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Radiobiology

From Wikipedia, the free encyclopedia
(Redirected from Radiation biology)

Radiobiology (also known as radiation biology, and uncommonly as actinobiology) is a field of clinical and basic medical sciences that involves the study of the effects of ionizing radiation on living things, in particular health effects of radiation. Ionizing radiation is generally harmful and potentially lethal to living things but can have health benefits in radiation therapy for the treatment of cancer and thyrotoxicosis. Its most common impact is the induction of cancer with a latent period of years or decades after exposure. High doses can cause visually dramatic radiation burns, and/or rapid fatality through acute radiation syndrome. Controlled doses are used for medical imaging and radiotherapy.

Health effects

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In general, ionizing radiation is harmful and potentially lethal to living beings but can have health benefits in radiation therapy for the treatment of cancer and thyrotoxicosis.

Most adverse health effects of radiation exposure may be grouped in two general categories:

  • deterministic effects (harmful tissue reactions) due in large part to the killing or malfunction of cells following high doses; and
  • stochastic effects, i.e., cancer and heritable effects involving either cancer development in exposed individuals owing to mutation of somatic cells or heritable disease in their offspring owing to mutation of reproductive (germ) cells.[1]

Stochastic

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Some effects of ionizing radiation on human health are stochastic, meaning that their probability of occurrence increases with dose, while the severity is independent of dose.[2] Radiation-induced cancer, teratogenesis, cognitive decline, and heart disease are all stochastic effects induced by ionizing radiation.

Its most common impact is the stochastic induction of cancer with a latent period of years or decades after exposure. The mechanism by which this occurs is well understood, but quantitative models predicting the level of risk remain controversial. The most widely accepted model posits that the incidence of cancers due to ionizing radiation increases linearly with effective radiation dose at a rate of 5.5% per sievert.[3] If this linear model is correct, then natural background radiation is the most hazardous source of radiation to general public health, followed by medical imaging as a close second.

Quantitative data on the effects of ionizing radiation on human health is relatively limited compared to other medical conditions because of the low number of cases to date, and because of the stochastic nature of some of the effects. Stochastic effects can only be measured through large epidemiological studies where enough data has been collected to remove confounding factors such as smoking habits and other lifestyle factors. The richest source of high-quality data comes from the study of Japanese atomic bomb survivors. In vitro and animal experiments are informative, but radioresistance varies greatly across species.

The added lifetime risk of developing cancer by a single abdominal CT of 8 mSv is estimated to be 0.05%, or 1 in 2,000.[4]

Deterministic

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Deterministic effects are those that reliably occur above a threshold dose, and their severity increases with dose.[2]

High radiation dose gives rise to deterministic effects which reliably occur above a threshold, and their severity increases with dose. Deterministic effects are not necessarily more or less serious than stochastic effects; either can ultimately lead to a temporary nuisance or a fatality. Examples of deterministic effects are:

The US National Academy of Sciences Biological Effects of Ionizing Radiation Committee "has concluded that there is no compelling evidence to indicate a dose threshold below which the risk of tumor induction is zero".[5]

