Reproductive Health 1

REPRODUCTIVE HEALTH
Unit one Content..
Topic one: Standards of Reproductive health care in Kenya, Policies and

initiatives related to Reproductive Health
Definition of terms
 · Reproductive Health is a state of complete physical, mental,

emotional, and social well-being, and not merely the absence of disease or
infirmity, in all matters relating to the reproductive system and its functions
and processes.
 · Reproductive Health Care is the appropriate constellation of
methods, technologies and services that will ensure reproductive health and
well-being by preventing and solving problems related to human reproduction
and sexuality.
Basic Elements in Reproductive Health
 · Ability - to reproduce, regulate fertility and enjoy healthy relationships

 · Success - result in child survival, growth and health development
 · Safety - Fertility regulation, pregnancy and child health
Components of Reproductive Health
o · Family Planning
o · Safe motherhood (Maternal and Newborn Health)
o · Management of STIs/RTIs and HIV/AIDS
o · Promotion of Adolescent and Youth Sexual and Reproductive
Health
o · Management of Infertility
o · Gender Issues, Sexual and Reproductive Rights
o · Reproductive Health Research
o · Monitoring and Evaluation
o · Community Reproductive Health
o · Reproductive Tract Cancers
o · Reproductive Needs of the Elderly (Andropause/Menopause)
Significance of Studying RH
o · Reproductive health is a right

o · Lead a responsible and satisfied sex life.
o · To reproduce and freedom to decide when and how often to do
so
o · To be informed about advantages, possible risks and side
effects of contraceptives
o · To have free, equal access to safe, effective, affordable, and
acceptable method of fertility regulation.
o · To get access to appropriate health service of good quality to go
through safe pregnancy and child
 · Kenya has made steady progress in improving reproductive, maternal and

child health outcomes in the last decade.
 · Child mortality has declined by over 20 percent since 2008 and the country
achieved a total fertility rate of less than four.
 · Stunting, which remained stubbornly high over the past two decades has
started to decline.
 · Six out of ten pregnant women now receive skilled care at child birth and
over half receive postnatal care
 · However, despite this progress, Kenya could not achieve maternal and
child health Millennium Development Goals (MDGs).
 · In Kenya today, many women, neonates, children, and adolescents
continue to experience morbidity or die from preventable conditions that have
proven and cost-effective interventions.
 · Access to quality Reproductive Maternal Newborn Child and Adolescent
Health (RMNCAH) services remains a challenge across all levels of care, and
inequities continue to persist among population sub-groups, and between rich
and the poor.

 · The key supply side challenges include:
1. sub-optimal functioning of the health system with uneven

distribution of the health workforce as well as constraints in
competency and motivation of the health care providers to
provide quality care;
2. insufficient financing and weak supply chain management
resulting in missing critical inputs required for service delivery,
especially essential commodities; and
3. poor quality and utilization of routine data for evidence-based
decision making.
o · Sociocultural and economic barriers and constraints in physical

access to health services continue to limit demand
o
o · Globally, there is also a renewed momentum and support for
RMNCAH as part of the Sustainable Development Goals (SDGs) and
the updated Global Strategy for Women’s Children’s and Adolescent’s
Health (2016-2030) which aims to achieve the highest attainable
standard of health for all women, children and adolescents, and
ensures that every newborn, mother and child not only survives, but
thrives.
o
o · Such growing national and international commitments provide an
opportune time to enhance both domestic and external support for
RMNCAH in Kenya to ensure smart, scaled-up, and sustained
financing.
o
o · Improving coverage for RMNCAH services is a priority for the
Government of Kenya as is reflected in its Vision 2030, the Constitution
of 2010 and the Health Sector Strategic and Investment Plan 2014-18.
o · The Government has introduced new policies as well as initiatives
such as Free Maternity Services, Elimination of User Fee for Primary
Care and the Beyond Zero campaign to address the critical barriers.
Status of Key Indicators
Key indicators KDHS KDHS Sub-Saharan

2008/09 2014 Africa Region
NMR (per 1,000 Live births) 31 22 31.1
Infant mortality rate (per 1,000 Live births) 52 39 61.1
Under-five mortality rate (per 1,000 Live births) 74 52 92.4
Maternal mortality ratio (per 100,000 live births) 488 360 510
Total fertility rate (per women) 4.6 3.9 5.0
Teen pregnancy (%) 18 18 -
Children under-five stunted (%) 35 26 -
Deliveries attended by a skilled provider (%) 43 62 48.6
Pregnant women received any antenatal care (%) 92 96 77
Children received all basic vaccines (%) 65 71 -
Children under 6 months exclusively breastfed (%) 32 61 37.7
Contraceptive prevalence rate (any method) among 46 58 23.6
currently married women (%)

Unmet need for family planning (%) 25 18 24.4
Maternal Mortality
 "A maternal death is defined as the death of a woman while pregnant or within
42 days of termination of the pregnancy, irrespective of the duration and site
of pregnancy, from any cause related to or aggravated by the pregnancy or its
management, but not from accidental or incidental causes."
Direct Causes of Maternal Mortality
 These result from obstetric complications of pregnancy, labour and the

puerperium and from interventions or any after effects of these events.
 The Five major causes of direct maternal deaths in order of frequency are:
o Hemorrhage,
o Sepsis,
o Hypertensive disorders,
o Complications of abortion and
o obstructed labour
 Incidental/Coincidental causes
 are deaths that were neither due to direct nor indirect obstetric causes. E.g.
car accident, fire burn, bullet injury, etc.

 Indirect Causes of Maternal Mortality
 They result from previously existing disease or disease that develops during
pregnancy which was not due to direct obstetric causes, but which was
aggravated by physiologic effects of pregnancy.
 These include:
 o Malaria,
 o HIV/AIDS
 o Anemia.
 Maternal Morbidity
 For every woman who dies another 30 suffer long term injuries and illness
due to pregnancy and childbirth related complications.
 Maternal morbidity is any symptom or condition resulting from or made worse
by pregnancy.
 Severe maternal morbidity (Near Miss) is defined as: “any pregnant or
recently delivered woman (within six weeks after termination of pregnancy or
delivery), in whom immediate survival is threatened and who survives by
chance or because of the hospital care she receives.”
Causes of Maternal Morbidity
 Infection: There is high risk of infection of the genital organs (cervix, uterus,
tubes, Ovaries and peritoneum) after prolonged labor.
 Fistula: are holes in the birth canal that allow leakage from the urethra,
bladder or rectum into the vagina. Women present with continuous leakage of
urine or feces or both. The commonest cause in our country is obstructed
labor as opposed to surgery and cancer in the developed world.
 Incontinence: is involuntary leakage of urine.
 Uterine prolapse: the falling or sliding of the uterus from its normal position
into the vaginal canal. Commonest predisposing factors include prolonged
labor, heavy exercise, multiple childbirths, etc.
 Infertility: inability to become pregnant for a year despite unprotected sexual
intercourse.
 Nerve Damage: As a result of prolonged labor, there may be compression or
damage of the nerves in the pelvis (Sciatic nerve) may result in foot drop and
contractures.
 Psychosocial problems: such as anxiety, depression, and psychosexual
problem. Others Include pain during intercourse, low back pain, anemia, etc
 Underlying Causes of Maternal & Neonatal Mortality (The Three Delays)

 There are three distinct levels of delay which contribute to maternal morbidity
and mortality: (Thadaseus and Maine, 1994):
o
o Delay in deciding to seek appropriate care. This could be due to:
socio-cultural barriers, Failure to recognize danger signs, failure to
perceive severity of illness, and cost considerations
o Delay in reaching an appropriate health care facility. This is due to:
long distance to a facility, poor condition of roads, lack of transportation
and cost considerations
o Delay in receiving adequate emergency care at the facility. This
may be due to: Shortage of staff, supplies and basic equipment;
unskilled personnel, user fees among others
 Risk factors affecting maternal health

o Socio-cultural factors: lack of literacy, early marriage, early childbirth,
harmful traditional practices including female genital mutilation, etc.
o Economy: Socio economic status affects women’s status by affecting
their decision- making roles in the community, educational status,
health service accessibility, prostitution, etc.
o Inadequate Health Service Coverage: More than 70% mothers do
not get care during pregnancy and more than 90 % of deliveries are
unattended. This can be due to lack of transportation, distance from
health facilities, small number of health facilities, lack of knowledge
about importance of health services, lack of money, and lack of family
support
o Psychological factors: Fear of childbirth, too many pregnancies,
death of other children illness in family. Women are at great risk of
depression after sexual abuse, divorce as a result of marriage without
consent and after Vesico-Vaginal/Recto- Vaginal fistula (VVF/RVF).
o Health and nutrition services: The health status of women who are
not getting adequate nutrients and proper reproductive health services
could be affected
o Interaction with providers: Some health care providers are not
empathetic and caring. They do not respect women's cultural
preferences for privacy, birth position, or the preference for treatment
by women providers.
o Gender Discrimination: The family may give more attention to a male
child with regard to education, nutrition; may want the mother to
produce boys. Policy decisions, inheritance etc.
 Maternal Morbidity
 For every woman who dies another 30 suffer long term injuries and illness
due to pregnancy and childbirth related complications.
 Maternal morbidity is any symptom or condition resulting from or made worse
by pregnancy.
 Severe maternal morbidity (Near Miss) is defined as: “any pregnant or
recently delivered woman (within six weeks after termination of pregnancy or
delivery), in whom immediate survival is threatened and who survives by
chance or because of the hospital care she receives.”
Causes of Maternal Morbidity
 Infection: There is high risk of infection of the genital organs (cervix, uterus,
tubes, Ovaries and peritoneum) after prolonged labor.
 Fistula: are holes in the birth canal that allow leakage from the urethra,
bladder or rectum into the vagina. Women present with continuous leakage of
urine or feces or both. The commonest cause in our country is obstructed
labor as opposed to surgery and cancer in the developed world.
 Incontinence: is involuntary leakage of urine.
 Uterine prolapse: the falling or sliding of the uterus from its normal position
into the vaginal canal. Commonest predisposing factors include prolonged
labor, heavy exercise, multiple childbirths, etc.
 Infertility: inability to become pregnant for a year despite unprotected sexual
intercourse.
 Nerve Damage: As a result of prolonged labor, there may be compression or
damage of the nerves in the pelvis (Sciatic nerve) may result in foot drop and
contractures.
 Psychosocial problems: such as anxiety, depression, and psychosexual
problem. Others Include pain during intercourse, low back pain, anemia, etc
 Underlying Causes of Maternal & Neonatal Mortality (The Three Delays)

 There are three distinct levels of delay which contribute to maternal morbidity
and mortality: (Thadaseus and Maine, 1994):
o
o Delay in deciding to seek appropriate care. This could be due to:
socio-cultural barriers, Failure to recognize danger signs, failure to
perceive severity of illness, and cost considerations
o Delay in reaching an appropriate health care facility. This is due to:
long distance to a facility, poor condition of roads, lack of transportation
and cost considerations
o Delay in receiving adequate emergency care at the facility. This
may be due to: Shortage of staff, supplies and basic equipment;
unskilled personnel, user fees among others
 Risk factors affecting maternal health

o Socio-cultural factors: lack of literacy, early marriage, early childbirth,
harmful traditional practices including female genital mutilation, etc.
o Economy: Socio economic status affects women’s status by affecting
their decision- making roles in the community, educational status,
health service accessibility, prostitution, etc.
o Inadequate Health Service Coverage: More than 70% mothers do
not get care during pregnancy and more than 90 % of deliveries are
unattended. This can be due to lack of transportation, distance from
health facilities, small number of health facilities, lack of knowledge
about importance of health services, lack of money, and lack of family
support
o Psychological factors: Fear of childbirth, too many pregnancies,
death of other children illness in family. Women are at great risk of
depression after sexual abuse, divorce as a result of marriage without
consent and after Vesico-Vaginal/Recto- Vaginal fistula (VVF/RVF).
o Health and nutrition services: The health status of women who are
not getting adequate nutrients and proper reproductive health services
could be affected
o Interaction with providers: Some health care providers are not
empathetic and caring. They do not respect women's cultural
preferences for privacy, birth position, or the preference for treatment
by women providers.
o Gender Discrimination: The family may give more attention to a male
child with regard to education, nutrition; may want the mother to
produce boys. Policy decisions, inheritance etc.
The Kenya Maternal and Newborn Health Model (2009)
The Kenya Maternal and Newborn Health (MNH) Pillars
1. Family planning and pre-pregnancy care: To ensure that individuals and
couples have the information and services to plan the timing, number and spacing
of pregnancies.
2. Focused Antenatal Care – To prevent complications where possible and ensure
that complications of pregnancy are detected early and treated appropriately.
3. Essential Obstetric Care – To ensure that essential care for the high-risk
pregnancies and complications is made available to all women who need it.
4. Essential Newborn Care – To ensure that essential care is given to newborns from
the time they are born up to 28 days in order to prevent complications that may arise
after birth
5. Targeted Postpartum Care– To prevent any complication occurring after childbirth
and ensure that both mother and baby are healthy and there is no transmission of
infection from mother to child.
6. Post Abortion Care – to provide clinical treatment to all women and girls
seeking care, for complications of incomplete abortion and miscarriage as well as
counselling and contraceptives.
(Note that HIV services are now integrated into ALL the pillars of MNH and
clean and safe delivery is part of Essential Obstetric Care)
Skilled Attendance
 Evidence has shown that there are 2 key interventions that improve maternal
health and reduce maternal mortality, namely:
o Skilled attendance at delivery (skills, numbers, enabling environment)
and
o availability of Emergency Obstetric Care.
The term "skilled attendant" refers exclusively to people with midwifery skills (e.g.
doctors, midwives, nurses, clinical officers) who have been trained to
proficiency in the skills necessary to manage normal deliveries and
diagnose or refer obstetric complications.
Enabling Environment
 To ensure effective and efficient service delivery, the skilled attendant

requires an enabling environment.
 There is need for appropriate infrastructure as well as ensuring that the
continuum of care is connected by an effective referral system, and
supported by adequate supplies, equipment, drugs, good management
and supportive supervision.
Referral Systems
 A key aspect in ensuring a good maternal health service is a functional
referral system.
 Access to a telephone and/or vehicle, with emergency funds or fuel to
transfer urgent cases day or night is extremely important.
 Good record keeping and use of detailed referral letters will assist in reducing
delay in the care for women with obstetric emergencies and severely ill
newborns.
 The referring unit should be aware of the capacity of the referral point to
manage the client being referred.
Community Action, Partnerships
 Involving community members (particularly women and their families,

health care providers, and local leaders) in efforts to improve maternal
health helps to ensure programme success;
 Community education about obstetric complications and when and where to
seek medical care is important to ensure birth planning/ use of birth
preparedness cards, early recognition of complications and prompt care-
taking behaviour
Male Involvement and Participation
 it is evident that for successful programme implementation, male participation

in MNH results in good outcomes for both mother and baby.
 Male involvement and participation is critical in addressing the first and
second delay.
 In the Kenyan context, men have the resources and are the main decision
makers in the families and communities on issues relating to MNH.
Equity for All
 Rights based perspective helps legitimize prioritization of women’s health.

