major, even life-threatening side eects from the treatment.
Tus, the overall advantage to the patient is moot.
Tus, the ocial claims of success for toxic treatments such as radiation
and chemotherapy often refer to short-term eectiveness only. We will
be going into more detail about radiation and chemotherapy in the next
few pages, but rst, lets look at the very important dierence between
short-term and long-term eectiveness.
Short-Term Versus Long-Term Eectiveness
Studying and quoting short-term eectiveness is just one tactic of a
medical establishment that is not having success with long-term eec-
tiveness. Since mainstream medicine is losing its war on cancer, it is very
benecial for those in charge to only study short-term eectiveness. Tis
way, the actual long-term eectiveness (or real eectiveness) of conven-
tional treatment does not have to be considered. Better yet, long-term
side eects of treatment (which may kill the patient a few years down the
line) do not have to be considered.
For example, in Chapter I9, we saw that many European studies
showed the use of Tamoxifen for breast cancer to have no overall long-
term survival benet at all. According to Dr. Lee, Tamoxifen can tem-
porarily suppress tumors, and that is why the short-term studies done in
the United States made Tamoxifen look so good. However, the long-term
studies done on Tamoxifen in Europe showed breast tumors coming back
at just about the period of time when the studies in the United States were
being cut short. Te short-term U.S. studies did not show all the deaths
caused by Tamoxifens side eects later, such as from fatal blood clots in
the lungs, stroke, liver dysfunction, or from uterine cancer, all of which
can be directly caused by the Tamoxifen drug treatment.
But the most ludicrous aspect of short-term attention to conventional
treatments is represented by how the term cure is re-dened. By re-
dening the meaning of cure as alive ve years after diagnosis, our cur-
rent conventional cancer establishment is basically saying that the medical
establishment considers ve-year survival to be the best they can aspire
to. Make no mistakeby labeling anyone with cancer who reaches the
ve-year mark as cured, conventional medicine is proclaiming that once
you have lived ve years after diagnosis, they have done a great jobeven
403 Evaluating Conventional Methods
if you still have cancer and have been miserably sick the whole ve years.
Tis ocial tactic of re-dening the word cure also frequently creates
the ironic situation where a cancer patient can be listed as cured in the
ocial statistics data base, yet die from their cancer a short while later!
Maybe for some people, living another ve years is a great thing. For
instance, it may be wonderful for those who are quite elderly when they
are diagnosed with cancer, and they just want to live a few more years.
But what if you are 25 or 40 years old, or 50 or 60? Living only ve
more years is not good at all! Or maybe you are one of many people rais-
ing small children when you are diagnosed with cancer. Most parents do
not just want to see their children become teenagersthey also want to
see them become adults, go to college, get married, have their own chil-
dren, and so forth. And if it is your child who has been diagnosed with
cancer, then to aspire to your child living just ve more years is simply
unacceptable.
One of the most important things to know when considering treatment
for cancer is whether or not the statistics your oncologist presents to you
reect long-term or short-term eectiveness. After all, you obviously
want a long-term, not a short-term, recovery!
Response Rates
One way that short-term results are used by mainstream medicine to
imply long-term eectiveness is by the common conventional practice of
studying and quoting cancer treatment response rates. In mainstream
medicine, the response rate of a particular treatment is often quoted
as if it means recovery rate, or cure rate. But this is just another way that
people seeking cancer treatment are misled by meaningless numbers.
Te phrase response rate is not synonymous to recovery rate or cure
rate. Quite the contrary. Common conventional cancer studies dene a
response as simply meaning a 50 percent reduction in tumor size over
a particular period of time (usually about 28 days).
Because chemotherapy and radiation are cytotoxic (toxic to cells),
it is easy to make malignant tumors shrink for a time when bombarded
with these types of toxic treatments. However, that merely means that
the tumor has died a little after being poisoned or burned. If there are
any cancer cells left alive after the treatment, which there virtually always
are, then the tumor will start growing again as soon as there is a break
in the treatment. Since toxic treatments generally involve time breaks in
404 oursxair \oui caxcii
their administration to let the patients overall body recover, cancerous
tumors often have a chance to grow back.
Tus, when tumor response rates are quoted, these rates do not indicate
that patients regained their good health or their cancers were overcome.
Response rates are just a convenient way for conventional cancer research-
ers to report the short-term partial eectiveness of a particular treatment.
As Ralph Moss, Ph.D. states,
It is one of the central fallacies of chemotherapy that shrinkages or
response rates have been proven to correlate with increased survival
time. Yet, in answer to a patients inevitable question, What are my
chances? the doctor may give impressive-sounding response rates of,
say, 60 percent.
In other words, if your doctor tells you that the cancer treatment he
or she is recommending to you has a response rate of 60 percent, you
should know that what that really means is this: 60 percent of the time,
that particular treatment protocol will cause tumors to shrink by at least
half for at least a month. It does not mean that 60 percent of the cancer
patients who get that treatment will become cancer-free.
Since toxic cancer treatments can often damage vital organs and sup-
press the immune system, the use of toxic treatments that are unable to
eect a long-term cure must always beg the question as to whether or not
the patient might have lived longer without the treatment. W. John Dia-
mond, M.D., and W. Lee Cowden, M.D., report on this issue in their book,
An Alternative Medicine Denitive Guide to Cancer. In it, they write:
Virtually all the FDA-approved anticancer drugs are markedly immu-
nosuppressive, because they ruin a persons natural resistance to disease,
including cancer. Ulrich Abel, Ph.D., of the Heidelberg Tumor Center
in Germany, conducted a comprehensive review of the world literature
on survival among cancer patients receiving chemotherapy. He found
that chemotherapy can help only 3 percent of the patients with epithe-
lial cancers (e.g., cancers of the breast, lung, prostate, and colon). Tese
cancers account for about 80 percent of all cancer deaths. In a study of
chemotherapy-treated breast cancer patients, the researchers concluded,
Survival may even have been shortened in some [breast cancer] patients
given chemotherapy.
A few pages later, Dr. Diamond and Dr. Cowden follow with:
German cancer researcher Ulrich Abel, Ph.D., observes that the
405 Evaluating Conventional Methods
temporary shrinking of a tumor massdened as either a partial or
complete remissionis not necessarily a good sign, because the remain-
ing tumor cells often grow much faster and more virulently after the
rst series of chemotherapy treatments. Highly aggressive chemotherapy
actually shortens survival times compared with patients in whom che-
motherapy was delayed or administered less aggressively, says Dr. Abel.
Paradoxically, patients whose tumors showed no response to chemotherapy
actually survived longer than patients who did respond.
Dr. Diamond and Dr. Cowden also report on evidence that some
men with prostate cancer may survive longer without radiation treat-
ments. Tey write:
Radiation therapyimplanting radiation seeds in the prostate gland
routinely given for early signs of prostate cancer can actually hasten the
development of that cancer. Prostate cells can double in as little as I.2
months after radiation treatment while unradiated prostate cancer cells
may take an average of 4 years to double.
It is extremely misleading for doctors to allow cancer patients to believe
that quoted response rates are the same as recovery rates. It may be
that many doctors who quote response rates dont know, themselves, the
real meaning of what they are quoting. But for you, the person trying to
get well, knowing the real meaning of response rate statistics will help you
to more correctly evaluate treatment methods you may be considering.
Damage to the Heart
Tere are many ways that short-term eectiveness of conventional
cancer treatments can look very good for a while, yet long-term eective-
ness turns out to be not good at all. For instance, radiation to the chest
area for either lung cancer or breast cancer can cause damage to the heart
severe enough to cause a fatal heart attack at some point in the future. If
the heart attack does not occur until the patient has been pronounced in
remission, then the radiation treatment will look like it was successful.
Deaths from subsequent heart attacks caused by cancer treatment do
not have to be folded into the cancer treatment statistics. As mentioned
in Chapter I9, one study on radiation treatment given to women with
breast cancer showed that the use of radiation did reduce deaths from
breast cancer by I3.2 percent, and this was most likely the gure that
406 oursxair \oui caxcii
was publicly advertised. However, this same radiation increased deaths
from other causes (mostly heart failure) by 2I.2 percent!
Can Radiation or Chemotherapy Cause Cancer?
One fact that is often dicult for many people to believe is that many
of the conventional treatments for cancer commonly used today are actu-
ally carcinogenic. Tis means they can cause a secondary cancer to develop a
few years later, provided that the patient is lucky enough to survive their
rst cancer that long. Tis is just another way that short-term eectiveness
of conventional cancer treatments may look good, while the long-term
eectiveness may not look good at all.
Radiation-Induced Cancer
Evidence that radiation treatments can cause cancer goes back to
the early days of X-ray technology. In Te Cancer Industry, Ralph Moss
reports:
In I902 a German doctor recorded the rst case of human cancer
caused by radiation: the tumor had appeared on the site of a chronic
ulceration caused by X-ray exposure. Experimental studies performed
in I906 suggested that leukemia (cancer of the blood) could be caused
by exposure to the radioactive element radium. By I9II, 94 cases of
radiation-induced cancer had been reported, more than half of them
(54) in doctors or technicians. By I922, over I00 radiologists had died
from X-ray-induced cancer, and many other research workers, laboratory
assistants, and technicians had also succumbed. . . .
More and more cases of people developing cancer due to X-ray tech-
nology were reported in the early to mid-I900s. Ten, when radiation
started being used as a treatment for cancer, secondary radiation-induced
cancers began to be reported. Today, it is well-known that radiation treat-
ments for cancer may also cause secondary cancers.
In her video, Cancer Doesnt Scare Me Anymore, Dr. Lorraine Day
shows medical manuals that list the possibility of secondary cancers due
to radiation treatment. She also talks about the many other serious and
life-threatening side eects that can be caused by radiation treatments
for cancer. Dr. Day makes the point that the ACS, AMA, and FDA
refer to radiation treatments as safe and eective for cancer patients,
407 Evaluating Conventional Methods
yet radiation technicians, doctors, and nurses are all urged to protect
themselves against much lower, indirect doses of the same radiation by
wearing lead vests and carrying out other protective measures. In other
words, it is quite ironic that extremely high exposure to directed radia-
tion is considered safe for anyone with cancer, yet low indirect exposure
is considered extremely dangerous for healthy radiation technicians!
All oncologists are well aware of radiation-induced secondary cancers
in patients. An example is the real-life case of one woman who was able
to successfully beat her breast cancer only to nd herself facing another
life-threatening cancer I0 years later. Tis time, she was facing inoper-
able metastasized lung cancer that her oncologist was convinced had
been caused by the radiation treatments to her breast years before. Tus,
while radiation treatments may be necessary in some cases where cancer
is extremely advanced and needs to be reduced quickly, they are never
without risk. Understanding this and only using radiation when absolutely
necessary is important.