Phase Symptom Whole-body absorbed dose (Gy)
1–2 Gy 2–6 Gy 6–8 Gy 8–30 Gy > 30 Gy
Immediate Nausea and vomiting 5–50% 50–100% 75–100% 90–100% 100%
Time of onset 2–6 h 1–2 h 10–60 min < 10 min Minutes
Duration < 24 h 24–48 h < 48 h < 48 h — (patients die in < 48 h)
Diarrhea None None to mild (< 10%) Heavy (> 10%) Heavy (> 95%) Heavy (100%)
Time of onset 3–8 h 1–3 h < 1 h < 1 h
Headache Slight Mild to moderate (50%) Moderate (80%) Severe (80–90%) Severe (100%)
Time of onset 4–24 h 3–4 h 1–2 h < 1 h
Fever None Moderate increase (10–100%) Moderate to severe (100%) Severe (100%) Severe (100%)
Time of onset 1–3 h < 1 h < 1 h < 1 h
CNS function No impairment Cognitive impairment 6–20 h Cognitive impairment > 24 h Rapid incapacitation Seizures, tremor, ataxia, lethargy
Latent period 28–31 days 7–28 days < 7 days None None
Illness Mild to moderate Leukopenia
Fatigue
Weakness
Moderate to severe Leukopenia
Purpura
Hemorrhage
Infections
Alopecia after 3 Gy
Severe leukopenia
High fever
Diarrhea
Vomiting
Dizziness and disorientation
Hypotension
Electrolyte disturbance
Nausea
Vomiting
Severe diarrhea
High fever
Electrolyte disturbance
Shock
— (patients die in < 48h)
Mortality Without care 0–5% 5–95% 95–100% 100% 100%
With care 0–5% 5–50% 50–100% 99–100% 100%
Death 6–8 weeks 4–6 weeks 2–4 weeks 2 days – 2 weeks 1–2 days
Table source[6]

By type of radiation

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When alpha particle emitting isotopes are ingested, they are far more dangerous than their half-life or decay rate would suggest. This is due to the high relative biological effectiveness of alpha radiation to cause biological damage after alpha-emitting radioisotopes enter living cells. Ingested alpha emitter radioisotopes such as transuranics or actinides are an average of about 20 times more dangerous, and in some experiments up to 1000 times more dangerous than an equivalent activity of beta emitting or gamma emitting radioisotopes. If the radiation type is not known, it can be determined by differential measurements in the presence of electrical fields, magnetic fields, or with varying amounts of shielding.

External dose quantities used in radiation protection. See article on sievert on how these are calculated and used.

In pregnancy

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The risk for developing radiation-induced cancer at some point in life is greater when exposing a fetus than an adult, both because the cells are more vulnerable when they are growing, and because there is much longer lifespan after the dose to develop cancer. If there is too much radiation exposure there could be harmful effects on the unborn child or reproductive organs.[7] Research shows that scanning more than once in nine months can harm the unborn child.[8]

Possible deterministic effects include of radiation exposure in pregnancy include miscarriage, structural birth defects, growth restriction and intellectual disability.[9] The deterministic effects have been studied at for example survivors of the atomic bombings of Hiroshima and Nagasaki and cases where radiation therapy has been necessary during pregnancy:

Gestational age Embryonic age Effects Estimated threshold dose (mGy)
2 to 4 weeks 0 to 2 weeks Miscarriage or none (all or nothing) 50 - 100[9]
4 to 10 weeks 2 to 8 weeks Structural birth defects 200[9]
Growth restriction 200 - 250[9]
10 to 17 weeks 8 to 15 weeks Severe intellectual disability 60 - 310[9]
18 to 27 weeks 16 to 25 weeks Severe intellectual disability (lower risk) 250 - 280[9]

The intellectual deficit has been estimated to be about 25 IQ points per 1,000 mGy at 10 to 17 weeks of gestational age.[9]

These effects are sometimes relevant when deciding about medical imaging in pregnancy, since projectional radiography and CT scanning exposes the fetus to radiation.

Also, the risk for the mother of later acquiring radiation-induced breast cancer seems to be particularly high for radiation doses during pregnancy.[10]

Measurement

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The human body cannot sense ionizing radiation except in very high doses, but the effects of ionization can be used to characterize the radiation. Parameters of interest include disintegration rate, particle flux, particle type, beam energy, kerma, dose rate, and radiation dose.

The monitoring and calculation of doses to safeguard human health is called dosimetry and is undertaken within the science of health physics. Key measurement tools are the use of dosimeters to give the external effective dose uptake and the use of bio-assay for ingested dose. The article on the sievert summarises the recommendations of the ICRU and ICRP on the use of dose quantities and includes a guide to the effects of ionizing radiation as measured in sieverts, and gives examples of approximate figures of dose uptake in certain situations.