 It focuses attention on social, economic and geographic inequities.
 Strong political support and national ownership are essential to create
enabling policies to attract resources for maternal and newborn health
and to ensure those resources reach groups with the highest maternal
mortality and morbidity.

Reproductive Rights
 Health care providers should appreciate that most maternal and neonatal
deaths are avoidable, and therefore maternal and newborn health must
be given its due prominence.
 Safe Motherhood is a basic human right as women are entitled to enjoy a
safe pregnancy and childbirth.
Emergency Obstetric Care
 Emergency Obstetric Care refers to a set of minimal health care elements,

which should be availed to all women during pregnancy and delivery.
 It includes both life-saving and emergency measures e.g. Caesarean section,
manual removal of placenta, etc, as well as non-emergency measures (e.g.
use of the partograph to monitor labour, active management of the third
stage of labour, etc.).
 Emergency Obstetric Care functions are generally categorized as Basic
Emergency Obstetric Care (BEmOC) and Comprehensive Emergency
Obstetric care (CEmOC).
 Basic Emergency Obstetric Care Include:
 Administration of IV antibiotics.
 Administration of magnesium sulphate.
 Administration of parental oxytocics.
 Performing manual removal of the placenta.
 Performing removal of retained products.
 Performing assisted vaginal delivery (e.g. by vacuum
extraction).
 Performing newborn resuscitation
 Comprehensive Emergency Obstetric Care

 includes all the seven above, PLUS:
 Performing surgery (Caesarean section), including provision of
emergency obstetric anaesthesia.
 Administration of blood transfusion.
Client Rights
 Right to Information
o All members of the community have a right to information on the
benefits of reproductive health including Maternal and Newborn health
for themselves and their families. They also have a right to information
on how to access the services.

 Right to Access
o All members of the community have a right to receive services from
reproductive health / MNH programs, regardless of their socio-
economic status, political affiliations, religious beliefs, ethnic origin,
marital status or geographical location. Access includes freedom
from barriers such as policies, standards and practices, which are not
scientifically justifiable.

 Right of choice
o Individuals and couples have the right to decide freely where to obtain
RH /MNH services.

 Right to safety
o Clients have a right to safety in the practice of MNH

 Right to Privacy
o Clients have a right to privacy while holding conversation with
service providers and while undergoing physical examination.

 Right to Confidentiality
o The client should be assured that any information she/he provides or
any details of the service received will not be communicated to other
parties without her/his consent.

 Right to Dignity
o Reproductive Health /MNH clients have a right to be treated with
courtesy, consideration, and attentiveness and with full respect of their
dignity regardless of their level of education, social status or any other
characteristics, which would single them out or make them vulnerable
to abuse.

 Right to Comfort
o Clients have a right to comfort when receiving services. This can be
ensured by providing quality services in hygienically safe and
conveniently located service delivery sites.

 Right to Continuity of Care
o Clients have a right to receive services and reliable supply of RH /MNH
commodities and drugs for as long as they need them.

 Right of Opinion
o Clients have a right to express their views freely on the services they
receive.

 Providers’ Rights
 Training
o To continuously have access to the knowledge and skills needed to
perform all the tasks required of them.

 Information
o To be kept informed on issues related to their duties

 Infrastructure
o To have appropriate physical facilities and organization to provide
services at an acceptable level of quality.

 Supplies
o To receive continuous and reliable supplies and materials required for
providing reproductive health services at acceptable standards of
quality.

 Guidance
o To receive clear, relevant and objective guidance.
o
 Back up
o To be reassured that whatever the level of care at which they are
working they will receive support from other individuals or units.

 Respect
o To receive recognition of their competence and potential, and respect
for their human needs.

 Encouragement
o To be given stimulus in the development of their potential, initiative and
creativity.

 Feedback
o To receive feedback concerning their competence and attitudes as
judged by others.

 Self–expression
o To express their views freely, concerning the quality and efficiency of
the reproductive health program.
Policies and initiatives related to Reproductive health
THE SAFE MOTHERHOOD INITIATIVE (SMI)
 Safe motherhood is women’s ability to have a safe and healthy pregnancy and
delivery
 The Global Safe Motherhood Initiative launched in Nairobi in 1987 aimed at reducing
the burden of maternal deaths and ill health in developing countries.
 The Safe Motherhood Initiative differed from other health initiatives in that it focused
on the well-being of women as an end in itself.
 In the SMI, the prevention of the death of a pregnant woman is considered to be the
key objective, not because death adversely affects children and other family
members but because women are intrinsically valuable (Thaddeus and Maine
1994).
 It underscored the fact that Safe motherhood is a basic human right

Summary of SMI Events
 International Conference for Population and Development (ICPD)

 The 1994 International Conference on Population and Development in Cairo
recommended to the international community a set of important
population and development objectives.
 The Programme of Action was striking for the attention it devoted to the issue of
women’s health.
 It also included goals with regard to education, especially for girls, and for the further
reduction of infant, child and maternal mortality levels.
International Conference For Population and Development (ICPD)
 For Kenya, the ICPD recommendations were then translated into the
National Reproductive Health Strategy (NRHS 1997 – 2010) and
implementation plan whose goal was to reduce maternal, perinatal and
neonatal morbidity and mortality.
 Another event that followed the ICPD was the Millennium Declaration in
2000 and the development of goals (MDGs) with indicators.
National Reproductive Health Policy 2007
 The goal of the RH policy is to enhance the Reproductive Health status of all
Kenyans through:
o Increased equitable access to RH services
o Improved quality, efficiency and effectiveness of service delivery at all
levels
o Improved responsiveness to clients’ needs
 The main objective for Safe Motherhood in this RH Policy is to reduce
maternal, peri-natal and neonatal morbidity and mortality in Kenya
 The National Health Sector Strategic Plan (NHSSP II)-2005-2010
 The aim of NHSSP II was to reverse the decline in the health status of
Kenyans through an efficient, high quality health care system that is
accessible, equitable and affordable for every Kenyan household.
 A major feature of the NHSSP is the introduction of the Kenya Essential
Package for Health (KEPH), which focuses on the health needs of individuals
through the six stages of the human life cycle.
 The strategic plan emphasizes strong community involvement in health care
through the community Strategy
 National Reproductive Health Strategy (NRHS): 2009- 2015
 This is a revision of the NRHS 1997-2010 and includes issues and
challenges that had not been incorporated in the original strategy.
 The revision was also necessary in order to align it to the National RH Policy -
2007.
The KEPH Life-Cycle Cohorts
 · They are delineated in the NHSSP II as follows

 o Cohort 1: -Pregnancy, delivery
and the newborn child (up to 2 weeks
of age)
 o Cohort 2: - Early childhood (3
weeks to 5 years)
 o Cohort 3: - Late childhood (6-12
years)
 o Cohort 4: - Adolescence (13-24
years)
 o Cohort 5: - Adulthood (25-59
years)
 o Cohort 6: - Elderly (60 years and
over)
Levels of Care in KEPH
 · The KEPH approach is not only limited to a definition of the target

groups in terms of life-cycle cohorts.
 · It also defines where the health services will be delivered.
 · Under KEPH, promotive, preventive and curative services are provided
at six levels of care:
o Level 6 : tertiary hospitals
o Level 5: secondary hospitals
o Level 4: primary hospitals
o Level 3: health centres,

maternity, nursing homes
o Level 2: dispensaries / clinics
o Level 1:
villages/household/families/individ
uals
NB
 · As a result of the implementation of the constitution of Kenya 2010,

health functions have been devolved to the county.
 · In the structure, County Health Services are organized around three
levels of care:
o Community,
o Primary care, and
o Referral services.
Annual Operational Plans (AOPs)
 The Annual Operational Plans (AOPs) translate Kenya Essential Package for
Health and the National Health Sector Strategic Plan II 2005-2010 into
‘actionable’ operational plans.
 AOPs also improve the planning process within the Ministry in particular
highlighting the need for
 o Improved coordination and decision-making
 o Elimination of duplication of activities and
 o More efficient use of available resources
The Community Strategy
 The community-based approach, is the mechanism through which households

and communities take an active role in health and health-related development
issues.
 Initiatives outlined in the approach target the major priority health and related
problems affecting all cohorts of life at the community and household levels –
level 1 of the KEPH-defined service delivery.
Vision 2030
 Kenya Vision 2030 is the country’s new development blueprint covering the
period 2008 to 2030.
 The vision is based on three “pillars” namely;
 o the economic pillar,
 o the social pillar and
 o the political pillar.
 Health is part of the social pillar.
 To improve the overall livelihoods of Kenyans, the country aims to provide an
efficient and high-quality health care system with the best standards.
 This is in order to reduce health inequalities and improve indicators in key
areas where Kenya is lagging, especially in lowering infant and maternal
mortality.
 Specific strategies include:
 o provision of a robust health infrastructure network;
 o improving the quality of health service delivery to the highest
standards and promotion of partnerships with the private sector.

 In-addition the Government has put in place health financing mechanisms to
make quality MNH services affordable and accessible to all especially the
poor and vulnerable women.
 These include the provision of free MNH /FP services at the lower levels,
National Health Insurance Fund (NSSF), Health Sector Support Fund (HSSF),
Hospital Management Support Fund (HMSF), FIF, Voucher system /Output
Based Aid (OBA).
 The government is also encouraging initiatives that promote community-
based health financing.
Assignment: study the following policies/initiatives
 The Kenya Constitution (2010) calls for the highest attainable standard for
health including reproductive health for all Kenyans
 The Kenya Health Policy (2014-30) commits to strengthening the health care
system and service delivery.
 Kenya Health Sector Strategic and Investment Plan (2014-18) (MOH 2014A,
B, MOH 2012).
 Free Maternity Care
 Elimination of User Fee for Public Primary Health Care Services,
 Beyond Zero campaign.
 Kenya RMNCAH investment framework
 Universal Health Coverage
Millennium Development Goals (MDGs)
 MDGs were set by all Government leaders at the UN Millennium Summit,

September 2000)
 All UN organisations decided to be guided by MDGs in their future action:
unity of purpose, coherent action, synergies and strategic approaches by the
UN system as a whole (guided by CEB)
 Leaders pledged to strive, individually and collectively, towards these goals
through international, regional and national action, concerted by the UN.
Why the MDGs ?
 The 1990s was a decade of faltering progress on:

 Under-5 mortality rate
 Maternal mortality rate
 Child malnutrition
 Water and sanitation
 Income poverty
 Primary education
 MDGs were meant to accelerate progress

Millennium Development Goals (MDGs)
· Goal 1. Eradicate extreme poverty and hunger
· Goal 2. Achieve universal primary education
· Goal 3. Promote gender equality and empower women
· Goal 4. Reduce child mortality
· Goal 5. Improve maternal health
· Goal 6. Combat HIV/AIDS, malaria and other diseases
· Goal 7. Ensure environmental sustainability
· Goal 8. Develop a Global Partnership for Development
MDGS related to RH
· Goal 3 Promote gender equality & empower women
· Goal 4 Reduce child mortality by 2015 the no at 1990
· Goal 5 Improve maternal health
Progress of MDGs Related To RH 2014

Infant Mortality Rate
 The KDHS 2014 shows a decrease in the infant mortality rate from 52 to
39 per 1,000 live births, and a decrease in the under-five mortality rate from
74 to 52 per 1,000 live births between 2008 and 2014.
 These declines have been driven mainly by:
o o Enhanced use of mosquito nets,
o o Increases in antenatal care,
o o skilled attendance at childbirth,
o o Postnatal care,
o o Contraceptive use,
o o exclusive breastfeeding practices and
o o a decrease in unmet family planning (FP) needs,
o o as well as overall improvements in other social indicators such as
education and access to water

Neonatal Mortality Rate
 The NMR declined from 31 per 1,000 births to 22 per 1,000 live births
between 2008-2014.
 However, during the past decade, the NMR exhibited the slowest decline.
 Further reductions in infant and child mortality require steeper decline in the
NMR, which is closely linked to improvements in maternal health services
including intrapartum care.
Maternal Health
 The MMR of 362 per 100,000 live births estimated by KDHS in 2014 is still
high
 Coverage/utilization indicators also show some improvements but much more
needs to be done to address inequities and to reach Universal Health Care
(UHC).
 The contraceptive prevalence rate (CPR, any method) among married women
has increased to 58% in 2014 from 46% in 2008/9 with a decline in unmet
need for FP.
 Nearly two thirds (61%) of births took place in a health facility and 62% of
pregnant women were delivered by a skilled attendant.
 Postnatal care (PNC) increased from 42% in 2009 to 51% in 2014
 The total fertility rate has declined from 4.6 in 2008/9 to 3.9 in 2014; however,
there has been no change in teen pregnancy with one in five (18%)
adolescents in the 15-19 years age group having started child bearing due to
early marriage, high unmet need for contraception and poor access to FP
services.
 Nutritional status of children under-five has improved with a decline in stunting
from 35% in 2008/9 to 26% in 2014.
 However, one out of every four children still remain shorter for their age, a
factor that adversely affects their future health, well-being and economic
productivity.
 Nearly half (48%) of households have access to an insecticide treated net;
 53% of women and 46% of men were tested for HIV in the past 12 months
and received the test results.
 Overall immunization coverage for basic vaccines increased from 65.3
percent 2008/9 to 71.3 percent in 2014 and coverage for measles,
pentavalent and pneumococcal vaccine remained high.
 Prevalence of exclusive breastfeeding among children under 6 months has
nearly doubled from 32 percent to 61 percent
SUSTAINABLE DEVELOPMENT GOALS (SDGs) - The 2030 Agenda for