Chemotherapy-Induced Cancer
Many people are already aware that some sources of radiation can cause
cancer because they have heard reports of cancer resulting from nuclear
fallout, radiation accidents, and so forth. But it seems counter-intuitive
that a carcinogenic drug would be intentionally given to someone trying
to recover from cancer. A brief look at the history of chemotherapy will
help to shed light on this.
Te roots of modern chemotherapy go back to the early I940s when
poisonous mustard gas was being developed for chemical warfare. A potent
form of mustard gas had already been used during World War I and, in
I942, the U.S. government contracted with various research centers to
further investigate possible war-time chemical agents. Researchers at Yale
University experimented with substituting a nitrogen atom for a sulfur
atom in mustard gas, which, at the time, was called nitrogen mustard.
A Yale anatomist then came up with the idea that it would be interesting
to inject this nitrogen mustard into mice with cancer to see what would
happen.
As luck would have it, the rst such mouse experimented on showed
impressive tumor regression. Although the mouses cancer never com-
pletely went away, the mouse lived about four times longer than it was
expected to live with no treatment at all and this got peoples attention.
408 oursxair \oui caxcii
Researchers followed with more experiments and, though they could
not achieve similarly good results on subsequent mice, it was eventu-
ally decided to try the nitrogen mustard treatment on a human cancer
patient.
Te rst man experimented on had late-stage lymphosarcoma. Like the
rst mouse, he showed dramatic tumor regression after receiving nitrogen
mustard. Researchers were ecstatic. But as with all the mice, the mans
cancer was never cured. Within the rst month of treatment, his white
blood cell count fell dismally low. Ten his cancer regenerated in his
bone marrow and he died.
But because the mans tumor had regressed
within the rst few days, his case was considered to have been a success.
One-hundred-sixty more cancer patients were then administered experi-
mental chemotherapy. Te results showed that not one of these patients
recovered from their cancer. In other words, all the evidence from early
chemotherapy experiments indicated that the use of chemotherapy to
treat cancer was an unqualied failure!
But in the early I940s nitrogen mustard was the only synthesized
chemical agent that had ever shown anti-tumor activity, and some people
in positions of power were too excited about this to let it go. Chief of the
U.S. Army Chemical Warfare Service, Cornelius Dusty Rhoads, was
one of these people. Rhoads became a powerful advocate of chemotherapy
when World War II ended and he became head of the Memorial Sloan-
Kettering Institute for Cancer Research. He initiated tests on more than
I,500 dierent types of nitrogen mustard, and by I955, about 20,000
of these types of chemicals were being looked at every year.
Because chemotherapy was developed out of poisonous chemical warfare
agents (and is still poisonous), there has always been a ne line between
giving a therapeutic dose and killing the patient. In his outstanding book,
When Healing Becomes a Crime, author Kenny Ausubel notes that in one
clinical trial on the chemotherapy drug called ICE, 8 percent of the
patients died from the drug treatment directly, and in another trial on a
chemotherapy drug studied for leukemia, 42 percent of the patients died
from the drug treatment directly.
From the days when chemotherapy was rst used to the current day,
this mode of treating cancer has never shown signicant long-term eec-
tiveness. Dr. Dean Burk was a chemist at the National Cancer Institute
from I939 to I974. He also taught biochemistry at Cornell University
Medical School from I939 to I94I. When he retired in I974, Dr. Burk
left the position of chief chemist at the National Cancer Institute. Te
409 Evaluating Conventional Methods
year before he retired, Dr. Burk wrote a letter to Dr. Frank Rauscher, a
higher-up member in the NCI. In it, Burk wrote:
Ironically, virtually all of the chemotherapeutic anti-cancer agents
now approved by the Food and Drug Administration for use or testing
in human cancer patients are (I) highly or variously toxic at applied dos-
ages; (2) markedly immunosuppressive, that is, destructive of the patients
native resistance to a variety of diseases, including cancer; and (3) usu-
ally highly carcinogenic [cancer-causing]. . . . Tese now well established
facts have been reported in numerous publications from the National
Cancer Institute itself, as well as from throughout the United States and,
indeed, the world. . . .
In your answer to my discussion of March I9, you readily acknowl-
edged that the FDA-approved anti-cancer drugs were indeed toxic,
immunosuppressive, and carcinogenic, as indicated. But then, even in
the face of the evidence, including your own White House statement
of May 5, I972, all pointing to the pitifully small eectiveness of such
drugs, you went on to say quite paradoxically it seems to me, I think the
Cancer Chemotherapy program is one of the best program components
that the NCI has ever had.. . . One may ask, parenthetically, surely this
does not speak well of the other program areas?
Ralph Moss claries the subject of chemotherapy being carcinogenic
even further in his book Questioning Chemotherapy, where he writes:
Perhaps the strangest thing about chemotherapy is that many of
these drugs themselves are carcinogenic. Tis may seem astonishing to
the average readerthat cancer-ghting drugs themselves cause cancer.
Yet this is an undeniable fact.
It is sometimes said that only the alkylating agents, such as busulfan,
carmustine, and melphalan, are carcinogenic. But this is not true. Te
authoritative International Agency for Research on Cancer (IARC) has
identied 20 single agents or regimens which cause cancer in humans,
and about 50 more in which such eects are suspected (236,248). Many,
but not all, of these are alkylating agents. Te oending drugs include
doxorubicin and streptozocin (toxic antibiotics used as cytotoxic agents),
BCNU (a nitrosourea), as well as the various hormone-like products.
Perhaps the distinction between alkylating agents and other drugs in
this regard is moot, since alkylating agents are predominantly included
in most of the regimens commonly used in cancer.
To give just one example of carcinogenicity, doctors looked at one-year
survivors of ovarian cancer from ve randomized trials. Te incidence
rates for acute nonlymphocytic leukemia and for pre-leukemia were about
410 oursxair \oui caxcii
I00 times more common in women who got the drug melphalan than
in those who received no chemotherapy.
Te magnitude of these risks suggests that the drugs are causally
related to leukemia, NCI epidemiologists cautiously concluded. However,
they add, characteristically, that the identication of a carcinogenic eect
does not preclude its use for treatment in patients. In other words, the
fact that these drugs cause cancer is immaterial in the doctors decision
to administer these cytotoxic agents.
Using my home copy of Te PDR Family Guide to Prescription Drugs
(New Second Edition, copyright I994), I looked up one commonly used
chemotherapy drug called Cyclophosphamide, which is also referred
to as Cytoxan. On page I67 of the Physicians Desk Reference, where
side eects of Cytoxan are listed, I found this statement: One possible
Cytoxan side eect is the development of a secondary cancer, typically
of the bladder, lymph nodes, or bone marrow. A secondary cancer may
occur up to several years after the drug is given.
Cyclophosphamide, or Cytoxan, is an alkylating agent. It is also an
integral part of the following commonly used chemotherapy protocols:
BACOP CHOP COMLA MACC
CA CHOP-B COP M-BACOD
CAMP CISCA COP-BLAM Pro-MACE
CAP CMF CVP Pro-MACE-cytaBOM
CAV CMFP CyVADIC
CFPT CMFVP FAC
COAP Hexa-CAF VAC
Cyclophosphamide is also known as Neosar in the United States and
Endoxan in Germany. According to Dr. W. John Diamond,
A study of over I0,000 patients shows clearly that chemos supposedly
strong track record with Hodgkins disease (lymphoma) is actually a lie.
Patients who underwent chemo were I4 times more likely to develop leu-
kemia and 6 times more likely to develop cancers of the bones, joints, and
soft tissues than those patients who did not undergo chemotherapy.
And, the March 2I, I996, issue of the distinguished New England
Journal of Medicine, reported:
Children who are successfully treated for Hodgkins disease are I8
times more likely later to develop secondary malignant tumors. Girls
411 Evaluating Conventional Methods
face a 35 percent chance of developing breast cancer by the time they
are 40which is 75 times greater than the average. Te risk of leukemia
increased markedly four years after the ending of successful treatment,
and reached a plateau after I4 years, but the risk of developing solid
tumors remained high and approached 30 percent at 30 years.
Some people may be willing to take the risk of developing a secondary
cancer from the treatment they receive to rid themselves of their current
cancer. But other people might not like the idea of seeing their cancer go
into remission only to have to go once again into battle a few years later
against a secondary treatment-induced cancer. (Especially when there are
non-toxic, non-carcinogenic treatments they could choose from.) Do not
assume your oncologist will tell you whether or not the chemo he or she
wants to prescribe to you is carcinogenic or not. Generally, this subject
is not addressed at all.
Also, the fact that so many chemotherapy drugs actually cause cancer
is a very real threat to the public at large as well as to the environment.
When cancer patients receive chemotherapy, much of their drug treat-
ment gets passed into the public sewage systems through their urine. It
thereby becomes an environmental poison that may eventually cause
health problems or cancer to occur in other humans or animals. Remem-
ber, whenever we put poisons in ourselves, we are putting them in the
environment, too.
False Hope?
How many times are doctors prescribing chemotherapy or radiation
when there is very little evidence that this type of treatment will improve
long-term life expectancy? About 80 percent of all cancer patients today
are given chemotherapy, yet some researchers believe that chemotherapy
may only show long-term eectiveness in as little as 2 to 3 percent of all
cancer cases. And how often are radiation treatments prescribed to cancer
patients when there is little evidence that doing so will help achieve long-
term recovery for their particular type of cancer situation?
I know of a woman whose elderly father-in-law was prescribed radia-
tion treatments for his late-stage, metastasized prostate cancer. When
this woman called her father-in-laws oncologist directly to nd out what
his life-expectancy was, she was told by the oncologist that he had only
about six months to live. Te woman, being a clear thinker, then asked
the oncologist if that prognosis for her father-in-law was with radiation
412 oursxair \oui caxcii
treatments, or without. Te unbelievable answer she got was either way.
Yet her father-in-law had been prescribed radiation treatments and was
not told that his survival chances were exactly the same whether he did the
treatment or not. Both this elderly man and his wife thought the radiation
treatments could cure him. Tese people were never told the truth, but
instead were given false hope by their conventional oncologist.
I believe that the following statements are accurate: It is false hope when
patients are prescribed a conventional cancer treatment and not told that
the treatment is only considered to be palliative (not expected to cure the
patient). It is false hope when response rates are quoted and presented in a
way that implies long-term recovery. And it is false hope when any cancer
cure-rate statistic that has been fudged is presented to a cancer patient
as representative of his or her chances for real recovery and survival. Since
all these things happen on a daily basis in conventional oncologists oces,
the logical conclusion is that conventional medicine is the biggest source
of false hope given to cancer patients today.