The committed dose is a measure of the stochastic health risk due to an intake of radioactive material into the human body. The ICRP states "For internal exposure, committed effective doses are generally determined from an assessment of the intakes of radionuclides from bioassay measurements or other quantities. The radiation dose is determined from the intake using recommended dose coefficients".[11]

Absorbed, equivalent and effective dose

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The absorbed dose is a physical dose quantity D representing the mean energy imparted to matter per unit mass by ionizing radiation. In the SI system of units, the unit of measure is joules per kilogram, and its special name is gray (Gy).[12] The non-SI CGS unit rad is sometimes also used, predominantly in the USA.

To represent stochastic risk the equivalent dose H T and effective dose E are used, and appropriate dose factors and coefficients are used to calculate these from the absorbed dose.[13] Equivalent and effective dose quantities are expressed in units of the sievert or rem which implies that biological effects have been taken into account. These are usually in accordance with the recommendations of the International Committee on Radiation Protection (ICRP) and International Commission on Radiation Units and Measurements (ICRU). The coherent system of radiological protection quantities developed by them is shown in the accompanying diagram.

Organizations

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The International Commission on Radiological Protection (ICRP) manages the International System of Radiological Protection, which sets recommended limits for dose uptake. Dose values may represent absorbed, equivalent, effective, or committed dose.

Other important organizations studying the topic include:

Exposure pathways

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External

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A schematic diagram showing a rectangle being irradiated by an external source (in red) of radiation (shown in yellow)
A schematic diagram showing a rectangle being irradiated by radioactive contamination (shown in red) which is present on an external surface such as the skin; this emits radiation (shown in yellow), which can enter the animal's body

External exposure is exposure which occurs when the radioactive source (or other radiation source) is outside (and remains outside) the organism which is exposed. Examples of external exposure include:

  • A person who places a sealed radioactive source in his pocket
  • A space traveller who is irradiated by cosmic rays
  • A person who is treated for cancer by either teletherapy or brachytherapy. While in brachytherapy the source is inside the person it is still considered external exposure because it does not result in a committed dose.
  • A nuclear worker whose hands have been dirtied with radioactive dust. Assuming that his hands are cleaned before any radioactive material can be absorbed, inhaled or ingested, skin contamination is considered to be external exposure.

External exposure is relatively easy to estimate, and the irradiated organism does not become radioactive, except for a case where the radiation is an intense neutron beam which causes activation.

By type of medical imaging

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Target organs Exam type Effective dose in adults[14] Equivalent time of background radiation[14]
CT of the head Single series 2 mSv 8 months
With + without radiocontrast 4 mSv 16 months
Chest CT of the chest 7 mSv 2 years
CT of the chest, lung cancer screening protocol 1.5 mSv 6 months
Chest X-ray 0.1 mSv 10 days
Heart Coronary CT angiography 12 mSv 4 years
Coronary CT calcium scan 3 mSv 1 year
Abdominal CT of abdomen and pelvis 10 mSv 3 years
CT of abdomen and pelvis, low dose protocol 3 mSv[15] 1 year
CT of abdomen and pelvis, with + without radiocontrast 20 mSv 7 years
CT Colonography 6 mSv 2 years
Intravenous pyelogram 3 mSv 1 year
Upper gastrointestinal series 6 mSv 2 years
Lower gastrointestinal series 8 mSv 3 years
Spine Spine X-ray 1.5 mSv 6 months
CT of the spine 6 mSv 2 years
Extremities X-ray of extremity 0.001 mSv 3 hours
Lower extremity CT angiography 0.3 - 1.6 mSv[16] 5 weeks - 6 months
Dental X-ray 0.005 mSv 1 day
DEXA (bone density) 0.001 mSv 3 hours
PET-CT combination 25 mSv 8 years
Mammography 0.4 mSv 7 weeks

Internal

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Internal exposure occurs when the radioactive material enters the organism, and the radioactive atoms become incorporated into the organism. This can occur through inhalation, ingestion, or injection. Below are a series of examples of internal exposure.