Sustainable Development
 A set of 17 goals for the world’s future, through 2030

 Backed up by a set of 169 detailed Targets
 Negotiated over a two-year period at the United Nations
 Agreed to by nearly all the world’s nations, on 25 Sept 2015
SDGs:
#1: End poverty in all its forms everywhere
#2: End hunger, achieve food security and improved nutrition and promote
sustainable agriculture
#3: Ensure healthy lives and promote well-being for all at all ages
#4: Ensure inclusive and quality education for all and promote lifelong learning
#5: Achieve gender equality and empower women and girls
#6: Ensure access to water and sanitation for all
#7: Ensure access to affordable, reliable, sustainable and modern energy for all
#8: Promote inclusive and sustainable economic growth, employment and decent
work for all
#9: Build resilient infrastructure, promote sustainable industrialization and foster

innovation
#10: Reduce inequality within and among countries
#11: Make cities inclusive, safe, resilient and sustainable
#12: Ensure sustainable consumption and production patterns
#13: Take urgent action to combat climate change and its impacts*
#14: Conserve and sustainably use the oceans, seas and marine resources
#15: Sustainably manage forests, combat desertification, halt and reverse land
degradation, halt biodiversity loss
#16: Promote justice, peaceful and inclusive societies
#17: Revitalize the global partnership for sustainable development
What is New and Different about the 17 SDGs?
 These Goals apply to every nation … and every sector. Cities, businesses,

schools, organizations, all are challenged to act. This is called Universality
 The Goals are all inter-connected, in a system. We cannot aim to achieve just
one Goal. We must achieve them all. This is called Integration
 Achieving these Goals involves making very big, fundamental changes in how
we live on Earth. This is called Transformation
 The vision is for the goals to promote sustainable development and poverty
eradication.
The first 16 goals address priority areas that:
 o Increase the ambition/ improving and sustaining current achievements

on existing MDG goals (poverty, health education, gender) with added
dimensions on
 o Economic sustainability (inclusive growth, jobs, infrastructure,
industrialization)
 o Environmental sustainability (climate change, oceans and land-based
ecosystems, sustainable consumption and production)
 o All held together by the glue of ‘peaceful and inclusive societies for
sustainable development’ (governance agenda, rule of law, violence).
The 17th goal covers means of implementation (finance, trade, technology, capacity

building, partnerships, and data)
The SDGs versus MDGs
 Key Strengths of the proposed SDGs include: -


o The notion of leaving no one behind – with many targets aspiring
zero/fully coverage (raising the ambition of the MDGs)
o
o Stand-alone goal of Inequality (within and between countries)
o
o Stand-alone goal on gender inequality, including ending of all forms
of violence, discrimination, child marriages, and female genital
mutilations

The SDGs versus MDGs
 Environmental issues are strongly represented – fulfilling a long-sought

marriage between development and environment (climate change, marine
and land base ecosystems, and sustainable consumption and production)
 Governance - for the first time – incorporating a goal and targets
on governance and peaceful societies (legal identity, tackling corruption
and bribery etc)
 Participatory/Inclusiveness Process in formulation of the SDGs : The
participation and buy in of a wide range of stakeholders including member
states and non-governmental organizations
 The broad nature of the SDG is also a reflection of the nature of challenges
facing the world today
Kenya SDG Targets For RH
 Kenya RMNCAH Investment Framework (January 2016)

 The Kenya RMNCAH investment framework sets ambitious targets to
increase:
 o skilled deliveries to 87%,
 o 4+ ANC visits to 69%,
 o full immunization to 76 %,
 o contraceptive use by currently married women in
reproductive age to 73%, and
 o pregnant women tested for HIV who received results
and post-test counseling to 75% by 2020 from the
baselines of the Kenya Demographic and Health Survey
2014 with enhanced focus on quality of services.
 It also aims to reduce stunting to 19%, teenage pregnancy to 11%, and
contribute to decrease in neonatal mortality to 18%.
 The absolute number of deaths of children under-five years is projected to
reduce from 77,761 to 48,590 and maternal from 5,453 to 3,276 between
2014/15 and 2019/20.
 Finally, the framework aims to ensure that at least three out of four births will
be registered, thereby providing more robust denominators to effectively plan
and monitor RMNCAH service delivery.
 Progress on improvements in quality, productivity and efficiency will be
tracked through strengthened routine data, independent surveys, and
implementation research of innovations.
 Impact and outcome level indicators in reducing neonatal, infant, and under-
five mortality rates, and maternal mortality ratio (MMR) will be tracked through
population-based surveys such as the KDHS.
 The proposed Maternal Death Surveillance and Response (MDSR) helps to
identify and register maternal deaths, and support appropriate actions to be
implemented to prevent them.
 Active citizens’ participation and feedback, independent verification and

progress reviews will be used to track achievements of the investments made
in RMNCAH.

 Strengthening Civil Registration and Vital Statistics (CRVS) will be an
essential intervention to inform better planning and enhance accountability to
results.
Devolution in Achieving SDGs Related to RH
 Kenya has introduced an ambitious devolution initiative, which could help to

address the major demand and supply side challenges.
 National RMNCAH serve as a guide for the development and implementation
of county RMNCAH implementation plans, which will be an integral part of
County Integrated Development Plans and aligned with the County Health
Strategic and Investment Plans.
 Devolution has the potential to address inequities and to enhance
accountability.
 Increased government spending is necessary to scale-up interventions but
ensuring effective coverage with an equity focus is critical to improve health
outcomes.
Areas to improve on
 Effective partnerships are critical for success as fragmented financing and

governance cause high transaction costs, hindering effective harmonization at
the country level.
 Integration can optimize the efficient use of resources and reduce duplication
and wastage.
 Incentives are effective in changing and influencing behavior of providers and
users to improve health outcomes.
 Political commitment has been key to improved RMNCAH outcomes in all
countries that have made progress on MDGs 4 and 5.
Innovation and Research
The following research questions have been identified by MOH:
What are the factors that contribute to poor health seeking behaviors for
RMNCAH services?
What are the most cost-effective models that can promote male involvement?
What are the factors contributing to non-adherence to standard operating

procedures and guidelines by health care providers in both private and public
sectors?
what is the impact of comprehensive RMNCAH training on the competency and

skills of providers?
Does task sharing work; if not, what are key barriers?

What is the impact of current RMNCAH behavior change communication
interventions?
How effective are the different service delivery models, social media and mobile
technologies in delivering adolescent sexual and reproductive health?
What is the impact of maternal shelters?
What are the mechanisms to get real time feedback from adolescents on health
services (satisfaction with services)?
How effective is the ongoing innovations such as cash-plus program and what
are the implementation challenges?
What models work best to reach out of school adolescents?
Unit Two Content..
Topic 1: The Reproductive System
Female and Male Parts
•External
•Internal
•Accessory reproductive organs -breasts
Male:
•External
•Internal
Female Reproductive system

External Genitalia
EXTERNAL GENITALIA (SYN: VULVA, PUDENDUM)
 The vulva or pudendum includes all the visible external genital organs in the
perineum
 The vulva includes:
Ø mons veneris,
Ø labia majora,
Ø labia minora,
Ø clitoris,
Ø vestibule and
Ø conventionally the perineum.
 These are all visible on external examination.

 It is, therefore, bounded anteriorly by the mons veneris, and posteriorly by the
rectum, laterally by the genitocrural fold.
 The vulvar area is covered by keratinized stratified squamous epithelium.
MONS VENERIS (MONS PUBIS)
 It is the pad of subcutaneous adipose connective tissue lying in front of the pubis and
in the adult female is covered by hair.
 The hair pattern (escutcheon) of most women is triangular with the base directed
upwards.
LABIA MAJORA
 The vulva is bounded on each side by the elevation of skin and subcutaneous tissue
which form the labia majora.
 They are continuous where they join medially to form the posterior commissure in
front of the anus.
 The skin on the outer convex surface is pigmented and covered with hair follicle.
 The thin skin on the inner surface has sebaceous glands but no hair follicle.
 The labia majora are covered with squamous epithelium and contain sweat glands.
 The adipose tissue is richly supplied with venous plexus which may produce
hematoma, if injured during childbirth.
 The labia majora are homologous to the scrotum in the male. The round ligament
terminates at its upper border.
LABIA MINORA
 They are two thin folds of skin, devoid of fat, on either side just within the labia
majora.
 Except in the parous women, they are exposed only when the labia majora
are separated.
 Anteriorly, they divide to enclose the clitoris and unite with each other in front
and behind the clitoris to form the prepuce and frenulum respectively.
 The lower portion of the labia minora fuses across the midline to form a fold of
skin known as fourchette.
 It is usually lacerated during childbirth.
 Between the fourchette and the vaginal orifice is the fossa navicularis.
 The labia minora contain no hair follicles or sweat glands.
 The folds contain connective tissues, numerous sebaceous glands, erectile
muscle fibers and numerous vessels and nerve endings.
 The labia minora are homologous to the penile urethra and part of the skin
of penis in males.

CLITORIS
 · It is a small cylindrical erectile body, measuring about 1.5–2 cm

situated in the most anterior part of the vulva.
 · It consists of a glans, a body and two crura.
 · The clitoris consists of two cylindrical corpora cavernosa (erectile
tissue).
 · is richly supplied with nerves.
 · Clitoris is homologous to the penis in the male but it differs in being
entirely separate from the urethra.
 · It is attached to the under surface of the symphysis pubis by the
suspensory ligament.
VESTIBULE
 · The vestibule is the cleft between the labia minora.

 · It is a triangular space bounded anteriorly by the clitoris, posteriorly by
the fourchette and on either side by labia minora.
 · There are four openings into the vestibule.
 o Urethral opening
 o Vaginal orifice and hymen
 o Opening of Bartholin’s ducts
 o Skene’s glands
a. Urethral opening
 · The opening is situated in the midline just in front of the vaginal orifice
about 1–1.5 cm below the pubic arch.
 · The paraurethral ducts open either on the posterior wall of the urethral
orifice or directly into the vestibule.
b. Vaginal orifice and hymen
 ü The vaginal orifice lies in the posterior end of the vestibule and is of varying
size and shape.
 ü In virgins and nulliparae, the opening is closed by the labia minora, but in
parous, it may be exposed.
 ü It is incompletely closed by a septum of mucous membrane, called hymen.
 ü The membrane varies in shape but is usually circular or crescentic in
virgins.
 ü The hymen is usually ruptured at the consummation of marriage.
 ü During childbirth, the hymen is extremely lacerated and is later represented
by cicatrized nodules of varying size, called the carunculae myrtiformes.
 ü On both sides it is lined by stratified squamous epithelium.
c. Opening of Bartholin’s ducts:
 · There are two Bartholin glands (greater vestibular gland), one on each
side.
 · The vestibular bulbs are two oblong masses of erectile tissue that lie on
either side of the vaginal entrance.
 · They contain a rich plexus of veins within the bulbospongiosus muscle.
 · They are homologous to the bulb of the penis and corpus
spongiosum in the male.
 · Bartholin's glands, each about the size of a small pea, lie at the base of
each bulb and open via a 2 cm duct into the vestibule between the hymen and
the labia minora – outside the hymen at the junction of the anterior two-third
and posterior one-third in the groove between the hymen and the labium
minus.
 · They are pea-sized and yellowish white in color.
 · During sexual excitement, it secretes abundant alkaline mucus which
helps in lubrication
 · Bartholin’s glands are homologous to the bulb of the penis in male.
d. Skene’s glands
 · are the largest paraurethral glands.

 · Skene’s glands are homologous to the prostate in the male.
 · The two Skene’s ducts may open in the vestibule on either side of the
external urethral meatus.
hymen
 · is a thin fold of mucous membrane across the entrance to the vagina.
 · There are usually openings in it to allow menses to escape.
 · The hymen is partially ruptured during first coitus and is further
disrupted during childbirth.
 · Any tags remaining after rupture are known as carunculae myrtiformes.

blood supply to VULVA
Arteries—
 Branches of internal pudendal artery—the chief being labial,

transverse perineal, artery to the vestibular bulb and deep and dorsal
arteries to the clitoris.
 Branches of femoral artery—superficial and deep external pudendal.
Veins—
 The veins form plexuses and drain into:

 Internal pudendal vein,
 vesical or vaginal venous plexus and
 · Long saphenous vein. Varicosities during pregnancy are not
uncommon and may rupture spontaneously causing visible bleeding or
hematoma formation.
NERVE SUPPLY
 · The supply is through bilateral spinal somatic nerves—

 o anterosuperior part is supplied by the cutaneous
branches from the ilioinguinal and genital branch of
genitofemoral nerve (L1 and L2) and the
 o posteroinferior part by the pudendal branches from the
posterior cutaneous nerve of thigh (S1.2.3).
 o Between these two groups, the vulva is supplied by
the labial and perineal branches of the pudendal nerve
(S2.3.4).
LYMPHATICS
 · Vulval lymphatics have bilateral drainage. Lymphatics drain into—

 Ø Superficial inguinal nodes,
 Ø intermediate groups of inguinal lymph nodes—gland
of Cloquet and
 Ø External and internal iliac lymph nodes.
Embryology of VULVA
 · External genitalia is developed in the region of the cranial aspect of

ectodermal cloacal fossa;
 · clitoris from the genital tubercle;
 · labia minora from the genital folds;
 · labia majora from the labioscrotal swelling and
 · the vestibule from the urogenital sinus.
Age changes
 · In infancy the vulva is devoid of hair and there is considerable adipose
tissue in the labia majora and pubis that is lost during childhood but reappears
during puberty, at which time hair grows.
 · After menopause the skin atrophies and becomes thinner.
 · The labia minora shrink, subcutaneous fat is lost and the vaginal orifice
becomes smaller.
INTERNAL GENITAL ORGANS
 · The internal genital organs in female include:

 Ø vagina,
 Ø uterus,
 Ø fallopian tubes and
 Ø the ovaries.
 · These organs are placed internally and require special instruments for
inspection.
VAGINA
 The vagina is a fibromuscular canal lined with stratified squamous epithelium that
leads from the uterus to the vulva.
 It constitutes the excretory channel for the uterine secretion and menstrual blood.
 It is the organ of copulation and forms the birth canal of parturition.
 The diameter of the canal is about 2.5 cm, being widest in the upper part and
narrowest at its introitus.
 It has got enough power of distensibility.
 The canal is directed upwards and backwards forming an angle of 45° with the
horizontal in erect posture.
 The long axis of the vagina almost lies parallel to the plane of the pelvic inlet and at
right angles to that of the uterus.
VAGINAL WALL
 · Vagina has got an anterior, a posterior and two lateral walls.
 · The anterior and posterior walls are opposed together but the lateral walls are
comparatively stiffer especially at its middle, as such, it looks “H” shaped on
transverse section.
 · The length of the anterior wall is about 7 cm and that of the posterior wall is
about 9 cm.
 · The vaginal walls are normally in apposition, except at the vault, where they
are separated by the cervix.
 · The vault of the vagina is divided into four fornices: posterior, anterior and two
lateral
FORNICES
 · The fornices are the clefts formed at the top of vagina (vault) due to the
projection of the uterine cervix through the anterior vaginal wall where it is blended
inseparably with its wall.
 · There are four fornices—
 o one anterior,
 o one posterior and
 o two lateral;
 · The posterior one being deeper and the anterior, most shallow one.
VAGINA
 · The vaginal walls are rugose, with transverse folds.