Does Newer Mean Better?
It is wrong for the mainstream medical establishment to mislead
patients about the actual long-term eectiveness of conventional cancer
treatments. But one thing that plays into this problem is the readiness of
the public to think that anything newer is better. One of the most
distressing patterns I have come across when talking to people who have
recently been diagnosed with cancer, is their frequent willingness to over-
look the proven long-term eectiveness of many alternative, non-toxic
cancer treatmentsand to eagerly look for the most recent conventional
cancer drugs or procedures for their healing instead. I have heard people
say things like, Tere is a new cancer drug that is showing great results
in clinical trials. Im going to talk to my doctor about that.
Moreover, the media supports the newer is better fallacy, even when
some of the new cancer drugs have not been tested for more than a few
months. Tese drugs are often given great acclaim as possible magic
bullets in newspaper or magazine articles. Ever since antibiotics were
developed, and ever since strides in technology helped to make medical
accomplishments soar, people in the modern world have come to think
that anything new in medicine must be better. But cancer is not a simple
bacterium that can be targeted by a simple antibiotic, nor is it a type of
wound that can easily be closed up by modern technology and hardware.
413 Evaluating Conventional Methods
Terefore, the newer is better stance does not necessarily apply to can-
cer, especially when cancer research continues to stick to the paradigm
that cancer drugs must be toxic poisons in order to work and must be
patentable.
Doctors play a role in the newer is better syndrome as well whenever
they recommend that a cancer patient take part in a Phase I clinical
trial. You, yourself, may have been recommended this and are possibly
considering it. But what all cancer patients should know about Phase I
clinical trials is that they are little more than toxicity tests. Tey are clini-
cal trials used to establish safe doses of new toxic drugs. In any Phase I
trial, medical researchers have established acceptable response rates in
laboratory animals, but they do not yet know the safe dose of that par-
ticular treatment for humans. So they put a bunch of patients through
various doses of the new treatment in a Phase I trial and watch for side
eects. Sometimes the doctors recommending Phase I trials dont even
believe that the patient will be likely to benet from the trial at all. But
they hope that, in the long run, patients in the future may benet from
the trial. Basically, in Phase I clinical trials, you are little more than a
guinea pig being used for determining human dosage levels. Phase 2 clini-
cal trials are somewhat better because they have already done the Phase I
for establishing toxic dosage levels, but they are still far from determin-
ing whether the new drug is truly eective for humans. Usually, Phase 2
trials show temporary shrinkage of tumors in some patients, but dont
result in any long-term recoveries.
Of course, some new drugs may actually show promise. Tey might put
a certain percentage of people into temporary remission. But, remember,
remission simply means that all clinical evidence of the cancer is gone. It
does not mean that all the cancer cells in the body are gone. Tus, remis-
sion often does not equate to long-term cure either. Basically, if a treatment
has only been tested for a short time, then the only results available on it
are short-term. In looking for long-term recovery, it makes more sense to
go with a treatment that already has a good long-term track record.
When an oncologist says to a patient, Id like you to try this new
treatment that clinical trials are just starting on, one has to wonder if
this isnt just a little bit like a pilot saying, Well, I dont have a plane
available right now that I know can get you to where you want to go
but over here, on this other runway, is a brand-new type of plane we are
just trying out. Its never been own successfully before, but the pre-ight
tests show it to be very promising. If it were me, looking for a plane to
414 oursxair \oui caxcii
get me somewhere, Id much rather walk a couple blocks down the road
to another airport with a tried-and-true plane that has already success-
fully made the trip many times. Tis is what you do when you avoid the
newer is better syndrome and look into which treatments (conventional
or alternative) have actually worked in a long-term way for many people
before you. Again, it all boils down to a simple question: Are you inter-
ested in surviving your cancer short-term or long-term?
A Deadly Double Standard
One of the things I have heard over and over from people looking into
alternatives for cancer is, What formal, large-scale studies have been done
on this or that alternative cancer treatment? When the person then hears
that no large-scale studies have been done, they often gure the treatment
approach must not be any good and no longer consider it.
Te rst thing to understand is that the developers of most of the
alternative treatments mentioned in this book did try for many years to
get formal, large-scale studies done on their innovative cancer treatments.
If these approaches had been fairly evaluated by mainstream medicine,
as they should have been, there would be large-scale formal studies to
quote from. But only the richly funded mainstream research organiza-
tions (backed by pharmaceutical or government money) can aord to
do these types of studies. So, if a treatment approach is not considered
by pharmaceutical companies to be something that could be extremely
protable for them, large-scale formal studies will not be done. And,
unfortunately, the government agencies involved in cancer treatment
research, such as the National Cancer Institute and the FDA, simply act
as watchdogs and protectors of Big Pharmas prots.
Te second thing to understand is that, in many cases, small but sig-
nicant studies have been done on alternative cancer treatments with
great success. Some examples of these studies are:
In I946, a congressional committee looked into the Gerson therapy and
ocially concluded it was a sound and eective cancer treatment.
In I954, a team of I0 reputable doctors studied the clinical records
of patients using the Hoxsey therapy and found it to be an eective
cancer treatment. Tey strongly recommended it over other cancer
treatments of that era.
415 Evaluating Conventional Methods
Between I972 and I977, Memorial Sloan-Ketterings head research
scientist, Dr. Kanematsu Sugiura, studied Laetriles eects on cancer
in laboratory animals. He found Laetrile to be eective against cancers
of all types, and pronounced it more eective than any substance he
had ever tested for cancer.
In the early I980s, Dr. Nicholas Gonzales performed a detailed scien-
tic analysis of 500 cases of cancer patients treated with Dr. Kellys
enzyme therapy with a focus on pancreatic cancer. He found it to be
signicantly more eective than anything conventional medicine had
to oer.
Several scientic studies done in the U.S. and Japan on Dr. Burzynskis
antineoplaston therapy showed it to be signicantly better than con-
ventional methods for numerous types of cancer, and phenomenally
so for brain cancers and lymphomas.
In the early I990s, in vitro studies done by the National Cancer Insti-
tute on Jim Sheridans formula now called Protocel
showed results
that were much better than chemotherapy results for a variety of dif-
ferent cancer cell lines. Yet they declined to study it further.
Generally, the public is not aware that any of these studies have been
done, nor are they aware of their highly positive results. What most people
want to see are modern large-scale clinical trials on alternatives for cancer.
Tis is understandable considering that in most cases these peoples lives
are at stake. However, these types of expensive studies will not be done
until the current medical climate changes.
But more importantly, people expect there to be unbiased, third-party,
large-scale studies done on everything, without realizing that these types
of studies have not even been done on conventional cancer treatments.
In other words, cancer patients rarely say to their oncologist, Doctor, I
cant consider this particular type of chemotherapy or radiation treatment
unless you are able to show me positive results from unbiased, large-scale
studies showing that people who used this treatment got wellreally got
well, not just managed to live with their cancer for ve years after their
diagnosis. Tis is largely because patients assume that the studies for
conventional treatments have already been done. Tey havent.
What is so ludicrous about this double standard is that radiation and
most chemotherapy agents are still ocially listed as unproven cures
416 oursxair \oui caxcii
by the FDA and are legally required in many cases to be classied as
experimental. Te fact is that many doctors and most of the public mis-
takenly assume that anything approved by the FDA has been rigorously
proven to be eective in scientic studies. In his June 6, 2003 newsletter,
Dr. Moss shows us that this is not the case and gives an example of the
process of ocially approving a new cancer drug:
Te FDA has approved the drug Iressa (getinib) for the treatment
of non-small cell lung cancer, despite evidence that it does not prolong
the lives of patients. Approval came after an FDA panel heard testimony
from patients, one of whom claimed to feel much better after taking
the little brown pill. Her moving story helped convince members of the
Oncologic Drug Advisory Committee to give nal approval.
. . . Some critics are beginning to wake up to the fact that the FDA is
now approving drugs that emerge from Big Pharma without requiring
the rigorous proof once considered necessary. In fact, when proof is oered
that the drugs in question do not work it seems that the FDA is quite
willing to throw out the studies and revert to anecdotal accounts.
When extremely high standards of clinical results are required for under-
funded alternative treatments but are not required for richly-funded conven-
tional treatments, then we are dealing with a deadly double standard.
But it is not only Big Pharma that is biased toward their types of con-
ventional treatments. Tere is also often a strong personal bias among
conventional doctors against alternative treatments for cancer. Here is one
story to illustrate some problems people face when they discuss treatment
options with their oncologist. Tis was from a man whose wife was suf-
fering from late-stage cancer, most of which was in her brain and growing
fast. She didnt have much time. Te man claimed he had looked into
many alternative treatments for his wife, but said, Te problem with
those is that so many of them turn out to be bogus. I found out later
from him that the way he had decided they were bogus was by asking
his wifes doctor what he thought of the alternative treatment every time
he heard of one. Since the doctor looked at all alternative cancer treat-
ments as bogus, that is what he replied in every case, without having any
knowledge of the specics of the therapy.
Tis mans wife died of her brain cancer a few months later. None
of her doctors had anything eective to oer her, and yet they were all
quite eective at keeping her from trying any alternative treatments
treatments they were totally uninformed about, but adamantly claimed
were ineective.
417 Evaluating Conventional Methods
Unfortunately, most conventional doctors are completely uninformed
or worse, misinformed, about any treatment that is not conventional.
By this I mean that they usually know very little about anything not
endorsed by pharmaceutical companies (or by medical organizations that
are inuenced by pharmaceutical companies). Tus, there is a very real
problem in thinking that your doctor is going to know the truth about
alternative cancer treatments. And doctors are not motivated to nd out
more about alternative cancer treatments because, in most U.S. states, it
is illegal for them to prescribe any treatment for cancer other than what
is specically approved by the FDA.
We have been brought up to regard doctors and medical organiza-
tions as experts. We have been brought up to think that if we dont get
our doctors approval on some treatment approach we are interested in,
then we are being irresponsible, maybe even killing ourselves. We have
not been brought up to believe that big industry, and not true science, is
aecting which medical treatments are available to us.