  • The exposure caused by potassium-40 present within a normal person.
  • The exposure to the ingestion of a soluble radioactive substance, such as 89Sr in cows' milk.
  • A person who is being treated for cancer by means of a radiopharmaceutical where a radioisotope is used as a drug (usually a liquid or pill). A review of this topic was published in 1999.[17] Because the radioactive material becomes intimately mixed with the affected object it is often difficult to decontaminate the object or person in a case where internal exposure is occurring. While some very insoluble materials such as fission products within a uranium dioxide matrix might never be able to truly become part of an organism, it is normal to consider such particles in the lungs and digestive tract as a form of internal contamination which results in internal exposure.
  • Boron neutron capture therapy (BNCT) involves injecting a boron-10 tagged chemical that preferentially binds to tumor cells. Neutrons from a nuclear reactor are shaped by a neutron moderator to the neutron energy spectrum suitable for BNCT treatment. The tumor is selectively bombarded with these neutrons. The neutrons quickly slow down in the body to become low energy thermal neutrons. These thermal neutrons are captured by the injected boron-10, forming excited (boron-11) which breaks down into lithium-7 and a helium-4 alpha particle both of these produce closely spaced ionizing radiation. This concept is described as a binary system using two separate components for the therapy of cancer. Each component in itself is relatively harmless to the cells, but when combined for treatment they produce a highly cytocidal (cytotoxic) effect which is lethal (within a limited range of 5-9 micrometers or approximately one cell diameter). Clinical trials, with promising results, are currently carried out in Finland and Japan.

When radioactive compounds enter the human body, the effects are different from those resulting from exposure to an external radiation source. Especially in the case of alpha radiation, which normally does not penetrate the skin, the exposure can be much more damaging after ingestion or inhalation. The radiation exposure is normally expressed as a committed dose.

History

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Although radiation was discovered in late 19th century, the dangers of radioactivity and of radiation were not immediately recognized. Acute effects of radiation were first observed in the use of X-rays when German physicist Wilhelm Röntgen intentionally subjected his fingers to X-rays in 1895. He published his observations concerning the burns that developed, though he misattributed them to ozone, a free radical produced in air by X-rays. Other free radicals produced within the body are now understood to be more important. His injuries healed later.

As a field of medical sciences, radiobiology originated from Leopold Freund's 1896 demonstration of the therapeutic treatment of a hairy mole using the newly discovered form of electromagnetic radiation called X-rays. After irradiating frogs and insects with X-rays in early 1896, Ivan Romanovich Tarkhanov concluded that these newly discovered rays not only photograph, but also "affect the living function".[18] At the same time, Pierre and Marie Curie discovered the radioactive polonium and radium later used to treat cancer.

The genetic effects of radiation, including the effects on cancer risk, were recognized much later. In 1927 Hermann Joseph Muller published research showing genetic effects, and in 1946 was awarded the Nobel prize for his findings.

More generally, the 1930s saw attempts to develop a general model for radiobiology. Notable here was Douglas Lea,[19][20] whose presentation also included an exhaustive review of some 400 supporting publications.[21][page needed][22]

Before the biological effects of radiation were known, many physicians and corporations had begun marketing radioactive substances as patent medicine and radioactive quackery. Examples were radium enema treatments, and radium-containing waters to be drunk as tonics. Marie Curie spoke out against this sort of treatment, warning that the effects of radiation on the human body were not well understood. Curie later died of aplastic anemia caused by radiation poisoning. Eben Byers, a famous American socialite, died of multiple cancers (but not acute radiation syndrome) in 1932 after consuming large quantities of radium over several years; his death drew public attention to dangers of radiation. By the 1930s, after a number of cases of bone necrosis and death in enthusiasts, radium-containing medical products had nearly vanished from the market.

In the United States, the experience of the so-called Radium Girls, where thousands of radium-dial painters contracted oral cancers[23]— but no cases of acute radiation syndrome[24]— popularized the warnings of occupational health associated with radiation hazards. Robley D. Evans, at MIT, developed the first standard for permissible body burden of radium, a key step in the establishment of nuclear medicine as a field of study. With the development of nuclear reactors and nuclear weapons in the 1940s, heightened scientific attention was given to the study of all manner of radiation effects.