 · The vagina is kept moist by secretions from the uterine and cervical glands
and by some transudation from its epithelial lining.
 · It has no glands.
 · The epithelium is thick and rich in glycogen, which increases in the
postovulatory phase of the cycle.
 · However, before puberty and after the menopause, the vagina is devoid of
glycogen because of oestrogen deficiency.
 · Doderlein's bacillus is a normal commensal of the vagina that breaks down the
glycogen to form lactic acid, producing a pH of around 4.5.
 · This has a protective role for the vagina in decreasing the growth of
pathogenic organisms.
VAGINAL RELATIONS
Anterior—
 The upper one-third is related with base of the bladder and the lower two-thirds are
with the urethra, the lower half of which is firmly embedded with its wall.
Posterior—
 The upper one-third is related with the pouch of Douglas,
 the middle-third with the anterior rectal wall separated by rectovaginal septum and
 the lower-third is separated from the anal canal by the perineal body
Lateral walls—
 The upper one-third is related with the pelvic cellular tissue at the base of
broad ligament in which the ureter and the uterine artery lie approximately 2 cm from
the lateral fornices.
 The middle third is blended with the levator ani and
 the lower-third is related with the bulbocavernosus muscles, vestibular bulbs and
Bartholin’s glands
STRUCTURE OF VAGINA:
 · Layers from within outwards are—

 · mucous coat which is lined by stratified squamous epithelium without
any secreting glands
 · submucous layer of loose areolar vascular tissues
 · muscular layer consisting of indistinct inner circular and outer
longitudinal muscles and
 · Fibrous coat derived from the endopelvic fascia and is highly
vascular.

VAGINAL SECRETION
 · The vaginal pH, from puberty to menopause, is acidic because of the presence
of Döderlein’s bacilli which produce lactic acid from the glycogen present in the
exfoliated cells.
 · The pH varies with the estrogenic activity and ranges between 4 and 5.
BLOOD SUPPLY TO VAGINA
 · The arteries involved are—

 Cervicovaginal branch of the uterine artery,
 Vaginal artery—a branch of anterior division of internal
iliac or in common origin with the uterine,
 Middle rectal and
 internal pudendal. These anastomose with one another
and form two azygos arteries— anterior and posterior.
 · Veins drain into internal iliac veins and internal pudendal veins.

LYMPHATICS TO VAGINA:
 · On each side, the lymphatics drain into—

 o Upper one-third—internal iliac group,
 o middle one-third up to hymen—internal iliac group,
 o below the hymen—superficial inguinal group.
NERVE SUPPLY TO VAGINA:
 · The vagina is supplied by sympathetic and parasympathetic from the pelvic

plexus.
 · The lower part is supplied by the pudendal nerve.
DEVELOPMENT
 · The vagina is developed from the following sources:

 · Upper 4/5th, above the hymen—the mucous membrane is derived
from endoderm of the canalized sinovaginal bulbs. The musculature is developed
from the mesoderm of two fused Müllerian ducts.
 · Lower 1/5th, below the hymen is developed from the endoderm of the
urogenital sinus.
 · External vaginal orifice is formed from the genital fold ectoderm after
rupture of the urogenital membrane.
Age changes
 · At birth, the vagina is under the influence of maternal oestrogens, so the
epithelium is well developed.
 · After a couple of weeks, the effects of the oestrogens disappear and the pH
rises to 7 and the epithelium atrophies.
 · At puberty the reverse occurs, and finally, at the menopause, the vagina tends
to shrink and the epithelium atrophies.
THE UTERUS
THE UTERUS
 The uterus is a hollow pyriform muscular organ situated in the pelvis between the
bladder in front and the rectum behind.
 The uterus is shaped like an inverted pear, tapering inferiorly to the cervix, and in the
non-pregnant state is situated entirely within the pelvis.
 It is hollow and has thick muscular walls. Its maximum external dimensions are
approximately 7.5cm long, 5cm wide and 3cm thick
 An adult uterus weighs about 70 g.
POSITION OF UTERUS
 · The longitudinal axis of the uterus is, approximately, at right-angles to the

vagina and normally tilts forwards.
 · This is termed anteversion.
 · The uterus is usually also flexed forwards on itself at the isthmus - anteflexion.
 · Its normal position is one of the anteversion and anteflexion.
 · In around 20 per cent of women, this tilt is not forwards but backwards -
retroversion and retroflexion.
 · This does not have a pathological significance.
 · The uterus usually inclines to the right (dextrorotation) so that the cervix is
directed to the left (levorotation) and comes in close relation with the left ureter.

MEASUREMENTS AND PARTS:
 · The uterus measures about 8 cm long, 5 cm wide at the fundus and its walls
are about 1.25 cm thick.
 · Its weight varies from 50 gm to 80 gm.
 · It has got the following parts:
 o Body or corpus
 o Isthmus
 o Cervix
Body or corpus of the uterus
 · The body is further divided into:

 o fundus—the part which lies above the openings of
the uterine tubes.
 o The body proper is triangular and lies between the
openings of the tubes and the isthmus.
 · The superolateral angles of the body of the uterus project outwards from the
junction of the fundus and body and is called the cornua of the uterus.
 · The uterine tube, round ligament and ligament of the ovary are attached to it.
 · The area of insertion of each Fallopian tube is termed the cornu and the part of
the body above the cornu, the fundus
Isthmus of the uterus
 · is a constricted part measuring about 0.5 cm, situated between the body and
the cervix.
 · It is limited above by the anatomical internal os and below by the
histological internal os (Aschoff).
 · Some consider isthmus as a part of the lower portion of the body of the uterus
cervix
 · Cervix is cylindrical in shape and measures about 2.5cm.

 · It extends from the isthmus and ends at the external os which opens into the
vagina after perforating its anterior wall.
 · The part lying above the vagina is called supravaginal and that which lies
within the vagina is called the vaginal part
CAVITY:
 · The cavity of the uterine body is triangular on coronal section with the base
above and the apex below.
 · It measures about 3.5 cm.
 · There is no cavity in the fundus.
 · The cervical canal is fusiform and measures about 2.5 cm.
 · Thus, the normal length of the uterine cavity is usually 6.5–7 cm.

RELATIONS OF THE UTERUS
Anteriorly—
 · Above the internal os, the body forms the posterior wall of the
uterovesical pouch.
 · Below the internal os, it is separated from the base of the bladder by loose
areolar tissue.
Posteriorly—
 · It is covered with peritoneum and forms the anterior wall of the pouch of
Douglas containing coils of intestine.
Laterally—
 · The double fold of peritoneum of the broad ligament are attached between
which the uterine artery ascends up.
STRUCTURES - BODY
The wall consists of three layers from outside inwards:
 ü Parametrium: It is the serous coat which invests the entire organ except on the
lateral borders. The peritoneum is intimately adherent to the underlying muscles.
 ü Myometrium: It consists of thick bundles of smooth muscle fibers held by
connective tissues and are arranged in various directions. During pregnancy,
however, three distinct layers can be identified—outer longitudinal, middle interlacing
and the inner circular.
 ü Endometrium: The mucous lining of the cavity. As there is no submucous layer,
the endometrium is directly opposed to the muscle coat. It consists of:
 o lamina propria and
 o surface epithelium.
 The surface epithelium is a single layer of ciliated columnar epithelium.
 The lamina propria contains stromal cells, endometrial glands, vessels and nerves.
The glands penetrate the stroma and sometimes even enter the muscle coat.
 The endometrium is changed to decidua during pregnancy.
STRUCTURE-CERVIX
 · The cervix is composed mainly of fibrous connective tissues.

 · The smooth muscle fibers average 10–15%.
 · Only the posterior surface has got peritoneal coat.
 · Mucous coat lining the endocervix is simple non-ciliated columnar.
 · The vaginal part of the cervix is lined by stratified squamous epithelium.
 · The squamocolumnar junction is situated at the external os.
Uterine secretion
 · The endometrial secretion is scanty and watery.

 · Secretion of the cervical glands is alkaline and thick, rich in mucoprotein,
fructose and sodium chloride.
BLOOD SUPPLY
· Arterial supply —
 o uterine arteries one on each side (anterior division of the internal iliac or in
common with superior vesical artery.)
 o ovarian and vaginal arteries with which the uterine arteries anastomose.
 · The cervix is insensitive to touch, heat and also when it is grasped by
any instrument. The uterus, too, is insensitive to handling and even to incision
over its wall.
A) Showing pattern of basal and spiral arteries in the endometrium;
(B) Internal blood supply of uterus
Age changes
 · The disappearance of maternal oestrogens after birth causes the uterus to

decrease in length by around one-third and in weight by about one-half.
 · The cervix is then twice the length of the uterus.
 · At puberty, however, the corpus grows much faster and the size ratio reverses.
 · After the menopause, the uterus atrophies, the mucosa becomes very thin, the
glands almost disappear and the wall becomes relatively less muscular.
 · These changes affect the cervix more than the corpus; cervical loops
disappear and the external os becomes more or less flush with the vault.
FALLOPIAN TUBE (Synonyms: Uterine tube, oviduct)
 · The uterine tubes are paired structures, measuring about 10 cm and

are situated in the medial three-fourth of the upper free margin of the broad
ligament.
 · Each tube has got two openings:
 o one communicating with the lateral angle of the uterine cavity
called uterine opening and measures 1 mm in diameter,
 o the other is on the lateral end of the tube, called pelvic
opening or abdominal ostium and measures about 2 mm in
diameter.
Parts of oviduct
· From medial to lateral are—
 intramural or interstitial lying in the uterine wall and measures 1.25 cm

in length and 1 mm in diameter,
 isthmus—almost straight and measures about 3–4 cm in length and 2
mm in diameter,
 ampulla—tortuous part and measures about 5 cm in length which ends
in,
 wide infundibulum measuring about 1.25 cm long with a maximum
diameter of 6 mm.
 o The abdominal ostium is surrounded by a number of
radiating fimbriae (20–25), one of these is longer than the rest
and is attached to the outer pole of the ovary called ovarian
fimbria
The important functions of the tubes
· Transport of the gametes,
· To facilitate fertilization and survival of zygote through its secretion.
Blood Supply
· Arterial supply is from the uterine and ovarian.
· Venous drainage is through the pampiniform plexus into the ovarian veins.
THE OVARY
 · The ovaries are paired sex glands or gonads in female which are

concerned for:
 • germ cell maturation, storage and its
release and
 • steroidogenesis.
 •Each gland is oval in shape and pinkish gray in color and the surface is
scarred during reproductive period.
 •It measures about 3 cm in length, 2 cm in breadth and 1 cm in thickness.
 •Each ovary presents:
 •two ends—tubal and uterine,
 •two borders—mesovarium and free posterior and
 •two surfaces—medial and lateral.
 · The ovary is the only intra-abdominal structure not to be covered by
peritoneum
 · it lies in the ovarian fossa on the lateral pelvic wall.
 · it is attached to the posterior layer of the broad ligament by the
mesovarium, to the lateral pelvic wall by the infundibulopelvic ligament and to
the uterus by the ovarian ligament.

RELATIONS
· Mesovarium or anterior border
o o A fold of peritoneum from the posterior leaf of the broad ligament is

attached to the anterior border through which the ovarian vessels and
nerves enter the hilum of the gland.
· Posterior border
o is free and is related to the tubal ampulla. It is separated by the peritoneum
from the ureter and the internal iliac artery.
· Medial surface
o o is related to fimbrial part of the tube.
· Lateral surface
o o is in contact with the ovarian fossa on the lateral pelvic wall.
STRUCTURES:
•The ovary is covered by a single layer of cubical cell known as germinal epithelium.
•The substance of the gland consists of:
o a. outer cortex and

o b. inner medulla.
Cortex of the ovary
 · It consists of stromal cells which are thickened beneath the germinal
epithelium to form tunica albuginea.
 · During reproductive period the cortex is studded with numerous
follicular structures, called the functional units of the ovary, in various
phases of their development which include:
o primordial follicles,
o maturing follicles,
o Graafian follicles and
o corpus luteum.
· Atresia of the structures results in formation of atretic follicles or corpus
albicans.
· These are related to sex hormone production and ovulation
Medulla of the ovary
· It consists of loose connective tissues, few unstriped muscles, blood vessels
and nerves.
· There is a small collection of cells called “hilus cells” which are

homologous to the interstitial cells of the testes.
Blood supply
· Arterial supply – ovarian artery, a branch of the abdominal aorta.
· Venous drainage – pampiniform plexus.
· NERVE SUPPLY: Sympathetic supply comes down along the ovarian artery
from T10 segment. Ovaries are sensitive to manual squeezing.
DEVELOPMENT:
· The ovary is developed from the cortex of the undifferentiated genital ridges
by about 9th week; the primary germ cells reaching the site migrating from the dorsal
end of yolk sac.
PELVIC FLOOR (Synonym: Pelvic diaphragm)
· Pelvic floor is a muscular partition which separates the pelvic cavity

from the anatomical perineum.
· It consists of three sets of muscles on either side—
o pubococcygeus,
o iliococcygeus and
o Ischiococcygeus
 · these are collectively called levator ani.

 · Its upper surface is concave and slopes downwards, backwards and medially
and is covered by parietal layer of pelvic fascia.
 · The inferior surface is convex and is covered by anal fascia.
 · The muscle with the covering fascia is called the pelvic diaphragm.
Levator ani muscles viewed from above
Levator ani muscle
· ORIGIN:
o Each levator ani arises from the back of the pubic rami, from the condensed
fascia covering the obturator internus (white line) and from the inner surface of the
ischial spine.
· INSERTION:
o From this extensive origin, the fibers pass, backwards and medially to be
inserted in the midline from before backwards to the vagina (lateral and posterior
walls), perineal body and anococcygeal raphe, lateral borders of the coccyx and
lower part of the sacrum
GAPS ON PELVIC FLOOR
· There are two gaps in the midline—
 The anterior one is called hiatus urogenitalis which is bridged by the

muscles and fascia of urogenital triangle and pierced by the urethra
and vagina.
 The posterior one is called hiatus rectalis, transmitting the rectum.
STRUCTURES IN RELATION TO PELVIC FLOOR
The superior surface is related with the following:
 Pelvic organs from anterior to posterior are bladder, vagina, uterus and rectum.
 Pelvic cellular tissues between the pelvic peritoneum and upper surface of the levator
ani which fill all the available spaces.
 Ureter lies on the floor in relation to the lateral vaginal fornix. The uterine artery lies
above and the vaginal artery lies below it.
 Pelvic nerves.
 The inferior surface is related to the anatomical perineum.
FUNCTIONS OF THE PELVIC FLOOR
 To support the pelvic organs—The pubovaginalis which forms a “U” shaped sling,
supports the vagina which in turn supports the other pelvic organs— bladder and
uterus. Weakness or tear of this sling during parturition is responsible for prolapse of
the organs concerned.
 To maintain intra-abdominal pressure by reflexly responding to its changes.
 Facilitates anterior internal rotation of the presenting part when it presses on the
pelvic floor.
 Puborectalis plays an ancillary role to the action of the external anal sphincter.
 Ischiococcygeus helps to stabilize the sacroiliac and sacrococcygeal joints.
 To steady the perineal body.
PELVIC FLOOR DURING PREGNANCY AND PARTURITION

· During pregnancy
 levator muscles undergo hypertrophy, become less rigid and more distensible. Due
to water retention, it swells up and sags down.
· In the second stage,
 the pubovaginalis and puborectalis relax and the levator ani is drawn up over the
advancing presenting part in the second stage.
 Failure of the levator ani to relax at the crucial moment may lead to extensive
damage of the pelvic structures
PERINEUM
ANATOMICAL PERINEUM
· It is bounded above by:
o inferior surface of the pelvic floor,

o below by the skin between the buttocks and thighs.
o Laterally by the ischiopubic ramus, ischial tuberosities and sacrotuberous ligaments and
o posteriorly, by the coccyx.
· The diamond shaped space of the bony pelvic outlet is divided into two
triangular spaces with the common base formed by the free border of the urogenital
diaphragm.
o The anterior triangle is called the urogenital triangle which fills up the gap of the
hiatus urogenitalis and is important from the obstetric point of view.
o o The posterior one is called the anal triangle
Urogenital Triangle
 · It is pierced by the terminal part of the vagina and the urethra.
 · Has superficial and deep perineal pouch compartments.
 · The superficial pouch is formed by the deep layer of the superficial perineal
fascia (Colles fascia) and inferior layer of the urogenital diaphragm (perineal
membrane
 · The deep perineal pouch is formed by the inferior and superior layer of the
urogenital diaphragm—together called urogenital diaphragm or triangular ligament
Anal Triangle
 · The triangle has got no obstetric importance.