New Cancer Drugs Are Big Business
It is dicult to accept that the most eective non-toxic approaches
to treating cancer are not being used by oncologists and cancer clinics
everywhereand that toxic treatments that do not show signicant eec-
tiveness are being used. Te only answer to this is that cancer treatments
are big business. In particular, new cancer drugs are big business. And
the eectiveness of new drugs can easily be exaggerated and promoted in
press releases by drug companies. Ralph Moss, Ph.D. shows how this can
happen in his June I3, 2003, newsletter. Dr. Moss rst states that,
On July 30, 200I, Erbitux was hailed in a Business Week cover story,
Te Birth of a Cancer Drug. Te drug, then called IMC-225, was cel-
ebrated as a blockbuster that halts the spread of cancer. In an editorial
entitled Te Dawn of a New Era, the magazine claimed that Erbitux
seems eective against cancers of the colon, pancreas, head and neck
and lungs. It suggested that victory might be within sight in the war
on cancer.
Ten, Moss goes on to explain that the Associated Press, CNN, and
Wall Street all joined in with incredible excitement about this amazing
new cancer drug. But what these news organizations never did was to look
at the studies themselves. If they had, they would have found that, on
418 oursxair \oui caxcii
average, the studies done on Erbitux showed the overall response rate to be
only about I0 percent. (And we know that response rate is not equivalent
to recoveryit just means that a 50 percent reduction in tumor size was
achieved for a short while.) Plus, the studies on Erbitux showed an aver-
age of just 45 days to progression. Tis means that the common length of
time that Erbitux could slow the cancer was only about one-and-one-half
months before the cancer would progress and grow out of control again.
Moreover, about 50 percent of the patients given Erbitux in the studies
suered what were considered severe side eects.
Yet, with so little eectiveness to boast, Erbitux went into clinical trials
to get approval by the FDA as a cancer drug. If approved, Erbitux could
be worth billions of dollars a year in sales to drug companies.
Apparently, FDA approval of cancer drugs like Erbitux does not require
studies that show signicant long-term eectiveness. For example, another
highly touted cancer drug, Iressa, has already achieved FDA approval.
But according to Dr. Moss, Te approval came despite the fact that Iressa
has been shown in rigorous studies not to prolong overall survival.
Te FDA itself appears to operate in ways that involve huge con-
icts of interest. Tis organization is supposed to protect public safety
where drugs are concerned, yet many of its personnel, including heads
of departments, either have had or will move on to highly paid jobs in
pharmaceutical companies. Te FDA personnel are not unbiased! Not only
are they not unbiased, they are practically autonomous and untouchable
because much of what they do is not under direct control of Congress.
Unbelievably, congressional hearings that uncover problems in the FDA
are only allowed to make suggestions to the FDA where they think
change is warranted. It appears that the FDA does not have to do any-
thing Congress says!
Questions to Ask Your Oncologist
What can you do to protect yourself? At the very least, cancer patients
have the right to know what the long-term ecacy of a treatment being
oered them is, as well as what side eects they might experience. In other
words, they have a right to make a truly informed decision. To make sure
that you are able to make a truly informed decision for yourself, you can
start by asking your doctor the right questions. Some questions I highly
recommend that you ask your oncologist regarding the conventional
treatment he or she is recommending to you are the following:
419 Evaluating Conventional Methods
I. What kind of long-term eectiveness does this type of treatment oer
for my type of cancer? In other words, what are my chances of living
longer than ve years and becoming cancer-free?
2. If your oncologist quotes response rates to you, you might want to
say, I am not interested in hearing about tumor response rates because
I know that they only refer to short-term tumor shrinkage. What are
the long-term, cancer-free statistics on this treatment?
3. If you have a child who has been diagnosed with cancer, you might
want to ask your pediatric oncologist, What are the chances that my
child will recover using this treatment and grow up to be a healthy
adult? Have you seen any children fully recover from this type of
cancer with this treatment and go on to live totally normal lives?
4. Is the treatment you suggest considered a curative treatment in this
case, or just a palliative treatment? (Remember, a palliative treat-
ment is considered to be one that is not expected to save the patients
life, but is simply administered in the hope that it will prolong the
patients life. Sometimes this expectation for longer survival is only a
few months.)
5. What will this treatment do to my quality of life?
6. How long do you think I will live if I do not undergo any treatment
at all? And how long do you think I will live if I follow your treatment
suggestion?
7. Can you give me any phone numbers of other patients you have suc-
cessfully treated with the type of treatment you are suggesting to me?
Or, if you cant give out phone numbers, can you at least describe to
me any cases of people who fully recovered from their cancer using
the method you want to prescribe to me?
8. If I go through this treatment, what are all the serious, or even life-
threatening, side eects I might experience? For example, is it possible
this treatment could cause me to die from heart failure or a blood clot?
Is it possible this treatment could cause me to develop a secondary
life-threatening cancer within a few years?
Do not be shy about asking these direct questions. Tis is informa-
tion you have a right to know. You may be about to make a decision that
your life depends on. Also, if your oncologist is not comfortable with
420 oursxair \oui caxcii
these types of questions, then you should consider seeking out another
oncologist who will answer them honestly. Remember, you are paying
your doctorhe or she is working for you.
Hopefully, the information in this chapter will help you to evaluate
conventional methods that may be recommended to you, and allow you
to make a truly informed decision about the treatment method you want
to go with. I suggest you be just as open and objective about considering
the treatments your conventional oncologist recommends to you as you
are when you consider any alternative treatment for your cancer. However,
do not fall prey to a double standard. Do not let yourself be rushed into
treatment before you have considered your options. Understand the ter-
minology and statistics that are presented to you by your doctor. Be aware
of short-term versus long-term eectiveness. Be aware of all possible side
eects for any treatment you are considering, whether it is a conventional
or alternative approach. And try to nd out if other cancer patients have
used that approach successfully to become cancer-free (not to just live 5
years after diagnosis). Never forget that your goal is to recover from your
cancer and regain a normal cancer-free life!
Resources:
Books
Ralph W. Moss, Ph.D. Te Cancer Industry. New York: Equinox Press,
1999.
Ralph W. Moss, Ph.D. Questioning Chemotherapy. New York: Equinox
Press, 2000.
Video
Cancer Doesnt Scare Me Anymore, by Dr. Lorraine Day. To order, call
(800) 574-2437, or visit Dr. Days website: www.drday.com.
Newsletter
For the newsletter and special reports put out by Ralph W. Moss, Ph.D.,
go to www.cancerdecisions.com.
421
23
Choosing an Approach and
Monitoring Your Progress
A
fter reading the previous chapters of this book, I hope you have
gained an understanding of some of the many options you can
choose from to outsmart your cancer. However, if you make the deci-
sion for yourself to go with an alternative, non-toxic approach, you may
also feel somewhat overwhelmed by all the possible options. Tis chap-
ter will give you some important tips to help you choose an alternative
treatment plan that is right for you. Tese tips address narrowing down
your choices, contacting practitioners for more information, dealing with
conventional doctors, prioritizing your overall treatment program, and
monitoring your progress.
Narrowing Down Your Choices
How does one narrow down the choices? Te best way to start is by
evaluating four main treatment factors and how they apply to your par-
ticular situation. Tese are: (I) Ecacy of treatment; (2) Diculty of
treatment; (3) Cost of treatment; and (4) Level of supervision.
Keeping these factors in mind to see if there are some treatment
options you may want to rule out may help you to more easily zero in on
the approaches you want to consider. I would also recommend not just
422 oursxair \oui caxcii
considering those approaches that have whole chapters devoted to them
in this book. For instance, there might be an approach in Chapter I7 that
is only briey discussed, but after looking into it some more you decide
it is the best option for you.
Ecacy of Treatment
Ecacy of treatment is, of course, going to be foremost in importance.
But it is really impossible, without comprehensive comparative studies,
to say that any particular alternative cancer approach is more eective
than another in a general sense. And, with dierent peoples physical
conditions and medical issues varying so much, it is often very dicult
to know which approach will be the most eective for any particular case.
No cancer treatment, whether conventional or alternative, is I00 percent
eective for I00 percent of the people that use it.
When trying to ascertain for yourself the overall eectiveness of any
approach, there are some important issues to understand. For example,
you may be concerned about some people youve heard about for whom
that approach did not work. One thing to remember is that most of the
people who use alternative approaches start them at a much later stage
in their disease than is optimal. Because people are not usually aware
of the benets of alternative treatments when they are rst diagnosed,
they generally use conventional treatments rst. It is only after these
conventional treatments have failed that many people turn to alternative
methodsand this tends to bring down the success rates of alternative
approaches. (Because these people are often already seriously damaged
by the chemotherapy and/or radiation they have been given, or possibly
already damaged by the cancer that may have spread more extensively
throughout their body.) Te general rule is that, the sooner after diagno-
sis that you start any treatment, whether alternative or conventional, the
better your chances for recovery will be. Another thing to remember is
that, because alternative approaches are more often self-administered than
conventional approaches, there will always be a certain number of people
who do not use them as eectively as possible. I have heard more than
once about someone who claimed that a particular approach did not work
for them, but then I found out that they either did not give the treatment
enough time, or there were things they were doing that interfered with
the treatment. So, even though someone you know may not have had
423 Choosing an Approach and Monitoring Your Progress
success with a particular approach, that does not mean it wont work for
you. And you may be able to nd others that it did work for.
One issue for some types of alternative approaches, such as the herbal
therapies, is that it may be important to nd sources that provide these
treatments in as close to their original form as possible. Herbs are natures
medicine, but they must be grown, harvested, and used in optimal ways
to be eective. Te Hoxsey herbal formula, for instance, as well as Essiac,
were both originally harvested from wild-crafted herbs grown in healthy,
virgin soils. Tey were administered shortly after preparation and did
not have to be prepared for mass marketing and long-term storage. Even
though the Hoxsey therapy and Essiac are still achieving cancer recov-
eries for many people (especially in early stages of cancer), their overall
eectiveness, particularly for late-stage cancer, may not be quite as good
as when they were originally used.
Tus, if you are planning to use any herbal approach, I suggest you
research that treatment as much as you can and try to nd the best pos-
sible source to get the herbs from. If you decide to use the Hoxsey herbal
approach, you may want to go directly to the clinic in Mexico that Mil-
dred Nelson established to obtain good quality herbs and guidance on
how to use them. For good quality Essiac, you may want to search out
an independent herbal source that has high standards for the quality of
herbs they sell rather than use a mass-produced herbal formula, or at least
use a source that you know has brought about recovery for others.
In a similar way, diet-based approaches which focus primarily on high
amounts of fresh vegetables and fruits, such as the Gerson therapy, may
not be as eective as they were decades ago. Tis is partly because it is
dicult in this modern world to nd fruits and vegetables grown in truly
balanced, healthy soils. Even organically grown fruits and vegetables are
likely to come from soil that has been overused. Articial fertilization
techniques are helpful, but may not be able to produce crops that are as
abundant in nutrients as virgin soils can. It is also partly because people
are more toxic these days than they used to be. So the approaches that
place a large focus on detoxication may have further to go in todays
world than they did earlier in the 20th century.