The atomic bombings of Hiroshima and Nagasaki resulted in a large number of incidents of radiation poisoning, allowing for greater insight into its symptoms and dangers. Red Cross Hospital surgeon Dr. Terufumi Sasaki led intensive research into the Syndrome in the weeks and months following the Hiroshima bombings. Sasaki and his team were able to monitor the effects of radiation in patients of varying proximities to the blast itself, leading to the establishment of three recorded stages of the syndrome. Within 25–30 days of the explosion, the Red Cross surgeon noticed a sharp drop in white blood cell count and established this drop, along with symptoms of fever, as prognostic standards for Acute Radiation Syndrome.[25] Actress Midori Naka, who was present during the atomic bombing of Hiroshima, was the first incident of radiation poisoning to be extensively studied. Her death on August 24, 1945, was the first death ever to be officially certified as a result of radiation poisoning (or "atomic bomb disease").

The Atomic Bomb Casualty Commission and the Radiation Effects Research Foundation have been monitoring the health status of the survivors and their descendants since 1946. They have found that radiation exposure increases cancer risk, but also that the average lifespan of survivors was reduced by only a few months compared to those not exposed to radiation. No health effects of any sort have thus far been detected in children of the survivors.[26]

Areas of interest

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The interactions between organisms and electromagnetic fields (EMF) and ionizing radiation can be studied in a number of ways:

Radiation sources for experimental radiobiology

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Radiobiology experiments typically make use of a radiation source which could be:

See also

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References

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  1. ^ ICRP 2007, p. 49, paragraph 55.
  2. ^ a b c Christensen DM, Iddins CJ, Sugarman SL (February 2014). "Ionizing radiation injuries and illnesses". Emerg Med Clin North Am. 32 (1). Elsevier: 245–65. doi:10.1016/j.emc.2013.10.002. PMID 24275177.Note: first page available free at URL.
  3. ^ ICRP 2007, p. 55, Paragraph 83.
  4. ^ "Do CT scans cause cancer?". Harvard Health Publishing. Harvard University. March 2013. Retrieved 15 Jul 2020. Note: First paragraph provided free.
  5. ^ National Research Council (2006). Health Risks from Exposure to Low Levels of Ionizing Radiation: BEIR VII Phase 2. National Academy of Science. p. 10. doi:10.17226/11340. ISBN 978-0-309-09156-5. Retrieved 11 Nov 2013.
  6. ^ "Radiation Exposure and Contamination - Injuries; Poisoning - Merck Manuals Professional Edition". Merck Manuals Professional Edition. Retrieved 6 Sep 2017.
  7. ^ Ratnapalan, Savithiri; Bentur, Yedidia; Koren, Gideon (2 December 2008). ""Doctor, will that x-ray harm my unborn child?"". CMAJ. 179 (12): 1293–1296. doi:10.1503/cmaj.080247. ISSN 0820-3946. PMC 2585137. PMID 19047611.
  8. ^ Ratnapalan, Savithiri; Bentur, Yedidia; Koren, Gideon (2 December 2008). ""Doctor, will that x-ray harm my unborn child?"". CMAJ. 179 (12): 1293–1296. doi:10.1503/cmaj.080247. ISSN 0820-3946. PMC 2585137. PMID 19047611.
  9. ^ a b c d e f g "Guidelines for Diagnostic Imaging During Pregnancy and Lactation". American Congress of Obstetricians and Gynecologists. February 2016
  10. ^ Ronckers, Cécile M; Erdmann, Christine A; Land, Charles E (23 November 2004). "Radiation and breast cancer: a review of current evidence". Breast Cancer Research (Review article.). 7 (1). BMC (Springer Nature): 21–32. doi:10.1186/bcr970. ISSN 1465-542X. PMC 1064116. PMID 15642178.
  11. ^ ICRP 2007, p. 73, paragraph 144.
  12. ^ ICRP 2007, p. 24, glossary.
  13. ^ ICRP 2007, pp. 61–62, paragraphs 104 and 105.
  14. ^ a b Unless otherwise specified in boxes, reference is:
    - "Radiation Dose in X-Ray and CT Exams". RadiologyInfo.org by Radiological Society of North America. Retrieved 23 Oct 2017.
  15. ^ Brisbane, Wayne; Bailey, Michael R.; Sorensen, Mathew D. (2016). "An overview of kidney stone imaging techniques". Nature Reviews Urology (Review article). 13 (11). Springer Nature: 654–662. doi:10.1038/nrurol.2016.154. ISSN 1759-4812. PMC 5443345. PMID 27578040.
  16. ^ Zhang, Zhuoli; Qi, Li; Meinel, Felix G.; Zhou, Chang Sheng; Zhao, Yan E.; Schoepf, U. Joseph; Zhang, Long Jiang; Lu, Guang Ming (2014). "Image Quality and Radiation Dose of Lower Extremity CT Angiography Using 70 kVp, High Pitch Acquisition and Sinogram-Affirmed Iterative Reconstruction". PLOS ONE. 9 (6): e99112. Bibcode:2014PLoSO...999112Q. doi:10.1371/journal.pone.0099112. ISSN 1932-6203. PMC 4051648. PMID 24915439.
  17. ^ Wynn, Volkert; Hoffman, Timothy (1999). "Therapeutic Radiopharmaceuticals". Chemical Reviews (Review article). 99 (9). ACS Publications: 2269–92. doi:10.1021/cr9804386. PMID 11749482.
  18. ^ Y. B. Kudriashov. Radiation Biophysics. ISBN 9781600212802. Page xxi.
  19. ^ Hall, E J (1 May 1976). "Radiation and the single cell: the physicist's contribution to radiobiology". Physics in Medicine and Biology (Lecture). 21 (3). IOP: 347–359. doi:10.1088/0031-9155/21/3/001. PMID 819945. S2CID 250827449.
  20. ^ Lea, Douglas E. "Radiobiology in the 1940s". British Institute of Radiology. Retrieved 15 Jul 2020.
  21. ^ Lea, Douglas (1955). Actions of Radiations on Living Cells (2nd ed.). Cambridge: Cambridge University Press. ISBN 9781001281377.
  22. ^ Mitchell, J. S. (2 November 1946). "Actions of Radiations on Living Cells". Nature (Book review). 158 (4018): 601–602. Bibcode:1946Natur.158..601M. doi:10.1038/158601a0. PMC 1932419.
  23. ^ Grady, Denise (6 October 1998). "A Glow in the Dark, and a Lesson in Scientific Peril". The New York Times. Retrieved 25 Nov 2009.
  24. ^ Rowland, R.E. (1994). Radium in Humans: A Review of U.S. Studies. Argonne National Laboratory. doi:10.2172/751062. OSTI 751062. Retrieved 24 May 2012.
  25. ^ Carmichael, Ann G. (1991). Medicine: A Treasury of Art and Literature. New York: Harkavy Publishing Service. p. 376. ISBN 978-0-88363-991-7.
  26. ^ "Long-term health effects of Hiroshima and Nagasaki atomic bombs not as dire as perceived". Science Daily. 11 August 2016. Retrieved 16 Oct 2021.
  27. ^ Pattison JE, Hugtenburg RP, Beddoe AH, Charles MW (2001). "Experimental Simulation of A-bomb Gamma-ray Spectra for Radiobiology Studies" (PDF). Radiation Protection Dosimetry. 95 (2). Oxford Academic: 125–136. doi:10.1093/oxfordjournals.rpd.a006532. PMID 11572640. S2CID 8711325. Archived from the original (PDF) on 16 Jul 2020.

Sources

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Further reading

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  • Eric Hall, Radiobiology for the Radiologist. 2006. Lippincott
  • G.Gordon Steel, "Basic Clinical Radiobiology". 2002. Hodder Arnold.
  • The Institute for Radiation Biology at the Helmholtz-Center for Environmental Health [1]