 · It contains the terminal part of the anal canal with sphincter ani externus,
anococcygeal body, ischiorectal fossa, blood vessels, nerves, and lymphatics.
OBSTETRICAL PERINEUM:(Synonyms: Perineal body, central point of the

perineum)
 · The pyramidal shaped tissue where the pelvic floor and the perineal muscles
and fascia meet in between the vagina and the anal canal is called the obstetrical
perineum.
 · It measures about 4 cm × 4 cm with the base covered by the perineal skin
and the apex is pointed and is continuous with the rectovaginal septum.

Importance of obstetric perineum
• It helps to support the levator ani which is placed above it.
• By supporting the posterior vaginal wall, it indirectly supports the anterior

vaginal wall, bladder and the uterus.
• It is vulnerable to injury during childbirth.
• Deliberate cutting of the structures during delivery is called episiotomy.
PELVIC CELLULAR TISSUE
• It lies between the pelvic peritoneum and the pelvic floor and fills up all the
available empty spaces.
• It contains fatty and connective tissues and unstriated muscle fibers.
• Its distribution around the vaginal vault, supravaginal part of the cervix and into
the layers of the broad ligament is called parametrium.
Importance of the pelvic cellular tissue
• To support the pelvic organs.

• To form protective sheath for the blood vessels and the terminal part of the
ureter.
• infection spreads along the track, so formed, outside the pelvis to the
perinephric region along the ureter, to the buttock along the gluteal vessels, to the
thigh along the external iliac vessels and to the groin along the round ligament.
• Marked hypertrophy occurs during pregnancy to widen up the spaces.
POUCH OF DOUGLAS
• This is a narrow peritoneal cul-de-sac in the pelvis situated in the rectouterine

space.
• It is continuous with the pararectal fossa of either side.
Contents of Pouch of Douglas:
o It may remain empty but may contain coils of intestine or omentum.
Relations of POUCH OF DOUGLAS
• Anteriorly,
o it is bounded by the peritoneal covering of the cervix, posterior vaginal fornix
and upper-third of the posterior vaginal wall.
• Posteriorly,
o it is bounded by the peritoneal covering on the anterior surface of the rectum.
• Laterally,
o it is limited by the uterosacral folds of peritoneum covering the uterosacral

ligaments.
• The floor
o is formed by the reflection of the anterior peritoneum onto the anterior surface
of the rectum. It is about 6–7 cm above the anal orifice. Below the floor, there is a
thin fibrous tissue septum (rectovaginal).

Surgical Importance of Pouch of Douglas
• As it is the most dependent part of the peritoneal cavity, intraperitoneal blood or
pus usually settles down to the pouch to produce either pelvic hematocele or pelvic
abscess.
• Herniation of the pouch through the posterior fornix may occur producing the
clinical entity of enterocele.
• Vaginal ligation is done through opening the pouch.
• Culdoscopy, culdocentesis or at time pneumoperitoneum may be done through

the pouch.
• Nodules deposited in the pouch can help in the clinical diagnosis of pelvic
malignancy, endometriosis or genital tuberculosis.
Uterine Support
BROAD LIGAMENT
• The double fold of peritoneum which extends from the lateral border of the
uterus to the lateral pelvic wall of pelvis is called broad ligament.
• These, truly are not ligaments
BROAD LIGAMENT
• consists of two layers, anterior and posterior.
• The layers are continuous at its upper free border embracing the Fallopian tube.
• The lower part of the broad ligament is wider from before backwards and the
layers are reflected above the pelvic diaphragm.
PARTS OF BROAD LIGAMENT
1. Infundibulopelvic Ligament (Syn: Suspensory ligament of the ovary):
• It includes the portion of the broad ligament which extends from the
infundibulum to the lateral pelvic wall.
• It contains ovarian vessels and nerves and lymphatics from the ovary, Fallopian
tube and body of the uterus.
2. Mesovarium:
• The ovary is attached to the posterior layer of the broad ligament by a fold of

peritoneum called mesovarium (ovarian mesentery).
• Through this fold, ovarian vessels, nerves and lymphatics enter and leave the
hilum.
• The ovary is not enclosed within the broad ligament
3. Mesosalpinx:
• The part of the broad ligament between the fallopian tube and the level of
attachment of the ovary is the mesosalpinx.
• It contains utero-ovarian anastomotic vessels and vestigial remnants.
4. Mesometrium:
o The part of the broad ligament below the mesosalpinx is called mesometrium.
o It is the longest portion which is related with the lateral border of the uterus.
contents of the broad ligament
Fallopian tube.
Uterine and ovarian arteries with their branches, including the anastomotic branches
between them and corresponding veins.
Nerves and lymphatics from the uterus, Fallopian tube and ovary.
Proximal part of the round ligament which raises a peritoneal fold on the anterior
leaf.
Ovarian ligament which raises a peritoneal fold on the posterior leaf.
Parametrium containing loose areolar tissue and fat. The terminal part of the ureter,
uterine artery, paracervical nerve and lymphatic plexus are lying at the base of the
broad ligament.
Vestigial structures, such as duct of Gartner, epoophoron, and paroophoron.

MACKENRODT’S LIGAMENTS (SYN: CARDINAL LIGAMENT, TRANSVERSE
CERVICAL)
• Origin:
o Condensation of parietal fascia covering the obturator internus.
• Insertion:
o Lateral supravaginal cervix and upper part of lateral vaginal wall in a fan-

shaped manner. This insertion is continuous with the endopelvic and paricervical
fascial ring
Function:
• Lateral stabilization to the cervix at the level of ischial spine.
o Primary vascular conduits of the uterus and vagina
UTEROSACRAL LIGAMENTS
• Origin:
o Periosteum of sacral vertebra 2, 3 and 4.
• Insertion:
o Posterolateral surface of the cervix at the level of internal os
• Content:
o Uterosacral plexus of autonomic nerves. Smooth muscle and minimal vessels.
• Function:
o These are the primary proximal suspensory ligaments of the uterovaginal

complex.
o They hold the cervix posteriorly at the level of the ischial spines.
o Uterus is thus maintained anteflexed and the vagina is suspended over the
levator plate.

ROUND LIGAMENTS
 Each measures about 10–12 cm.

 It is attached at the cornu of the uterus below and in front of the fallopian tube.
 It courses beneath the anterior leaf of the broad ligament to reach the internal
abdominal ring.
 After traversing through the inguinal canal, it fuses with the subcutaneous tissue of
the anterior third of the labium majus.
 It contains plain muscles and connective tissue.
OVARIAN LIGAMENTS
 These are paired, one on each side.

 Each one is a fibromuscular cord-like structure which attaches to the inner pole of the
ovary and to the cornu of the uterus posteriorly below the level of the attachment of
the fallopian tube
 Morphologically, it is continuous with the round ligament.
Urinary System and breast
FEMALE URETHRA
• The female urethra extends from the neck of the bladder to the external urethral
meatus which opens into the vestibule about 2.5 cm below the clitoris.
• It measures about 4 cm and has a diameter of 6 mm.
• Its upper half is separated from the anterior vaginal wall by loose areolar tissue
and the lower half is firmly embedded in its wall.
• Numerous tubular glands called paraurethral glands open into the lumen
through ducts eg Skene’s ducts which open either on the posterior wall or into the
vestibule.
• These glands are the sites for harboring infection and occasional development
of benign adenoma or malignant changes.
THE URINARY BLADDER
• The bladder is a hollow muscular organ with considerable power of distension.
• Its capacity is about 450mL but can retain as much as 3–4 liters of urine.
• When distended it is ovoid in shape. It has got:
 o an apex
 o superior surface
 o Base
 o two inferolateral surfaces and
 o neck, which is continuous with the urethra.
• The base and the neck remain fixed even when the bladder is distended.
THE BREAST
• The breasts are large, modified sebaceous glands.
• The breasts are bilateral and in female constitute accessory reproductive organs
as the glands are concerned with lactation following childbirth.
• The shape of the breast varies in women and also in different periods of life.
• But the size of the base of the breast is fairly constant.
• It usually extends from the second to sixth rib in the midclavicular line.
• It lies in the subcutaneous tissue over the fascia covering the pectoralis major or
even beyond that to lie over the serratus anterior and external oblique.
• A lateral projection of the breast towards the axilla is known as axillary tail of
Spence.
• It lies in the axillary fossa, sometimes deep to the deep fascia.
• The breast weighs 200–300 gm during the childbearing age.
NB
G-spot
• The G-spot, also called the Gräfenberg spot (for German gynecologist Ernst

Gräfenberg, is characterized as an erogenous area of the vagina that, when
stimulated, may lead to strong sexual arousal, powerful orgasms and potential
female ejaculation.
• It is typically reported to be located 5–8 cm up the front (anterior) vaginal wall
between the vaginal opening and the urethra and is a sensitive area that may be part
of the female prostate.
• The existence of the G-spot has not been proven, nor has the source of female
ejaculation.
• Although the G-spot has been studied since the 1940s, disagreement persists
over its existence as a distinct structure, definition and location.
• A 2009 British study concluded that its existence is unproven and subjective,
based on questionnaires and personal experience.
• Other studies, using ultrasound, have found physiological evidence of the G-

spot in women who report having orgasms during vaginal intercourse
It is also hypothesized that the G-spot is an extension of the clitoris and that this is the cause
of orgasms experienced vaginally.
The Male reproductive system
• The reproductive system in men has components in the abdomen, pelvis, and
perineum
• The major components are a testis, epididymis, ductus deferens, and

ejaculatory duct on each side, and the urethra and penis in the midline.
• Three types of accessory glands are associated with the system:
o A single prostate;
o A pair of seminal vesicles;
o A pair of bulbourethral
o glands.
The scrotum
• The scrotum is an outpouching of the lower part of the anterior abdominal wall.
• It contains the testes, the epididymis’s, and the lower ends of the spermatic
cords.
• It is divided on its surface into two compartments by a raphé, which is continued
forward to the under surface of the penis, and
• backward, along the middle line of the perineum to the anus.
• Each compartment contains one of the two testes, and one of the epididymides.
• The wall of the scrotum has the following layers:
o Skin
o Superficial fascia
o Spermatic fasciae
o Tunica vaginalis
Skin
 • The skin of the scrotum is thin, wrinkled, and pigmented and forms a single
pouch. A slightly raised ridge in the midline indicates the line of fusion of the two
lateral labioscrotal swellings.
Superficial fascia
• This is continuous with the fatty and membranous layers of the anterior
abdominal wall.
• The fat is replaced by smooth muscle called the dartos muscle.
• This is innervated by sympathetic nerve fibers and is responsible for the

wrinkling of the overlying skin.
Spermatic fasciae
• It has three layers which lie beneath the superficial fascia and are derived from
the three layers of the anterior abdominal wall on each side.
• The external spermatic fascia is derived from the aponeurosis of the external

oblique muscle; the cremasteric fascia is derived from the internal oblique muscle;
and, finally, the internal spermatic fascia is derived from the fascia transversalis.
Tunica vaginalis
• This lies within the spermatic fasciae and covers the anterior, medial, and lateral
surfaces of each testis.
Lymph from the skin and fascia, including the tunica vaginalis, drains into the
superficial inguinal lymph nodes
Testes
 Testis has ellipsoid- shaped.

 Testes develop in the abdomen and move before birth into the scrotum.
 The left testis usually lies at a lower level than the right.
 The testis are covered by:
 A closed sac of peritoneum (the tunica vaginalis), which originally
connected to the abdominal cavity. Normally after testicular descent,
the connection closes, leaving a fibrous remnant.
 It is covered by a fibrous capsule called the tunica albuginea.
 In the inner surface of the capsule is a series of fibrous septa that divide the interior
of the organ into lobules.
 Lying within each lobule are 1 to 3 coiled seminiferous tubules.
 The tubules open into a network of channels called the rete testis.
 Small efferent ductules connect the rete testis to the upper end of the epididymis.
Epididymis
• The epididymis is a single, long coiled duct that courses along the

posterolateral side of the testis.
• The tunica vaginalis covers the epididymis with the exception of the posterior
border.
• Structurally, epididymis divided into:
o Head
o Body
o tail
Epididymis
It has two distinct components:
• The efferent ductules, which form an enlarged coiled mass that sits on the
posterior superior pole of the testis and forms the head of the epididymis;
• The true epididymis, which is a single, long coiled duct into which the efferent
ductules all drain, and which continues inferiorly along the posterolateral margin of
the testis as the body of epididymis and enlarges to form the tail of epididymis at the
inferior pole of the testis.
• The testicular artery is a branch of the abdominal aorta.
Venous drainage of the Testis and Epididymis
• The testicular veins emerge from the testis and the epididymis as a venous
network, the pampiniform plexus.
• This becomes reduced to a single vein as it ascends through the inguinal canal.
• The right testicular vein drains into the inferior vena cava, and the left vein joins
the left renal vein.
• Lymphatic drainage of the testes is to the para- aortic lymph nodes
Ductus deferens
• (Latin: "carrying-away vessel"), also called vas deferens.
• The ductus deferens is a long muscular duct that transports spermatozoa from
the tail of the epididymis to the ejaculatory duct
• The vas arises from the tail of the epididymis and traverses the inguinal canal
to the deep ring, passes downwards on the lateral wall of the pelvis almost to the
ischial tuberosity and turns medially to cross the ureter posterior to the bladder.
• It continues inferomedially along the base of the bladder, anterior to the rectum,
almost to the midline, where it is joined by the duct of the seminal vesicle to form the
ejaculatory duct.
• The terminal part of the vas deferens is dilated to form the ampulla of the vas
deferens.
• The ejaculatory duct penetrates through the prostate gland to connect with the