However, we can learn from all of the successful non-toxic approaches
and can often use parts of each in combination. For instance, pancreatic
enzymes (Kelley), Laetrile (Krebs), herbs (Hoxsey or Essiac), diet (Gerson
or Budwig), or coee enemas (Gerson and Kelley) can often be combined
424 oursxair \oui caxcii
with various other approaches to optimize ones chances for recovery.
Just make sure that the aspects you use from dierent approaches do not
conict with each other.
In general, alternative non-toxic cancer approaches tend to work well
for most types of cancer, and they are not focused on treating specic
cancers the way conventional treatments are. Tis is because they address
the common characteristics of all cancer cells. Tus, the ecacy of any
particular alternative approach will not be limited to one specic type
of cancer the way conventional chemo drugs often are. Having said that,
some alternative approaches may boast that they are particularly good
at dealing with cancer in particular systems of the body. For example,
Dr. Burzynskis antineoplaston therapy is particularly eective for primary
brain cancer and lymphatic cancers, and Dr. Kelleys enzyme approach is
particularly eective for pancreatic cancer. But both of these approaches
have also achieved great results for cancers in other locations of the body,
and there are other non-toxic approaches, such as Protocel
or axseed
oil and cottage cheese that are eective for brain cancer and lymphomas
as well.
Te most important way to ensure eectiveness of any alternative,
non-toxic approach is by acquainting yourself with it enough to make
sure you are using it optimally, and by nding a qualied practitioner
or support group to help guide you through it whenever possible. Tak-
ing care of yourself in other ways may also be important to your healing
process. Some people may have to continue going to work while they are
trying to recover from their cancer because of their nancial needs. But
if one can, it might be best to stay home and reduce stress while recover-
ing. Some key aspects of taking care of yourself may involve getting the
sleep you need, eating a nutritional and balanced diet, drinking lots of
good water for hydration and detoxication, reducing unnecessary stress,
and dealing with your emotions.
Diculty of Treatment
In some cases, diculty of treatment may be the biggest factor of all
when considering which treatment approach to go with. Tis factor par-
ticularly comes into play when treating very young children or elderly
people. In terms of sheer volume of work, the Gerson therapy presented
in Chapter 5 is considered by many to be the most dicult alterna-
tive cancer treatment available. It requires the juicing of fresh, organic
425 Choosing an Approach and Monitoring Your Progress
vegetables and fruits about I3 times every day, along with performing
multiple coee enemas every day and carrying out other specic daily
requirements. Even some strong, young adults have found it necessary,
when doing the Gerson therapy, to actually hire outside help in order to
carry out the daily juicing requirement. And the daily coee enemas may
not be possible for young children, some older people, and even some
middle-aged adults who do not have the energy or mobility to carry
out the process. (However, for those people who want to use a strictly
nutrition-based approach and have the energy or help required to do it,
the Gerson therapy may be a great choice.)
Another issue to think about is the number of pills required by the
approach you are considering. For example, the Gonzalez-Isaacs enzyme
therapy presented in Chapter 7 requires an extremely high number of
pills to be taken every day (up to about I50). Tis amount may be too
dicult for young children to swallow or for the elderly to digest. Tere
may be ways to work around this, such as opening the pills up and put-
ting the powdered contents into a drink, but it is certainly a factor to
consider when prioritizing ones treatment options.
Overall, some of the easiest approaches to administer to young chil-
dren or elderly adults are the following: Protocel
, Poly-MVA, LifeOne,
Burzynskis antineoplastons, axseed oil and cottage cheese, the Hoxsey
therapy, Essiac Tea, low dose naltrexone, Lapacho/Pau DArco/Taheebo,
and Ellagic Acid. (Remember, however, that Protocel
should not be
done along with most other approaches unless compatibility is specically
listed, though most of the other approaches can be combined together
without Protocel
.)
Tus, ruling out those approaches that may be too dicult to admin-
ister for your particular case can help narrow down your choices.
Cost of Treatment
Considering the cost of approaches is another way to narrow down your
choices. Te ideal situation would be for each person to have unlimited
money and unlimited time, but this is not usually the case. Fortunately,
most alternative treatments are much less expensive than conventional
treatments for cancer. Te down side is that health insurance policies
rarely cover alternative methods, even if the doctor you are working with
is a fully accredited M.D. Terefore, when it comes to using some of the
more expensive alternative methods, it might be important to nd out
426 oursxair \oui caxcii
ahead of time if your insurance company will pay for any part of it or
not or whether or not there is a way you can aord it.
Te costs for dierent alternative treatment approaches vary consider-
ably, so it is a good idea to consider the dierent prices listed at the back
of each treatment chapter. Tese are only estimates, but they will give you
a general idea of the expenses required. Besides the cost of treatment, one
must also consider possible time away from work. If you start an eec-
tive treatment soon after diagnosis, you may have a very good chance
of being able to carry on with your life normally while you recover. But
many cancer patients may not feel well enough to work at all for at least
some period of time. Or if you choose a very time-consuming method,
then just carrying out the treatment may rule out time to go to work and
bring home a paycheck. Tis means that when you consider treatment
expenses, you may also need to factor in a reduction of income occurring
at the same time.
Te important thing to remember is that, when considering your
treatment options, more expensive does not necessarily mean more eec-
tive. One of the more expensive approaches may turn out to be the best
choice for one person, while one of the least expensive approaches may
turn out to be the best choice for another. Te good news is that, if you
are particularly challenged nancially, there are still excellent low-cost
options available in the alternative cancer treatment world.
I believe that a good rule for anyone looking into alternative cancer
treatments is to rst try to decide which form of treatment you would
choose if money were not an issue. In other words, put aside all of the
money considerations you have, just at rst, and try to evaluate what
approach you think will give you the best chance for recovery. Once you
have sorted out which treatment you would like to try, then see if you can
come up with the money. Burzynskis antineoplaston therapy is the most
expensive alternative approach and may be too expensive for most people.
But it should always at least be considered whenever a person is dealing
with brain cancer or lymphoma because of its high level of eectiveness
for those types of cancer.
Tink carefully before choosing a treatment approach that is not your
rst choice just because you cant aord your rst choice approach. In
some cases, it may be that there is no way around this. But whenever pos-
sible, it is a good idea to try to pursue the treatment approach you feel
you can most fully commit to and have condence in.
427 Choosing an Approach and Monitoring Your Progress
Level of Supervision
Another factor to consider is the type and amount of guidance or
supervision you require to feel comfortable with your treatment approach.
If you are the type of person who can feel comfortable primarily self-
administering your own treatment after obtaining initial guidance, then
there are certain approaches that can be considered. If you are the type
of person who would be most comfortable with ongoing supervision and
guidance from a medical practitioner, then there are others to consider.
(E.g., Dr. Burzynskis Clinic in Houston, Dr. Gonzaless enzyme therapy
in New York, Cesium therapy at the Reno Integrative Medical Center,
the CAAT Protocol, Dr. Forsythes clinic for Poly-MVA in Reno, or the
Mexican or German cancer clinics.)
Preferably, geographical location will not be a deciding factor for most
people, because airline ights are not that dicult to take. For instance,
Americans who prefer treatment that is supervised by a doctor should not
rule out clinics in Mexico. For about the equivalent of travelling to San
Diego, California or San Antonio, Texas, these clinics can provide some
of the very best doctor-supervised treatment and oer cancer patients the
benets of multiple alternative therapies combined.
Contacting Practitioners for More Information
If you decide to try an alternative cancer approach, you may want to
quickly call each place of treatment you are considering. Tis could be
to verify that they are still in operation as well as to ask some detailed
questions about their treatment program. Feel free to ask what kind of
success they have had dealing with your particular type of cancer, but
dont expect formal statistics or studies. Te best type of answer you will
probably receive is a comment based on their own experience with their
patients. Tis information is valuable, especially since they sometimes
may be able to give you the phone number or email address of one or
more of those patients. If they have not yet treated your particular type
of cancer, this does not necessarily mean you should stop considering
them for treatment. After all, there are many dierent manifestations of
cancer, and yours may be one of the more rare types.
If your preliminary research looks promising, you may want to either
start treatment immediately or consider making a consultation appoint-
ment rst to discuss your particular case. Tis will use up some of your
428 oursxair \oui caxcii
valuable time and money, but it can be an important step in choosing
the treatment that will be best for you. Even if you have to go to several
dierent treatment center consultations before you decide, it could be
worth your eorts in the long run. Yes, it is important for you to start
treatment as soon as possiblebut it is also important to be able to make
a well-informed decision as to which treatment you choose.
Most alternative doctors will want you to come in for a consultation
with all of your diagnostic test results. Tese include biopsy reports, X-rays,
CT scan results, blood tests, and whatever else you have been able to get
from your conventional physicians so far. Ask rst over the phone what
types of records they want you to bring, and ask how much the consul-
tation will cost. Often, an in-person consultation with an alternative
practitioner or clinic can be of great help in determining which approach
you want to follow. It not only will give you an idea as to whether you
can feel comfortable with that practitioner or clinic, it also may give you
a better idea as to the likelihood of that approach working well for you,
and even possibly how long it may take. Another option is to ask for an
informational packet to be mailed to you.
Time is always of the essence when dealing with cancer. But spending a
little more time in the beginning can sometimes save time later on. It may
be hard to take a few extra days for research or a consultation appointment
in the beginning when your doctor and family members are urging you
to rush into surgery, radiation or chemotherapy. But just remember that
a well-spent number of days doing research in the very beginning can
sometimes make the dierence between life and death. Getting onto a
cancer treatment plan as fast as possible is always the priority, but getting
started on treatment that will give you your best chance for long-term
recovery is also of utmost importance.
Dealing With Conventional Doctors
Every person who chooses to use an alternative approach to outsmart
his or her cancer will be going against the grain of modern conventional
medicine. One problem that can arise as a result of this is the diculty
involved with declining the treatment your conventional doctor thinks you
should get. Most people with cancer are rst diagnosed by a conventional
doctor. If you are one of these people, you may have seen an oncologist
who is very committed to the mainstream accepted approaches. It is not
easy to turn down a medical specialists recommendationespecially when
429 Choosing an Approach and Monitoring Your Progress
you may be told that, in doing so, you will be killing yourself. One thing
to remember in this situation is that, specialist or not, your doctor works for
you. You are paying your doctor for his or her expertise and professional
service. It is important to listen to and consider any recommendation for
treatment your conventional doctor gives you. Doctors go through an
immense amount of training and then experience a great deal clinically,
so their input should be respected and sought. But when it comes to the
nal treatment decisions you make, that is up to you.
If you choose to use an alternative approach, you will most likely be
in a situation where you still want to see your conventional doctor at
certain intervals for diagnostic tests and monitoring of your progress.
Tis is desirable whenever possible. Even people using alternative meth-
ods will want to have blood tests, CT scans, MRIs, or other tests done
regularly to ascertain how well they are doing and make sure their cancer
is responding to the approach they have chosen. Also, getting diagnostic
tests performed by a conventional doctor will generally allow them to
be covered by your health insurance policy. Another reason to seek help
from a conventional doctor is in case there are any side complications
arising from your cancer.
I recommend being as open as possible with your conventional doctor.
I believe it is best to be honest and to give your doctor the opportunity of
deciding to follow your progress while you use an alternative approach.
You may be surprised to nd that your doctor is more open-minded than
you expected. If, however, your doctor takes a stance against alternative
approaches and will not prescribe diagnostic tests to you unless you undergo
conventional treatments, then you have the option of nding another doc-
tor or oncologist who will. If you phone dierent doctors oces, you may
be able to nd another doctor in your area who is willing to monitor your
progress even though you are not using a conventional method. Tough
many people see their oncologist over and over and never tell him or her
they are using an alternative approach, I recommend that you make an
eort to nd a doctor with whom you can work openly. In doing so, you
are not only standing up for yourself and your right to openly choose
your own treatment, you are also giving your doctor a chance to learn
how eective alternative methods can be.
But if you do employ a conventional doctor to prescribe diagnostic tests
for you, remember that, in some cases, your doctor may not know how to
interpret the results of the tests. A good example is, when using Protocel
,
cancer marker levels may rise as the cancer cells lyse and tumors break
430 oursxair \oui caxcii
down. Conventional doctors may not interpret these results correctly, since
they are trained to see any rise in cancer markers as indications that the
cancer is growing or spreading. It is up to you to be informed about the
particular approach you are using so that you can help your conventional
doctor understand the process you are going through.
Prioritizing Your Overall Treatment Program
Once you have decided on the primary approach you wish to use, g-
ure out your priorities. You may want to make a list to help you keep your
overall recovery plan in mind. I would suggest that you list the primary
treatment approach you have chosen as priority number I. Secondary to
that, you can list any adjunctive treatments you would like to add to your
program (as long as they are compatible with your primary treatment.)
Ten, lower on the priority list might be things like improving your diet,
dealing with toxic teeth, working on emotional or psycho-spiritual issues,
and anything else. Dierent people will list their priorities in a dierent
order from other people.
Seeing the important issues prioritized and listed on paper can help to
reduce some of the confusion that may arise when you think about what
it is you need to do to outsmart your cancer. As mentioned earlier, we
can learn from all of the successful alternative approaches, and many of
these can be combined eectively. Just be careful to not combine aspects
of dierent treatments that might conict. Most alternative cancer treat-
ment approaches have very specic guidelines, and these guidelines are
there for good reasons. Tus, an important rule to remember is to always
thoroughly research any approach you are using and make sure you fol-
low it or combine it with others correctly.
Monitoring Your Progress
Monitoring your progress is critical. One of the saddest things I have
come across (and more than once) is when a person uses an alternative
approach for a long time, maybe eight or ten months, and they just assume
that it is working for them. Ten they go in for a scan and nd out their
tumors have grown or their cancer has spread to new places, such as their
liver. Tese people are devastated when they nd out they are in a worse
situation than when they started.
No matter how miraculous an approach may appear, and no matter
431 Choosing an Approach and Monitoring Your Progress
how well it worked for your friend or your relative, you should never just
assume that it will work as well for you at the same dosing schedule that
was used for them. Every persons body is dierent and the success of the
treatment may be aected by how toxic a person is (with heavy metals
or other substances), how imbalanced hormonally a person is, whether
one has toxic teeth issues, how much damage ones body has already
undergone, etc.
Even though all of the alternative methods presented in this book have
better track records than conventional cancer treatments in general, that
does not mean they will cure I00 percent of the people who use them.
Having success with an alternative cancer treatment might be easy for
some people and the approach will denitely seem like a magic bullet
for them. But for others, it may be more dicult. Also, when using a
single product approach, such as Protocel
in a formal, scientic laboratory environment. Later, Sheridan worked
452 oursxair \oui caxcii
on his formula in the Biosciences Division of the Battelle Institute in
Columbus, Ohio. Tere, he tested his formula using the same rigorous
standards that were being used to test new chemotherapeutic agents
for the National Cancer Institute. Finally, in I990, the NCI tested
Sheridans formula in vitro on many dierent cancer cell lines and all
the results were excellent.
Te mechanism of anaerobic functioning in cancer cells was scienti-
cally proven by the famous biochemist, Otto Warburg, who received
a Nobel Prize for his contributions to science.
Dr. Johanna Budwig was a brilliant biochemist who was nominated
for a Nobel Prize seven dierent times. Her impeccable laboratory
research on essential fatty acids was a monumental contribution to
science and her own clinical work reportedly demonstrated over I,000
documented cases of cancer recoveries using her dietary approach.
Aubrey Keith Brewer, Ph.D., was the pioneering physicist for cesium
high pH therapy. He was highly qualied for his research that focused
on the study of cell membranes and, for a time, was chief of the
National Bureau of Standards Mass Spectrometer and Isotope section.
Clinical trials later proved his approach using cesium to be eective
at bringing about late-stage cancer recoveries in humans.
Royal Rife and Gaston Naessens were considered by many to be
two of the greatest geniuses of the 20
th
century. Teir contributions
to microbiology and the understanding of micro-organisms were
immeasurable. Brilliant inventors, they each independently developed
new types of microscopes to aid them in their work. Rifes Universal
Microscope and Naessenss Somatoscope were far more powerful
than any microscope being used at the time and both allowed obser-
vation of virus-size organisms in their alive state, something that still
cannot be done today with current technology.
Tus, the belief that alternative cancer treatments are non-scientic
is simply as wrong as it could be!
Medical Freedom
Some physicians are open to alternative approaches and to their patients
using them. More and more oncologists and other doctors are overseeing
453 Concluding Comments
patients using a non-toxic approach for their cancer. Many of these phy-
sicians are seeing the alternative approach work and are saying to their
patients, Keep doing what youre doing! But a very real obstacle to any
physician prescribing an alternative approach for cancer is that most states
in the United States do not legally allow physicians to do this. Many doc-
tors are in the unenviable position of having to say, Keep doing what
you are doing because it is working, but dont tell me the details of what
you are doing because I cant prescribe it anyway.
As a result of state laws restricting doctors to only prescribing cer-
tain types of treatments, medical freedom is not yet secure for us in the
United States. Moreover, medical freedom is not yet protected as a right
in the Constitution. However, at least one signer of our Declaration of
Independence had the foresight back in I776 to proclaim that medical
freedom should be a protected right, and should be in our Constitution.
Benjamin Rush, M.D., was the Pennsylvania delegate to the Continen-
tal Congress as well as a prominent medical doctor of his day. Dr. Rush
wisely stated:
Unless we put medical freedom into the Constitution, the time will
come when medicine will organize into an undercover dictatorship to
restrict the art of healing to one class of men and deny equal privileges to
others; the Constitution of this republic should make a special privilege
for medical freedom as well as religious.
Hopefully, the day will come when all eective medical approaches
are available to us. But until that time, how you choose to treat your
cancer is still your decision, not someone elses. Dont let others push you
into doing something you dont want to do, whether they happen to be
doctors, friends, or family. And dont let your own fear push you either.
Instead, take a deep breath and do your research as quickly as you can.
Get someone you trust to help you, if possible. Listen to your heart. Once
you have started treatment (whether conventional or alternative), keep
doing research at a slower pace. Tere may be even more you can do for
yourself as you start to recover.
Cancer is never easy, but many others have outsmarted their cancer
with alternative non-toxic treatments that work, and you can pursue the
same methods, too!
455
Recommended Resources
Multiple Alternative Cancer Treatments
Options: Te Alternative Cancer Terapy Book, by Richard Walters (Avery/
Penguin Putnam, New York, 1993).
An Alternative Medicine Denitive Guide to Cancer, by W. John Diamond,
M.D. and W. Lee Cowden, M.D., with Burton Goldberg (Future Medi-
cine Publishing, Inc., Tiburon, California, 1997).
Cancer Terapy: Te Independent Consumers Guide to Non-Toxic Treat-
ment and Prevention, by Ralph W. Moss, Ph.D. (Equinox Press, New
York, 1996).
Cancer-Free: Your Guide to Gentle, Non-toxic Healing, 3rd Edition, by Bill
Henderson (Booklocker.com, Inc., 2008).
Cancer: Step Outside the Box, 2nd Edition, by Ty M. Bollinger (Innity
510 Squared Partners, 2006).
Painless Cancer Cures and Preventions Your Doctor May Not Be Aware Of,
by Deanna K. Loftis, R.N., B.B.A. (JADA Press, 2005).
I Beat Cancer: 50 People Tell You How Tey Did It, by Zack Vaughan
(Awareness Publishing, Oxnard, California 2003).
456 oursxair \oui caxcii
Alternatives in Cancer Terapy, by Ross Pelton, R.Ph., Ph.D., with Lee
Overholser, Ph.D. (Simon and Schuster, New York, 1994).
Natural Strategies for Cancer Patients, by Russell Blaylock, M.D. (Kens-
ington, 2003).
Specic Alternative Cancer Treatments
Antineoplastons
Te Burzynski Breakthrough, by Tomas D. Elias (Lexikos, Nevada City,
California, 2001).
Cesium High pH Terapy
Cancer Cover-Up, by Kathleen Deoul (Cassandra Books, Baltimore, 2001).
www.cassandrabooks.com.
Essiac Tea
Te Essiac Report, by Richard Tomas (Te Alternative Treatment Infor-
mation Network, Los Angeles, 1993).
Essiac Essentials, by Sheila Snow and Mali Klein (Kensington Books, New
York, 1999).
Flaxseed Oil and Cottage Cheese
How to Fight Cancer and Win, by William L. Fischer (Agora Health Books,
Baltimore, Maryland, 2000).
Fats Tat Heal, Fats Tat Kill: Te Complete Guide to Fats, Oils, Cholesterol
and Human Health, by Udo Erasmus (Alive Books, British Columbia,
Canada, 1993).
Flax Oil as a True Aid Against Arthritis, Heart Infarction, Cancer, and
Other Diseases, by Dr. Johanna Budwig (Apple Publishing, Vancouver,
Canada, 1994).