prostatic urethra.
Seminal vesicle
• The seminal vesicles are an accessory gland of the male reproductive system.
• The seminal vesicles are two lobulated organs about 2 in. (5 cm) long lying on
the posterior surface of the bladder
• On the medial side of each vesicle lies the terminal part of the vas deferens.
• Posteriorly, the seminal vesicles are related to the rectum.
• Inferiorly, each seminal vesicle narrows and joins the vas deferens of the same
side to form the ejaculatory duct.
• Arteries
o The arterial blood supply from, the inferior vesicle and middle rectal arteries
• Veins
o The veins drain into the internal iliac veins.
Ejaculatory Ducts
• The two ejaculatory ducts are each less than 1 in. (2.5 cm) long and are formed
by the union of the vas deferens and the duct of the seminal vesicle.
• The ejaculatory ducts pierce the posterior surface of the prostate and open into
the prostatic part of the urethra, close to the margins of the prostatic utricle; their
function is to drain the seminal fluid into the prostatic urethra.
Prostate
• The prostate is an unpaired accessory structure of the male reproductive system

that surrounds the urethra in the pelvic cavity.
• It lies immediately inferior to the bladder, above the urogenital diaphragm,
posterior to the pubic symphysis, and anterior to the rectum.
• The prostate is shaped like an inverted rounded cone with a larger base, which
is continuous above with the neck of the bladder, and a narrower apex, which rests
below on the pelvic floor.
• The inferolateral surfaces of the prostate are in contact with the levator ani
muscles that together cradle the prostate between them.
• The two ejaculatory ducts pierce the upper part of the posterior surface of the
prostate to open into the prostatic urethra at the lateral margins of the prostatic
utricle.
Relations of Prostate
• Superiorly
o The base of the prostate is continuous with the neck of the bladder.
o The urethra enters the center of the base of the prostate.
• Inferiorly
o The apex of the prostate lies on the upper surface of the urogenital diaphragm.
o The urethra leaves the prostate just above the apex on the anterior surface
• Anteriorly
o The prostate is related to the symphysis pubis.
o The prostate is connected to the posterior aspect of the pubic bones by the
puboprostatic ligaments.
• Laterally
o The prostate is embraced by the anterior fibers of the levator ani.
• Posteriorly
o The prostate is closely related to the anterior surface of the rectal ampulla and
is separated from it by the rectovesical septum (fascia of Denonvilliers).
Structure of the Prostate
• Enclosed within thin dense fibrous capsule
• Inner loose sheath derived from pelvic fascia – “prostatic sheath”
– Continuous inferiorly with superior fascia of urogenital diaphragm
– Posteriorly it is part of rectovesical septum
– Separates bladder, seminal vesicles and prostate from rectum
• Prostatic venous plexus lies between fibrous capsule and prostatic sheath.
Prostate divided into:

– Two lateral lobes
– One median lobe
– Anterior and posterior lobes
Structure of the Prostate
• Anterior
– Tissue lying anterior to urethra
– No glands; fibromuscular tissue only
• Median
– Cone-shaped region between ejaculatory ducts and urethra
• Lateral (left & right)
– Main mass of gland, continuous posteriorly
– Separated by prostatic urethra
• Posterior
– Describes postero-medial part of lateral lobes palpable through rectum on DRE.
Blood Supply of The Prostate
• Arterial supply
– Arteries derived from internal pudenal, inferior vesical and middle rectal arteries

(branches of internal iliac)
• Venous drainage
– Veins form prostatic venous plexus around sides and base of prostate – located
between capsule and sheath
– Drains into internal iliac veins
– Also communicates with vesical venous plexus and vertebral venous plexuses.

Lymphatics and innervation of The Prostate
o Lymphatic drainage
§ Lymph vessels terminate in internal iliac and sacral lymph nodes
§ Some vessels from posterior surface pass with lymph vessels from bladder to
external iliac LN’s
o Innervation
§ Parasympathetic fibres arise from pelvic splanchnic nerves
§ Sympathetic fibres from inferior hypogastric plexuses
Penis
• The penis is a pendulous organ suspended from the front and sides of the pubic
arch and containing the greater part of the urethra.
• It consists of internal root, external shaft, & glans.
• Root: the portion of the penis that extends internally into the pelvic cavity.
• Shaft: the length of the penis between the glans and the body.
• Glans: the head of the penis; has many nerve endings.
• Foreskin: a covering of skin over the penile glans.
• The root of penis consists of the two crura, which are proximal parts of the
corpora cavernosa attached to the pubic arch, and the bulb of penis, which is the
proximal part of the corpus spongiosum anchored to the perineal membrane.
• The body of the penis is essentially composed of three cylinders of erectile

tissue enclosed in a tubular sheath of fascia (Buck's fascia).
• The erectile tissue is made up of two dorsally placed corpora cavernosa and a
single corpus spongiosum applied to their ventral surface.
• At its distal extremity, the corpus spongiosum expands to form the glans
penis, which covers the distal ends of the corpora cavernosa.
• On the tip of the glans penis is the slit like orifice of the urethra, called the
external urethral meatus.
External penile structures

• Corona: the rim of the penile glans.
• Frenulum: thin strip of skin connecting the glans to the shaft on the underside of
the penis.
• Both are highly sensitive areas to the touch
Blood Supply of The Penis
Arteries
• The corpora cavernosa is supplied by the deep arteries of the penis; the corpus
spongiosum is supplied by the artery of the bulb.
• In addition, there is the dorsal artery of the penis.
• All the above arteries are branches of the internal pudendal artery.
Veins
• The veins drain into the internal pudendal veins.
Lymphatics and innervation of The Penis
Lymph Drainage
• The skin of the penis is drained into the medial group of superficial inguinal
nodes.
• The deep structures of the penis are drained into the internal iliac nodes
Nerve Supply
• Sensation
• The nerve supply is from the pudendal nerve and the pelvic plexuses.
• Erectile function
• Parasympathetic(excitatory)
Sympathetic (inhibitory)
Summary
Penis Nerve Supply
• Sensation
• The nerve supply is from the pudendal nerve and the pelvic plexuses.
• Erectile function
• Parasympathetic (excitatory)
o Sympathetic (inhibitory)
Unit Three Content..
Topic 1: Obstetrics History Taking
CONFIDENTIALITY:
During history taking, the medical student should at all times show the patient the res
pect that is due to her; while full confidentiality must be maintained at all times
bearing in mind that the
relationship between the professional and his client is based on mutual trust and res
pect.
Classical Hippocratic Oath state: “All that may come to my knowledge in the exer
cise of my profession or in daily commerce with men, which ought not to be spread
abroad, I will keep secret and will never reveal.”
Criminal Code of Malta [Ch.9:257]. The law reads as follows: “If any physician, surge
on, obstetrician or apothecary or, in general, any other person who, by reason of his
calling or profession, becomes the
depository of any secret confided to him, shall, except when compelled by law to giv
e information to the public authority, disclose such secret, he shall, on conviction be l
iable to a fine.”
Summary of code of ethics
• Informed consent; rapport
• Confidentiality; Privacy; Dignity: chaperon
• Woman’s views
• Informed consent for clinical evaluation and management
• Professional etiquette
• Ultimate primacy of the patient in making treatment decisions
HISTORY TAKING IN OBSTETRICS
1. Introduce yourself and obtain consent to take history:
Ø “Hello. I am Mr/Ms ****, a medical student. Do you mind if I ask you some questio
ns about your medical condition?”
2. PARTICULARS:
Ø Name, age, address, marital status, occupation, religion, sex.
Ø LMP, parity, gravity, EDD - Naegele’s rule
o Gravidity is no. of pregnancies including current pregnancy (regardless of the

outcome Normal or abortion)
o Parity is no. of births beyond 24 wk gestation
3. PRESENTING COMPLAINT:
Ø “What is the problem that brought you to the hospital/clinic?”
Ø Best to record this in the patient’s own words.
Ø “Were you referred by your doctor or did you self‐refer yourself to
the hospital/clinic?”
Ø Duration of the presenting complain.
4. HISTORY OF PRESENT ILLNESS (HPI)
Ø In the obstetric patient, its may be best to consider the “presenting complaint” in t
wo
parts:
a. The history of present illness or complaint; and
b. The history of the current pregnancy.
Patient may not furnish sufficient details, in which case it will be necessary to amplify
with specific
Directed questions. E.g. SOCRATES relating to pain: ‐
i. Site: where, local/diffuse
ii. Onset: rapid/gradual, pattern, worse/better since onset
iii. Character: sharp/dull/stabbing, burning/cramp/crushing

iv. Radiation: “Does the pain affect you anywhere else?” [to thigh/loin/elsewh
ere]
v. Alleviating factors: “What do you do to make yourself comfortable?”
“Is the pain better after menstruation?”

vi. Time course: “When did the pain start?”; if pain is chronic “What made you
seek attention now” “Is the pain worse at any particular time of the cycle?”

vii. Exacerbating factors: “Is there anything that brings on the pain or makes
it worse?”

viii. Severity & Impact on life: “On a scale of 1 to 10, at what level would you classif
y the pain?”
"Does it interrupt your life?"
5. SYSTEMIC ENQUIRY OF ASSOCIATED SYMPTOMS
v GIT system:
v Respiratory system
v Cardiovascular system
v Cardiovascular system
v Urinary system
v CNS
v Musculoskeletal system
6. OBSTETRIC HISTORY
A. HISTORY OF PRESENT PREGNANCY
a. Menstrual history
ü The date of the first day of the last menstrual period (or LMP).
ü The length of the menstrual cycle refers to the time interval between the first day of
the period and
the first day of the subsequent period. This may vary from 21 to 35 days in normal w
omen, but menstruation usually occurs every 28 days
b. The estimated date of delivery (EDD)
ü Can be calculated from the first day of the last menstrual period (LMP) by adding

9months and 7days to this date.
ü However, to apply this Naegele's rule, LMP should be accurate and

the woman should have had regular 28day menstrual cycles.
ü The average duration of human gestation is 269 days from the date of conception
ü Therefore, in a woman with a 28day cycle, this is 283 days from the first day of the
last menstrual
period (14 days are added for the period between menstruation and conception)
ü In a 28
day cycle, the estimated date of delivery can be calculated by subtracting 3 months f
rom the first day
of the LMP and adding on 7 days (or alternatively, adding 9 months and 7 days).
ü It is important to
appreciate that only 40% of women will deliver within 5days of the EDD and about
twothirds of women deliver within 10 days of EDD.
ü The calculation of EDD based on a woman's LMP is therefore,
at best, a guide to a woman as to the
date around which her delivery is likely to occur.
ü If a woman's normal menstrual cycle is less than 28 days or is greater than 28 day
s, then an
appropriate number of days should be subtracted from or added to the estimated dat
e of delivery.
ü For example, if the normal cycle is 35 days, 7 days should be added to the estimat
ed date of delivery
a. GRAVITY
üThe term ‘gravidity’ refers to the number of times a woman has been pregnant, irre
spective of the
outcome of the pregnancy, i.e. termination, miscarriage or ectopic pregnancy.
ü A primigravida is a woman who is pregnant for the first time and a multigravida is
a woman who has been pregnant on two or more occasions.
ü This term ‘gravidity’ must be distinguished from the term ‘parity’, which describes th
e number of liveborn children and stillbirths a woman has delivered after 24 weeks
or with a birth weight of 500g.
ü Thus, a primipara is a woman who has given birth to one infant after 24 weeks.
ü A multiparous woman is one who has given birth to two or more infants, whereas,
a nulliparous woman has not given birth after 24 weeks.
ü The term ‘grand multipara’ has been used to describe a
woman who has given birth to five or more infants
ü A parturient is a woman in labour and a puerpera is a woman who has given birth t
o a child during the preceding 42 days.
b. Gestation by dates
c. FOCUSED ANTENATAL CLINIC
üWhen started, number of visits so far

üantenatal profile
o haemoglobin
o blood groups & rhesus factor
o syphilis test – VDRL / RPR
o HIV test
o Urinalysis
o Optional : blood slide for MPS, Stool for ova & cyst
üMedication presently and previously
üRadiological examinations during pregnancy
d. Assess about Symptoms of pregnancy and their severity
ü Nausea and vomiting
o commonly occur within 2 weeks of missing the first period and it is believed
to be secondary to human chorionic gonadotrophin (hCG.
o it is described as morning sickness, vomiting may occur at any
time of the day and is often precipitated by the smell or sight of food.
o Morning sickness commonly occurs in the first 3 months but, in some women, it
may persist throughout pregnancy
o Severe and persistent vomiting leading to maternal dehydration, ketonuria and
electrolyte imbalance is termed hyperemesis gravidarum
ü Increased frequency of micturition
o due to the pressure on the bladder exerted by the gravid uterus.
o It tends to diminish after the first 12 weeks of pregnancy as the uterus rises above
the symphysis pubis, i.e. into the larger abdominal cavity.
ü Excessive lassitude or lethargy
o is a common symptom of early pregnancy and may become
apparent even before the first period is missed.
o Often, it disappears after 12 weeks of gestation.
ü Breast tenderness and heaviness,
o which are really an extension of those experienced by many
women in the premenstrual
phase of the cycle, are common during early pregnancy.
o It is due to the effect of increasing serum progesterone as well as an increased

retention of water.
ü First maternal perception of fetal movements , also called ‘quickening’
o is not usually noticed until 20 weeks gestation during first pregnancy
and 18 weeks in the second or subsequent pregnancies.
o However, many women may experience fetal movements earlier than 18 weeks a
nd others may progress beyond 20 weeks of gestation without being aware of fetal
movements at all.
ü Some women may experience an abnormal desire for a particular food and this is
termed pica
ü Pseudocyesis
o Development of symptoms and many of the signs of pregnancy in a woman
who is not pregnant.
o This is often due to an intense desire for or fears of pregnancy that may result in
hypothalamic amenorrhoea
ü Leg cramps
ü Limb swelling
e. Enquire about symptoms which could indicate complications of pregnancy
üPer vaginal discharge, bleeding
üLAPs
üHeadache
üVisual disturbance
üPain on micturation
f. PREVIOUS OBSTETRIC HISTORY(Previous deliveries/miscarriages)
üDetail each previous pregnancy - dates of deliveries, where birth took place,
delivered at what gestation, how long did labour take, mode of delivery, condition of
baby at birth, sex, birth weight, other complications at delivery and postpartum, any
blood transufusion, did she breast fed if not why, Length of labour & complications,
outcome, Previous miscarriages
I. GYNAECOLOGY HISTORY
üUse of family planning
past medical surgical history
personal social , economic history
family history
summary of the history
Gynaecological History Taking
1. Personal identification
2. Chief complain
3. History of presenting illness
4. Review of systems
5. Gynaecology history
ü LMP, parity, last date of delivery
ü Menstrual history
o Age of menarche (10-16yrs)
o Duration of flow
o Regularity and duration of cycle
o Amount of bleeding (number of pads used)
o History of dysmenorrheal
ü Irregular bleeding – intermenestrual, post coital – so amount, timing, colour, pain