457 Recommended Resources
Gerson Terapy
A Cancer Terapy: Results of Fifty Cases, by Max Gerson, M.D. (Te Ger-
son Institute, Bonita, CA, 1999).
Censured For Curing Cancer: Te American Experience of Dr. Max Gerson,
by S. J. Haught (Te Gerson Institute [under the P.U.L.S.E. imprint],
Bonita, California, 1991).
Te Gerson Terapy, by Charlotte Gerson and Morton Walker, D.P.M.
(Kensington Publishing, New York, 2001).
Hoxsey Terapy
When Healing Becomes a Crime: Te Amazing Story of the Hoxsey Cancer
Clinics and the Return of Alternative Terapies, by Kenny Ausubel (Heal-
ing Arts Press, Rochester, Vermont, 2000).
Isselss Approach
CancerA Second Opinion, by Josef Issels, M.D. (Avery Publishing Group,
New York, 1999).
Kelleys Enzyme Approach
Cancer: Curing Te Incurable Without Surgery, Chemotherapy, or Radia-
tion, by Dr. William Donald Kelley, D.D.S., M.S., with Fred Rohe (New
Century Promotions, Bonita, California, 2000).
Laetrile
World Without Cancer: Te Story of Vitamin B, revised edition, by G.
Edward Grin (American Media, Westlake Village, California, 1997).
Alive and Well: One Doctors Experience with Nutrition in the Treatment of
Cancer Patients, by Philip E. Binzel, Jr., M.D. (American Media, Westlake
Village, California, 1994).
458 oursxair \oui caxcii
Poly-MVA
First Pulse: A Personal Journey in Cancer Research, 2nd Ed., by Dr. Merrill
Garnett (First Pulse Projects, Inc., 1998).
Robert D. Milne, M.D., & Melissa L. Block, M.Ed. Poly-MVA: A New
Supplement in the Fight Against Cancer, by Robert D. Milne, M.D. (Basic
Health Publications, Inc., 2004).
Fire in the Genes: Poly-MVAthe Cancer Answer? By Michael L. Culbert,
ScD. (Foundation for the Advancement of Medicine, 2000).
Protocel
, I83I94, 202
M
MALT (see mycosa-associated lym-
phoid tissue)
Mayo Clinic, 80, I09, 27I272
McQueen, Steve, 8I82
MDR (see multi-drug-resistant cancer
cells)
medulloblastoma, 35
Meinig, George E., 392, 394,
3967
melanoma, 5I, I58, I73, I9I, 200,
295296, 3I0
melanoma, case stories of, 9697,
I35I36
melphalan, 4094I0
Memorial Sloan-Kettering Cancer
Center, 78, 57, 808I, I55,
239, 25I252, 408, 4I5, 45I
Metabolic Terapy, 8598, 45I
current treatment, 9495
history of, 8594
Mexican Cancer Clinics, 279, 303
307, 427
microzymia, 232
milk thistle, I78
millet, 7I, 74, 79, 320
Mistletoe (see also Iscador), 275,
293, 308
Mitchell, Terri, 95
Mohr, P. E., 337338
mononucleosis, I73, I75
Moorehead, Agnes, 3I
morphine, 260, 298
mortal oscillatory rate (M.O.R.),
23I, 234235, 238
Moss, Ralph W., 79, II, 3I, 8I, 83,
88, 35I352, 40040I, 404,
406, 409, 4I64I8
multi-drug-resistant cancer cells
(MDR cells), 6
multiple myeloma, I73, 283, 295
296, 475, 479
multiple myeloma, case story of,
265267
multiple sclerosis, 94, I20, I73I74,
I8I, 297, 385
mycosa-associated lymphoid tissue
(MALT), I43
503 Index
N
Naessens, Gaston, 238, 243253,
324, 452
Nagasaki, Japan, 32, 476, 479
Narayanan, Ven, I56I57
National Cancer Institute (NCI),
79, 30, 32, 36, 68, 80, I04,
I52I53, I56I57, I63, I65,
I67, 252, 324, 350, 354,
408409, 4I44I5, 452,
473474, 479, 48I
Native Americans, 44, 46, 45I
natural progesterone, I78, 332349,
357, 360362
Navarro, Manuel, 7576, 78, 86
NCI (see National Cancer Institute)
Nelson, Mildred, 4748, 505I,
423
New England Journal of Medicine, 9,
4I0
Nieper, Hans, 7576, 78, 8I, 257,
260, 273
Nixon, Daniel, 3I03II
non-Hodgkins lymphoma, I8I9,
29, I08, II2, I43, I73, 267,
269, 295296
non-small cell lung cancer, I30, I58,
4I6
N-Tense, 279, 302303
nuclear radiation, 22, 29, 3I32, 38,
46I, 47448I
NutraSweet (see also Aspartame),
24, 3I9
nutritional deciency theory, 7I
O
occult tumor, 37I, 373
Ojibwa Indian, 55, 60
Ojibwa Tea of Life (see also Essiac),
60
omega-3 fatty acids, 23, 207, 209,
2II2I2, 2I9, 225227, 320
omega-6 fatty acids, 23, 207, 209,
2II2I2, 226227, 320
organochlorine compounds, 29, 349,
462464
ovarian cancer, I58, I73, I88, I97,
205, 288, 296, 332, 336,
357, 40I, 409
ovarian cancer, case story of,
27I273
oxygenation therapies, 308
ozone, I76I77, 304305
P
p53 gene, II0, 3I0, 335336, 340,
378, 380
pancreatic cancer, 9I, 9394, 97,
I73, 250, 295296, 3I03II,
4I5, 424, 45I, 479
pancreatic cancer, case stories of,
I32, 220222
Parkinsons Disease, I73, 297, 385
Pasteur, Louis, 232, 239
Pau DArco, I78, 279, 299302,
38I, 425
peptides, I02I03, I05
pesticides, I9, 2I22, 2629, 38,
345, 348, 469
and breast cancer, 349350
pets, I7I, I73, I75, I99203, 2I9,
284, 302
Philip Morris, 67
phytoestrogens, 346347
Pier, Florianne, 249
PKD (see primary kidney disease)
placebo eect, 435
negative placebo eect, 443444
pleomorphism, 23I232, 239, 246
Poly-MVA, I76, 279285, 305,
425, 427, 43I
504 oursxair \oui caxcii
Powell, Dick, 3I
prednisone,I43I45
Premarin, 34, 332, 34I343
Price, Weston A., 392395
prickly ash bark, 46
primary kidney disease (PKD), I02
procarbazine, I47
Proctor and Gamble, 30, 467
progesterone, I78, 33I345,
358359
cream versus oral, 360362
natural, and breast cancer,
336338
prostaglandins, 209, 2I22I4
prostate cancer, I8I9, III, I73, I8I,
I88, I94, 205, 26I, 284,
288, 295297, 30I, 309,
3II, 332, 357, 36338I,
405, 4II
prostate cancer, case stories of,
I07I08, I37I38, 2I9220,
223224, 27027I
prostatectomy, 367
Protocel
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Dylan's Story Brain Cancer (Pediatric Diffuse Pontine Glioma) CD-13
Sydney's Story Leukemia (Childhood Acute Lymphoblastic) CD-15
Mary's Story Bladder Cancer with Mets to Urethra CD-17
John's Story Melanoma with Mets to Lymph and Possibly Lung CD-17
Pam's Story Breast Cancer CD-18
Arch's Story Lung Cancer with Mets to Neck and Possibly Throat CD-21
Tricia's Story Breast Cancer with Mets to Hips, Legs, Ribs, Shoulder, CD-22
Spine and Skull
Herb's Story Prostate Cancer with Mets to Pelvis, Femur, Ribs, & Spine CD-24
CD-1
EVERYDAY MIRACLES
How 12 Ordinary People Outsmarted Their Cancer
Companion Audio CD to the book
Outsmart Your Cancer: Alternative Non-Toxic Treatments That Work, 2nd Ed.
by Tanya Harter Pierce, M.A., MFCC
[ MUSIC ]
Stream Of Brief Excerpts From Upcoming Testimonials:
Doctors tend to look at cancer through cancer-colored glasses. They don't think
sometimes that there are other treatments out there that are effective. The last scans that
I had actually showed that basically they couldn't see where there was any cancer there
anymore! . . . . My son Dylan, who was 18 months old at the time, was diagnosed with
a very rare, very aggressive and inoperable brain tumor. And when the oncologists came
in to give us the diagnosis, they told us that there was basically no chance of survival.
This past June, Dylan's test results came back perfect. There were no signs of cancer.
He's been without symptoms for over a year and he's completely symptom-free! . . . .
It's been 6 years now, she's in the second grade, she's 8 years old and there's no more
cancer. I would say to anyone looking, searching for something other than
chemotherapy I would say, "Take courage and then take charge!" . . . . My doctor
gave me a copy of Tanya Pierce's book "Outsmart Your Cancer" and suggested I study
the info about Protocel
is that it is so
safe, it can even be administered to infants! These next two testimonials are very
inspiring, given that so many young children today are developing cancer.
[ MUSIC ]
JOE for Dylan's Story: Hi. My name is Joe. I live in the state of Pennsylvania, and
Id like to give my testimony to the great efficacy of the supplement called Protocel
.
On January 22
nd
of 2004 my son Dylan, who was 18 months old at the time, was
diagnosed with a very rare, very aggressive and inoperable brain tumor referred to as a
CD-14
Diffuse Pontine Glioma. Dylan was diagnosed at one of the leading childrens hospitals
in the country, and when the oncologists came in to give us the diagnosis, they told us
that there was basically no chance of survival.
Their prognosis was two months without treatment, and nine to fifteen months with
six weeks of radiation in combination with some form of chemotherapy.
Needless to say, my wife and I were completely heartbroken and devastated. At the time,
our major concern was giving Dylan quality of life. We didnt want Dylan to be in any
pain or discomfort, and so we opted against doing any chemotherapy.
A couple weeks after diagnosis we came across Protocel
.
We supplemented heavily with various enzymes.
We stuck to mostly an organic diet. We cut out all wheat, gluten and dairy from Dylans
diet, and weve done a lot of work with subtle energy therapies like Reiki and Johrei, and
of course prayer has played an enormous part as well.
In late 2004 we came across an alternative cancer test, because we decided that we did
not want to do any more MRIs with Dylan. Being so young, each time we had to put
him under anesthesia, and we just didnt want that. And so we turned to this alternative
cancer test, and thus far weve done four tests. Dylans first test was done when he was
eleven months out from diagnosis, and his numbers, although not great, were much better
than expected for someone with his diagnosis. And each subsequent test continued to
show improvement.