associated
ü Per vaginal discharge=colour, timing, amount, smell

ü Per vaginal bleeding – colour. Amount, Smell, presence of clots
ü Fertility / infertility
o Use of family planning methods-duration & type
o Any problems on fertility
o Previous pregnancies & last date of delivery if applicable.
ü Sexual history
o Sexual partners and for how long
o Any problems – dyspareunia, electile dysfunction
o Frequency & timing of coitus (when applicable)
ü History of STIs
o Any previous STIs
o Treatment for STIs
o Use of protective measures
ü Past gynaecological problems and operations
6. Past medical surgical history
7. Personal social economic history
8. Family history
9. Summary of the history
10. Examination.
General Examination Techniques
Prerequisites when examining a patient
· Use your senses well – listen, look, touch, smell, when examining
· Knowledge of anatomical land marks
· Ensure adequate lighting in the room & Secondary tangential lighting from a
lamp
· Ensure the place is quiet to allow proper percussion and auscultation
· Ensure presence of necessary instruments
· Ensure privacy.
· Explain the procedure to the patient and ask permission to examine
· Be thorough without wasting time, systemic without being rigid, gentle yet not
afraid to cause discomfort
· Try to look calm, organized and competent even if you do not exactly feel that
way
· Avoid expressions of disgust, alarm, distaste, or other negative reaction
· Sequence the comprehensive examination in a manner designed to minimize

the patient’s need to change positions and maximize your efficiency. Variations are
possible and you may wish to develop a method of your own. In general it is helpful
to move from head to toe.
· Examine patient from the right side. Working from one side helps you master
skills more quickly and promotes efficiency. Left-handed students find it awkward but
are encouraged to practice it for convenience of themselves and others
GENERAL TECHNIQUES USED IN PHYSICAL EXAMINATION
1. Inspection:
· Definition: it’s the process of observing signs indicative of a healthy or a

pathological state of a certain body part or system within a patient
· Inspection should start as the patient enter consultation room (posture, gait,
appropriate clothing, colour and moisture of skin, unusual odours), during history
taking and during physical examination where you expose the areas of inspection as
you validate the inspection findings with your patient (“I see a black spot here, have
you noted it?)
2. Palpation
· Definition: it involves the use of your hands and fingers to gather information
through sense of touch.
· Certain parts of the hands are better than others for specific types of palpation
eg:
o Palmar surface & finger pads are most suitable to assess position, texture, size,
form, consistency and presence of fluid or crepitus of a mass or structure
o Ulnar surface of hands is suitable to assess vibration
o Dorsal surface of hands is suitable to assess temperature.
· Palpation may be light or deep controlled by amount of pressure applied. Light

palpation always precedes deep palpation.
· On the abdomen: always begin the palpation process with light systemic
palpation of four quadrants initially avoiding areas of tenderness or problem spot
· Light palpation is important in eliciting areas of muscle resistance and

tenderness.
· Deep palpation is normally only done in the abdomen
· Palpation can be made with one hand or by two hands on top of each other
with the upper one exerting the pressure (reinforced palpation)
· Bimanual palpation is a technique whereby an organ is palpated using both

hands.
· Preparation:
o Short nails
o Patient to lie supine to relax abdominal muscles
o Warm your hands to avoid producing muscle contractions
o Stand on right of the patient (if the patient is in a low bed – sit on or kneel besides
the patient’s right)
o Ensure patient is comfortable
o Ask patient to show areas of pain before you start palpation.
3. Percussion
· Definition: it involves striking one object against another, thus providing

vibration and subsequent sound waves.
· Your middle finger functions as the hammer and the vibration is produced by
the impact of the finger against the underlying tissue.
· Sound waves are heard as percussion tones (notes) that arise from vibrations
in the body tissue
· The degree of percussion tone is determined by the intensity of medium

through which the sound waves travel eg air, fluid or solid:
· Example
Tone Intensity Pitch Duration Quality Example

Tympanic Loud High Moderate Drum like Gastric bubble
Hyper- Very loud Low Long Boom like Emphysematous
resonant lung
Resonant Loud Low Long Hollow Health lung
Dull Soft to Moderate to Moderate Thud like Over liver
moderate high
Flat Soft High Short Very dull Over muscle

Percusion Technique
I. Your (dormant) middle finger acts as a hammer (plexor) and fingers on the
other hand (non-dorminant) acts as the striking surface (pleximeter) spread over
surface of the body. The middle finger should be slightly flexed, relaxed and posed
to strike. Plexor should be at right angles with pleximeter. Snap the wrist of the
tapping hand downwards, and with the tip of the plexor sharply tap the inter-
phalangeal joint or second phalanx of pleximeter
NB. The downward snap of the striking finger originates from the wrist and not
from movement in the forearm or shoulder. It should be quick, sharp but
relaxed wrist motion
Once your finger has struck, snap the wrist back quickly lifting the finger to prevent
dampening the sound.
Use the tip and not the pad of the flexor finger
You can percuss one location several times for ease interpretation of the tone
II. Alternative technique:
ü Strike your finger or hand directly against the body eg clavicle and skull
(hydrocephalus)
4. AUSCULTATION
· Definition: means listening for sounds produced by the body.

· It should be carried out last after the other techniques have provided
information that will assist in interpreting what you hear
· NB. Only abdomen you auscultate before palpation and percussion as the
latter two techniques sometimes influence the bowel sounds.
· Technique:
o Ensure a quiet environment
o Place bell or diaphragm of the stethoscope on naked skin as clothing obscures

sound
o Stabilize the stethoscope by holding the chest piece between the second and
third finger.
o When using the diaphragm press it firmly against the skin.
o Avoid touching the tubing with your hands or allowing it rub against any surface
as it creates extraneous noise.
o Listen to sound not only for its presence or absence but also for its characteristics
– intensity, pitch, duration and quality
o Closing your eyes may help you focus on the sound
o Target and isolate each sound, concentrating on one sound at a time.
General Examination and Vital Signs
General examination
· Observe the patients general state of health, height, built and sexual
development
· Note posture, motor activity, gait, dresss, grooming and personal hygiene –
any odours of the body and breath
· Watch patient’s facial expressions and notes manner and affect and reactions
to things in the environment
· Listen to manner of speaking and note state of awareness
CLINICAL PARAMETERS
1. PALLOR:
ü Sites in the body to examine pallor

v Conjunctiva
v Tongue
v Palms
v Nail bed: capillary refill
v Sole of foot
v Anus/ perineum
Conjunctiva: ask patient to be seated or lie supine, facing you. Place both
thumbs on the margins of the lower eyelids and gently pull the skin downwards to
evert lower lids (palpebral conjunctiva) and examine colour.
Tongue /lips: ask patient to open mouth and protrude the tongue. Observe
colour of the tongue. Pull and evert the upper and lower lips gently to observe colour
of inner parts.
Palms: ask the patient to supinate the two palms. Observe colour while you
compare with your own palms
Capillary refill test: blanch the nail bed with the thumb and sustain the
pressure for several seconds on fingernail or toenail. Release the pressure, observe
the time elapsed before the nail regains its full colour. Normally this should occur
almost instantly – in less than 2seconds.
Soles: with the patient lying supine or seated: look at the soles and observe
colour
Anus / perineum: patient in lithotomy position (supine, hips and knees flexed)
or lying on side, assess the perineum / anus for colour if applicable. Use gloves
2. JAUNDICE:
Ø Means having a yellowish discoloration.
Ø Can be observed at: sclera, mucous membranes and skin
Ø With patient seated or supine, gently elevate upper eyelids using both thumbs
with patient facing a light source, ask him/her to look downwards to expose sclera
and assess colour.
Ø Ask patient to open mouth assess colour of mucous membrane

Ø Examine skin and assess colour – light skinned people and infants.
Ø Look at palms and soles for yellowish discoloration
3. HYPOXAEMIA : CYANOSIS
· A bluish discolouration these sites
· TYPES:
o Central cyanosis – lips & frenulum and
o peripheral cyanosis – extremities at hands and feets
· examine palms, sole, lips and frenulum for colour
4. HYPOXAEMIA: FINGER CLUBBING
I. look at the shape of nails as compare with yours
a. Nail base angle should measure about 160 degrees.
b. Observe this by placing a ruler or a sheet paper across the nail and dorsal
surface of the finger and examine the angle formed by the proximal nail fold and nail
plate.
II. In clubbing the angle increases and approaches or exceeds 180
degrees
a. Ask the patient to place together the nail (dorsal) surfaces of the fingertips
from the right and left hands
b. When nails are clubbed, the diamond – shaped window at the base of the nails
disappears and the angle between the distal tips increases (shamroth technique)
III. Gently squeeze nail between your thumb and the pad of your finger to
test for adherence of the nail to the nail bed.
a. The nail bed should feel firm
b. A boggy nail base accompanies clubbing.
5. DEHYDRATION
· Sites: fontanels, eyes, mucous membranes, skin (abdomen or chest)
· Fontanels – below 18months – sunken in dehydration
· Eyes – sunken in dehydration. Absent tears in dehydration
· Mucous membranes – dry in dehydration
· Skin turgor – pinch skin over chest or abdomen using thumb and index
finger. Observe duration skin takes to go back.
6. OEDEMA
· Sites: face, sacrum, abdomen. Extremities.
· Face: observe peri-orbital oedema
· Sacrum: press sacral area with thumb for 30seconds
· Lower limbs: use both thumbs to apply pressure on the lower limbs 1cm
above medial malleolus for 30seconds as you look patient face.assess for pitting by
running you finger over the site
· Report oedema as – bi- or unilateral, tender or non-tender, pitting or non-

pitting.
7. LYMPH NODES.
ü Small, mobile and painless lymph nodes are often palpable in healthy individuals
ü A painful lymph node is suggestive for inflammatory process
ü A firm or fixed non-motile LN is very suggestive for a malignant process
Technique:
Inspect area of LN for apparent LN, oedema, erythema, red streaks and skin lesions
Using pads of 2rd 3rd & 4th fingers gently palpatefor superficial nodes
Note location, consistency, mobility, tenderness, size, shape, discreteness &

warmth. Move skin over area.
Head & neck LN: Palpate the anterior LN from behind the patient and vice varsa.
Sternocleidomastoid muscle divide into anterior & posterior
Axillary LN:
Other LN.
8. ORAL THRUSH
VITAL SIGNS
The word vital signs means essential to life.
They include:
· Pulse rate
· Respiratory rate
· Blood pressure
· Temperature
1. PULSE RATE
Radial pulse is mostly used to assess:
· Heart rate
· Cardiac cycles per minute
· Collapsing pulse
· Arrhythmias
· Condition of the blood vessels
· Assessing the blood pressure
Sites for taking pulse rate:
· Radial: on the thumb side of the wrist
· Temporal: lateral to eye brow on the temporal bone
· Brachial: medial aspect of cubital fossa
· Femoral: upper inner aspect of thigh
· Popliteal: behind the knee

· Dorsalis pedis: upper surface of the foot
· Carotid pulse: side of the neck
Characteristics of pulse
ü Rhythm:
o Regular
o Irregular
§ Regular irregular
§ Irregular irregular
ü Character:
o Feeble (small volume – eg dehydration)
o Pounding eg anxiety
o Collapsing
ü Pulse volume.

2. BLOOD PRESSURE
Requirements:
· Mercury sphygmomanometer
· Aneroid sphygmomanometer
· Electronic sphygmomanometer
· Stethoscope
False reading may occur in:
· Bp machine defect
· Dehydration
· Anxiety
· Exercise
· Individuals with small and large biceps
· Differences between supine and erect Bp especially in elderly.
Classification of hypertension
Pre-hypertension: Systolic BP 120-140 or diastolic BP 80-90.
Stage I hypertension: Systolic BP > 140-160 or diastolic BP >90-100.
Stage II: Systolic BP > 160 or diastolic BP > 100.
3. TEMPERATURE
Sites:
· Armpit (most used)
· Oral – adults & children who can follow instructions
· Groin – in children
· Rectal – for children and unconscious. Most accurate but uncomfortable.
Requirements:
· Thermometer:
o Mercury
o Electronic
o Inflated auxiliary thermometers
o Low reading thermometer
· A container containing cotton soaked in disinfectant. Change disinfectant

every 24hours
· A quick assessment of temperature can be done by use of back of the hand.
4. RESPIRATORY RATE
Note character and rhythm.

1. OBSTETRIC ABDOMINAL EXAMINATION
Regular abdominal examination is an important component of both antenatal care

and monitoring labour
By abdominal examination you can ascertain:
· The size of the uterus and note whether it corresponds to the period of
amenorrhea
· The size of the foetus
· The lie presentation and attitude of the foetus
· The relative sizes of the brim of the pelvis and the presenting part
· Whether the foetus is alive
· The presence of the abnormal condition eg excess liquor amnii, twin

pregnancy, abdominal tumours
Requirements
· Foetoscope
· Watch with second hand
· A bowl with dry gauze and cotton swabs
· Tape measure
· Receiver for the dirty swabs
· Couch
· Bed sheet
Examination
Explain the procedure to the patient
Ensure privacy
Wash and dry your hands to ensure they are warm

Expose the abdomen
Inspection
Inspect for shape, size, skin, linear nigra, striae gravidarum, scars, foetal
movements, umbilicus
Palpation
LEOPOLD’S MANEUVER
 First maneuver: Fundal Grip

 Second maneuver: Umbilical Grip
 Third maneuver: (1st pelvic grip) = The Pawlick's Grip,
 Fourth maneuver: (2nd Pelvic Grip) = pelvic grip
First Leopold’s maneuver: Fundal Grip