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This past June we did our fourth test, and Dylans test results came back
PERFECT. There were no signs of cancer!
Hes been without symptoms for over a year. We are almost 20 months out from
diagnosis, which is almost unheard of for this type of tumor, and how aggressive it was
when he was diagnosed. And hes completely symptom free.
Dylan has been taking Protocel
.
We heard good news about it. Other people had experienced success with Protocel
. We
bought it. We put her on it. She was on it for about a month. We met with the doctor.
We told him, you know, what we were doing. He had never heard of Protocel
so he
couldnt really say anything bad about it, and we asked him, You know, if we do the
bone marrow transplant, what can we expect? We were told a 5% survival rate. That
was not good enough. We said, No thank you. Well stick with the Protocel
.
Every week we took Sydney to the doctor to have her blood work, and we'd also have the
spinal fluid checked, and theyd also do bone marrow aspirations.
There was never any cancer ever again. Its been six years now. Shes in the second
grade. Shes eight years old, and theres no more cancer!
I would say to anyone looking, searching for something other than chemotherapy, I
would say, Take courage, and then take charge. Thank you.
TANYA: With cancer now the leading cause of death by disease in children, it is
critical for parents to know about alternative non-toxic approaches that are safe and won't
damage their child's body during their formative years. Another thing parents MUST
consider, if they have a child battling cancer, is that the chemotherapy given their child
MAY be carcinogenic!
This means that, if their child is lucky enough to survive their current cancer, the
chemo drugs used may cause a secondary life-threatening cancer to develop in their
child's body years later!
Alternative non-toxic methods AVOID this type of tragedy.
So, what IS Protocel
is an inexpensive, easy-to-take
liquid formula that was developed by an American chemist named Jim Sheridan. Jim
Sheridan spent about 50 years developing and perfecting this product and Outsmart Your
Cancer is the definitive source of published information on this approach. You can read
all about its history and how it works in the book, but for just a brief explanation here,
Protocel
is based on the concept that ALL cancer cells are primarily anaerobic in their
cell respiration, which is how they produce energy for themselves on the cellular level.
This common characteristic of all cancer cells was proven first by Nobel Prize-winning
scientist, Otto Warburg, then confirmed over and over again by other scientists.
Protocel
very ingeniously targets this weakness in a way that eventually starves the
cancer cells to death.
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This does not happen overnight, but over time, if used correctly, Protocel
can make
every cancer cell in a person's body become so weak that it will literally fall apart. Thus,
Protocel
testimonials:
MARY: My name is Mary. I am an 80 year old who works five days a week in the
home health care field. Eight years ago my physician told me I had bladder cancer.
Over seven years and several surgical procedures later, my physician found that the
cancer had spread to the urethra. He said I needed to have my bladder removed and wear
a bag.
My husband began a diligent search to solve the problem a different way. May 1
st
of
2004, I began taking the dietary supplements, Fucoidan, and Protocel
.
I have another lady that has cancer throughout her body that has been taking it as well.
Shes very happy. Her doctors are surprised at what theyre seeing, and they love it.
Everybodys happy with this. I would recommend it to anybody, and Im happy that I
did not go with the Interferon.
PAM: Hi. This is Pam in Michigan. In January of 2004 I was diagnosed with
invasive ductile positive estrogen-driven breast cancer. It came as an extreme shock
to me because I had always spent a lifetime in the field of nutrition and wellness, and
doing things to keep my body healthy, so this just came as a total shock.
Early on, though, immediately I made up my mind that there was no way I was going to
have anything to do with anything conventional medicine had to offer. I wanted nothing
to do with chemotherapy, radiation, lumpectomy I dont think chemotherapy kills
anything except, eventually, the patient. Ive just seen too many people go that route, and
they just didnt make it. And they weakened their system, their immune system.
I just decided I was going to keep myself strong. I was going to feed my body the
things that it needed to fight this. And I had already heard about an effective
treatment.
The stories that Id heard, it was extremely effective against not only breast cancer, but
cancers of all kinds, and it was a product called Protocel
to be extremely effective.
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I trusted the Lord through this whole thing. I walk very close to the Lord, and I really
look to Him for answers. And I was very diligent about making sure that I stayed on what
I was supposed to do with Protocel
. Im extremely grateful for the support that Ive received from some of
the people that had been on Protocel
formula.
ARCH: Hello. I'm Arch, and I'm 83 years old. A couple of years ago, I didn't
think I'd live this long but here I am, bright-eyed and bushy-tailed. Well,
bright-eyed anyway!
In early June 3 years ago, my doctor found a spot in one lung during a routine chest x-
ray. We had all kinds of trouble getting appointments for follow-up, so it was late July
before I got a biopsy on the lung spot. It was a non-small cell carcinoma.
CT and PET scans showed something suspicious in my neck and at the base of my
tongue. The thing on the neck was biopsied in August and was a carcinoma of the same
type as in the lung. I spent most of one day with a panel of specialists at a medical center
who went over the whole thing. They didn't want to commit, but the general consensus
was that I had 5 to 15 percent chance of a cure and a life expectancy of 3 to 4 years.
Surgery on the lung was not advised.
I questioned my doctor about whether we could cure cancer in the lung by any
means other than surgery and he said reluctantly, "No, you really can't". All in all,
it wasn't too encouraging.
Various doctors kept looking for whatever was at the base of my tongue, but it wasn't
until late September that they found a tonsil that just didn't look right. In October, I had
surgery on the neck and the tonsil. That wasn't a lot of fun. Starting in November, I got
radiation to the lung and to the neck and shoulder 5 days a week. I made them stop the
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neck and shoulder part early because they were burning me to a "crispy critter" and I
couldn't take it anymore. Now, to the Protocel
part.
My doctor gave me a copy of Tanya Pierce's book Outsmart Your Cancer and suggested
I study the info about Protocel
before surgery.
The surgeon had told me that it was about 6 cm long, but the pathologist found only a
1 cm carcinoma in the yellowish jelly-like material removed during surgery.
I've had CAT scans first every 3 months, now every 6 months. All have shown no
cancer, only some scarring in the lung.
So I said, "Is it gone?" He said, "As far as I can tell, it's gone. There's nothing
there but a little scar tissue."
So I feel that Protocel
took that away! At my lowest point in all this, among many low
points, I had lost about 30 pounds, had lost my sense of taste, and was very, very tired.
I'm a lot better now, and I'm struggling not to get too fat, but still taking Protocel
. It's so
easy to do and so inexpensive, I think anybody with cancer ought to take it!
TRICIA: Hi, I'm Tricia. I live in a small country town in Queensland, Australia.
Back in July of 2006, I was knocking on heaven's door when I was diagnosed and
hospitalized with metastasized estrogen-receptive breast cancer and given no chance
of survival by mainstream doctors.
I had a huge mass in one breast. The other breast also had abnormal cells.
Metastases went to my bones. It was in my skull, shoulders, ribs, pelvis, hips, legs
and my spine. And my bones weren't just spotted with cancer, they were BLACK
with it.
My spine had deteriorated badly. I had a broken back, I couldn't walk, I couldn't keep
anything down, not even a sip of water. It was extremely tiring to speak, my
concentration span was very short, and my pain was excruciating. The doctors were
amazed that I hadn't severed my spinal cord.
No cancer was ever removed from me. I had titanium rods screwed into both my hips
and upper legs down to my knees so that those bones wouldn't break. On my second day
in hospital, the medical oncologist came into my room to discuss a palliative treatment
plan with me. I insisted on doing an alternate treatment which I had started taking that
day. My treatment choice was Protocel
.
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I am grateful to this day that my oncologist wrote it up on my hospital chart so his
nursing staff was able to give it to me as I wasn't able to at that time. Protocel
was the
first treatment I used for my cancer and it was the main treatment.
I was in hospital for 2 months and then sent home in a wheelchair to palliative care.
From the beginning of my ordeal, I went from lying flat on my back in bed for months,
unable to roll, to a wheelchair, to walking frames, to a cane, until I was finally able to
give that cane a flick.
It was recommended that I do some radiation treatment, so I allowed 5 doses of
radiation to my spine to try and stop it from crumbling any further. Because of the
cancer damage to my bones, I am now much shorter than I once was.
I also chose to do 4 doses of chemo. That was in 2006. I hoped this way my body would
cope a little better. I thought by doing the chemo, it would buy me some time for
Protocel to get on top of things.
Although the chemo produced a small reduction in tumor size, there was still a large mass
there. I took Tamoxifen for about 5 months and then stopped. I felt really uncomfortable
taking it as I was concerned it would compromise Protocel
Formula 23.
Within 2 weeks, I noticed less pain and I discontinued the pain patches. I also felt
less lethargic.
I was diligent about taking Protocel
in the
beginning, I never would have gone through the impotence and incontinence and all that
goes along with that, because it was a struggle for years.
It's my contention that, if I'd have done Protocel
, I
took another PET scan. My daughter in Colorado is a chiropractor and I had the scan
report scheduled to be FAXED to her. She got it before I did. She phoned and said,
"Dad, put on your dancing shoes!" It read, "Marked improvement on the previous pattern
of widespread osseous metastatic disease. No new bone lesions are seen and the previous
have nearly resolved."
My next test was a bone scan on 2/11/09. It reads, "No definite evidence of osseous
metastatic disease is identified!" Thank you, Lord. Hopefully, my story will encourage
and help others.
TANYA: Those were truly miraculous recoveries! At least in the eyes of conventional
medicine! I do believe that, if the most successful alternative treatments could be
embraced by mainstream cancer organizations, doctors and clinics everywhere, then these
types of recoveries would become commonplace and would no longer be seen as
miracles.
Sometimes people can use chemo or radiation along with an alternative method for
a short while, but many times it is best to stop all toxic treatments altogether.
For instance, Jim Sheridan wrote that chemotherapy can bring the percentage of success
down for those people using his formula for cancer. There are only two chemo drugs
known to be compatible with Protocel
's
effectiveness.
Last but not least, it is also important to know that Protocel
.
I've come across a number of cases where women did not do as well as expected on
Protocel
while they were using Tamoxifen. Tamoxifen DOES alter the metabolism of
breast cancer cells, by putting the cancer cells into a sort of "sleep state," and, since
Protocel
interacts with the metabolism of cancer cells, this alteration MAY make it
harder for Protocel
.
One approach, presented in Outsmart Your Cancer, that DOES appear to work well with
Tamoxifen is called Poly-MVA. This is a more recent method that is having great
results and getting a lot of attention in the alternative cancer treatment field. Poly-MVA
is also a liquid formula, and it also directly kills cancer. But it works on the cancer cells
in a completely different way than Protocel