Facing the mother, palpate the fundus with both hands
– Assess for shape, size, consistency and mobility
Fetal head: firm, hard, and round
– Moves independently of the rest
– Detectable by ballottement
Breech/buttocks: softer and has bony prominences
– Moves with the rest of the form
Fundal height
· Using your left hand, place either the ulnar/radial border of the index finger on
the abdomen from xiphisternum
· Apply pressure as you move downwards in steps to locate the underlying

mass
· Once the mass is encountered maintain the hand or finger at that level
· Using the right hand, determine the number of fingerbreaths from the superior
border of the umbilicus up to the level of fundus
· Each finger breath multiplied by 2. Fundal height at umbilicus is 22/40, at

sympysis pubis is 12/40
· Alternatively you can use tape measure to check fundal height from symphysis
pubis through umbilicus to xiphoid sternum. Note the fundal height
Second Leopold’s maneuver - Determine position of the back (lie)
· Lie is the relation of the baby’s long axis to the mother’s uterus long axis
· Still facing the mother, place both palms on the abdomen
· Hold right hand still and with deep but gentle pressure, use left hand to feel for
the firm, smooth back. Repeat using opposite hands
· Feel for:
· The foetal poles
· Regularity or irregularity and convexity
· Absence of foetal poles in the flanks = longitudinal lie
· Presence of foetal poles on the flanks = transverse lie (long axis of the fetus
is perpendicular to that of the mother’s)
· Oblique lie = long axis of the fetus is 0-90 degrees (or 90-180 degrees) to
that of the mother’s
· Uniform, firm convexity of contour = side of the foetal back
· Determine whether convex contour is nearer the front or far out in the flank –
gives idea about position
Third Leopold’s Maneuver - presentation
· Determine what part is lying above the inlet.
· Using the right hand apply the pawlik’s grip (single handed palpation) to fell
the part of foetus overlying the pelvic inlet
· If transverse, any mass felt is most likely the shoulder = shoulder
presentation
· If longitudinal lie differentiate between cephalic and breech presentation. A

hard rounded mass indicates cephalic presentation
· Pawlick’s grip gives precise findings when head is not engaged
Fourth leopold’s maneuver - engagement
· Engagement is checked while facing the mothers lower limbs and with both
hands placed on the lower abdomen
· If the fingers seem to meet below the presenting part then engagement has
not occurred. When engagement occurs, the head will be fixed on the pelvis
· Before deep engagement, as the fingers are passed down the presenting part,
the area that is most prominent on the head is noted.
· If the cephalic prominence is on the side of the small parts (limbs), it implies
the head is well flexed hence Vertex presentation
· If prominence is felt equally on both sides – deflexed hence brow
presentation
· If prominence is on the side opposite that with the small parts and indistinct
back curvature, the findings suggest face presentation.
Attitude
· Refers to the position of the foetal head to its trunk.
· The normal position is complete flexion giving vertex presentation
· When deflexion = brow presentation
· When extension = face presentation
DENOMINATOR
· Denominator is the arbitrary point on the presenting part used as a point of

reference in denoting the position of the presenting part in relation to the pelvis.
o Vertex presentation - the denominator is OCCIPUT
o Brow presentation – the denominator is sinciput
o Face presentation – the denominator is mentum or chin
o Breech presentation – the denominator is sacrum
Position
· Relation of denominator (occiput/ sacrum) of presenting part to the quadrants

of pelvis.
· Eight positions are described
o When the denominator is directed towards symphysis pubis it gives a direct

anterior position and when directed towards sacrum it gives direct posterior
position
o When denominator is directed towards the ileopectineal eminences, the position

is left or right anterior position
o If the denominator is directed towards the mid points of the ileopectineal line, it
gives left or right anterior position
o If the denominator is directed towards the left or light sacro-iliac joint then it is left
or right posterior position
· Normal presentation is anterior position with commonest being left occipital
anterior.
· Left Occipito Posterior (LOP) – 3%
· Left occipito lateral (LOL) – 40%
· Left occipito anterior (LOA) – 15%
· Right occipito anterior (ROA) – 10 %
· Right occipito lateral (ROL) – 24%
· Right occipito posterior (ROP) –
DESCENT AND ENGAGEMENT
· Refers to entry of the presenting part into the pelvis
· Head is the presenting part in 99% of all labours
· Descend is recorded in terms of the span of the foetal head still palpable in the
abdomen above the level of symphysis pubis
· The whole span of the head is subdivided into 5 fifths and each finger breaths
spans 1 fith (1/5)
· When is completely free, the descend is 5/5 then to 4/5, 3/5, 2/5, 1/5, 0/5.
· Once the widest diameter of foetal head has entered, only 2/5 is

palpable and strictly speaking, this is when engagement has occurred
· If a portion has sunk in the pelvis, pawlik’s grip may not determine the identity
of the presenting part.
AUSCULTATION
v Place the foetoscope on the back of the foetus, apply sufficient pressure to
exclude external sounds
v Take note of foetal heart rate count and regularity.
OBSTETRIC VAGINAL EXAMINATION
Indications:
ü To confirm labour
ü Pelvic assessment
ü Assess progress of labour
ü Assessment of cervical ripening before induction of labour
ü Diagnose or rule out complications of labour
Contraindications
ü Suspected PROM
ü Suspected placenta praevia.
Procedure
ü Explain the procedure to the patient
ü Let patient empty bladder
ü Provide privacy
ü Ensure adequate working space
ü Aseptic technique
Inspection of the external genitalia
ü Inspect for: scars, warts, scratch marks, varicose veins, hair distribution,
ü Any discharge – colour, consistency, smell, quantity,
ü State of urethral meatus
VULVA TOILET
ü Aseptic technique – sterile gloving
ü Roll the sterile cotton wool swabs into five small balls and Soak them in a galipot
containing antiseptic solution
ü Take them on the right hand, then drop one the left hand – swab with left hand the
furthest labia majora from the top to the perineum. Similarly, swab the other side of
labia majora.
ü Similarly, swab labia minora on both sides with the next two swabs using left
hand.
ü Separate labia minora using your left hand then swab vestibule with the swab in
the right hand from clitoris to fourchette using the right hand.
ü Drape the mother by placing the sterile towel under her buttocks and another one
on the abdomen up to the hairline of the pubic area.
SPECULUM EXAMINATION IN OBSTETRIC
Read section on speculum examination below
DIGITAL VAGINAL EXAMINATION
ü Lubricate index and middle fingers of the right hand
ü Separate the labia with two fingers of the left hand
ü Insert index and middle finger of the right hand into the vaginal canal
o The terminal phalange of the middle finger is inserted first and pressed against
the perineal body in order to relax introitus
o The index finger is then slipped in and the two fingers are directed toward the
cervix
ü Assess features at the cervis:
o Dilatation of the cervix
o Degree of thinning and softness (effacement)
o Presence or absence of membranes
o Confirm presenting part and its state eg moulding, caput
o Direction of sutures and position of fontanels
o Level of presenting part compared to the ischial spines
ü pelvic assessment
o Feel for sacral promontory

o Assess curvatures of the sacrum by sweeping your fingers downwards towards
the outlet
o Assess prominences of the ischial spines and tip of coccyx by sliding the
examining fingers along the iscial spines and coccyx
o Measure the sub-pubic angle by fitting the two examining fingers in the sub-pubic
angle
o Measure the inter-tuberous diameter by fitting the four knuckles of the examining
hand between the ischial tuberosity.
GYNAECOLOGICAL PELVIC EXAMINATION
Indication
v Suspicion of pathology of female genital system
v Exclusion of pathology
Contraindication
v Intact hymen
Requirements
v Couch with stirrups
v Sterile speculum: cusco’s, sims’, ferguson’s
o Assignment: types of speculums and different sizes. How to examine

patient using univalve speculums.
v Sterile gloves
v Non-sterile gloves
v Receiver with decontamination solution.
v chaperone, consent, good lighting
Procedure
Preparation
v Prepare environment for pelvic examination – privacy, equipment & supplies

v Explain the procedure to the patient
v Patient empty bladder, remove underclothing, position in lithotomy
v Cover her to avoid unnecessary exposure
Method: speculum examination
1. Maintain infection prevention throughout the examination – wash hands, put

on sterile gloves, use high-level disinfected / sterile instruments
2. Inspect external genitalia to screen for STI / FGM
v Warts, abnormal discharge, ulcers, bleeding from vagina, sores, swelling,

presence and distribution of hair, obvious anatomical anomalies, female genital
mutilation, cosmetics (eg rings)
3. Reassure the patient throughout the procedure
4. Choose speculum size for the patient
5. Warm blades under a stream of tepid water
6. Hold speculum in the right hand while the index finger of the left hand presses
downwards on the fourchette to expose the introitus
7. Slide the closed blades obliquely (away from the urethral area and clitoris)
over the fingers into the introitus , introduce the instrument into the vagina
8. While inserting the instrument rotate it to a clockwise direction until the anterior
and posterior blades run along the anterior and posterior vaginal walls with the
handles pointing towards the anus.
9. Open the blades to expose the cervix
10. Inspect cervix- erosion, colour, growths, friability, discharge,
11. Take lab specimens if necessary for investigation for PAP smear for cytology,
vaginal secretions for microscopy.
12. Rotate the speculum and inspect vaginal wall for: warts, abnormal discharge,
sores, bleeding
13. Remove the speculum gently in horizontal position and place it in

decontamination solution.

DIGITAL VAGINAL EXAMINATION IN GYNAECOLOGY
v Put on sterile gloves
v Clean the vulva
v Insert the index and middle fingers of right hand gently into the vaginal canal while
you avoid touching clitoris with your thumb
v Examine the cervix:
ü Ostium- open or closed
ü Irregularity
ü Growth
ü Consistency
ü Mobility
ü Tenderness
v Examination of uterus – bimanual examination
ü Place your left hand on the abdomen, just above sympysis pubis
ü Locate uterus by feeling it between your left hand over abdomen and the finger
tips of your right index and middle fingers placed on the cervix
ü Palpate for:
o size, shape and consistency, mobility,
o position : anteverted or retroverted
v Examination of the adnexia
ü locate the left fornix and place the finger tips in this fornix
ü together with left hand placed over the left side of lower abdomen, try to palpate
for any mass or tenderness
ü repeat same on the right side
v Excitation of the cervix for endometritis

ü use your right index and middle fingers to gently move the cervix from left to right
and check for any pain
v palpate the anterior, left and lateral walls of the vagina walls for: ruggae, growth,
tenderness
v check vaginal muscle tone by asking the client to tighten vaginal muscle
v check for cystocele and rectocele
ü press the left index and middle finger downwards and ask patient to cough =
rectocele
ü press the left index and middle finger upwards and ask patient to cough =
cystocele
 palpate bartholins glands on both sides of the labia majora
 press on the trigone muscle to exclude cystitis
 Milk the skenes glands with left hand.
 Palpate the inguinal LN.
EXAMINATION OF THE MALE GENITALIA
Requirements:
ü Gloves
ü Penlight
Inspection:
ü The pubic hair characteristics and distribution
ü The glans penis (retract the foreskin if patient uncircumcised):
o Colour
o Smegma
o External meatus of urethra
o Urethra discharge
Palpation:
ü The penis:
o Tenderness
o Induction
ü Strip the urethra for any discharge (you can ask the patient to perform this part of
procedure for you:
o Firmly compress the base of the penis with your thumb and forefinger and move
them towards the glans
o Press the glans penis between the thumb and forefinger
o Collect discharge
Scrotum and ventral surface of the penis:
Inspection:
ü Colour
ü Texture
ü Asymmetry
ü Unusual thickening
ü Presence of hernia
ü Trans – illuminate any masses in the scrotum
o When any mass is felt other than the testicle or spermatic cord determines
whether it is filled with gas, fluid or solid material using penlight
Palpation:
a. Inguinal canal for direct and indirect hernia
ü With patient standing, ask him to bear down as if having bowel movement
ü While he is straining inspect the areas of inguinal canal and the region of fossa
ovalis
ü Ask patient to relax, insert the pulp of your examining finger into the lower part of
the scrotum and carry it upward along vas deferens into the inguinal canal. (the
finger depends on the size of the external ring which is normally palpable)
ü With your finger placed at the external ring ask the patient to cough and feel for a
viscous mass against your finger (present if a hernia is present)
b. The testis, epididymitis, vasa deferentia

ü Use the thumb and first two fingers to assess:
i. Consistency
ii. Size
iii. Tenderness
iv. Fluid
v. Lumps or nodules
c. The inguinal lymph nodes
d. Cremasteric reflex
ü Elicit the cremasteric reflex bilaterally
ü Stroke the inner thigh with a blunt instrument such as the handle of the reflex
hammer or with your finger
ü Normally the testicle and scrotum rise on the stroked side
EXAMINATION OF THE FEMALE BREAST AND AXILLA
Breast is an appendix of the skin in the milk-lines from axilla to groin.
The development has different stages – tanner’s classification
Preparation
Undress patient as far as waist, sits upright
It is necessary after examining the patient sitting upright to ask the patient to lie flat
and reexamine the breasts
Both breasts must be exposed completely
Method
Inspection
Ø While patient in the following positions:
o Arms hanging loosely at the sides (arms aside)

o Arms held over head
o Arms held at hips
o Leading (bending) forward
Ø Inspect each breast and compare them for:
o Size
o Symmetry
o Contour
o Skin colour
o Venous pattern
o Lesions
Ø Inspect nipple for:
o Size (compare both breast)
o Retraction
o Discharge
o Ulceration
Ø Inspect the areola for pigmentation
Palpation
Ø Systematically palpate the breast, axilla and supra-clavicular regions
Ø Ask the patient to find first herself the lump and to point the lesion she has
detected, before you attempt to do so and before you start palpation
Ø Start with the normal breast to have her impression of the normal breast
Ø Palpate the areola and nipple and finish with axilla
Techniques
Ø Two techniques:
o Palpation “with the flat of the hand”
o Palpation “between the pulps of the fingers and the thumb”

Ø Flat-hand- technique:
o Exert a slight pressure on skin with the pulps of the middle and end phalanges of
the fingers 2-5 and perform a small circular movement
o Normal breast gives a firm lobulated impression with fine nodularity a feature
particularly before the periods. In fat and after menopause expect to feel both
lobulation and nodularity less easily
o With flat-hand-technique accepted techiniques include:
§ Vertical zigzag palpation
§ Concentric circular palpation
§ Quadrant palpation
o Most used technique is quadrant for clinician and self breast examination.
Ø Perform palpation calmly, with patience, without skipping any part including axilla.
Ø Palpation of areola:
o Gently squeeze the areola skin between thumb and index together with a rolling
movement (small retention cysts and glands of Montgomery can be noted as well as
small centrally located tumours)
o Indirectly by pressing with the top of index on different places of the areola, elicit
nipple secretion, if present.
Ø Palpation of nipple
o Inform patient the procedure may hurt
o Perform a short but firm squeeze of nipple between thumb and index finger
o Notice secretion
Ø Palpation of the tail of Spence and axillae
o Palpate the tail as it enters axillae by gently compressing the tissue between the
thumb and fingers
Ø Palpation of the LN
o With patient seated with arms flexed at elbow
o Support the patient’s right lower arm with your right hand to examine the right

axilla & vice varsa
o Examine-apex, medial, lateral, anterior & posterior.
NB: Make always a well documented record of your examination
v Localization : name the quadrant or describe the location using “hours”
v Size: in mm or cm
v Shape: round –discoid – regular – irregular
v Consistency: very soft, soft, firm, hard, stony or bony hard
v Contour: in relation to surrounding tissue
v Tenderness: yes or no, spontaneous
v Mobility: in relation to the skin, breast tissue, fascia, thorax wall.
COMMON INVESTIGATIONS IN REPRODUCTIVE HEALTH PRACTICE
 Learning objectives
 • At the end of the lecture, the student is expected to be able to:-
– Know the scope of the common investigations in RHC
– Acquire insight into the rational & objective request for relevant
investigations
– Apply the same or similar investigations in different clinical situations
– Interpret results of investigations for the benefit of patients
Introduction: Investigations
• Important aspect of patient management
• Should always be rational/objective
• Normal parameters should be known
• Can be expensive
• May be invasive
• Supplement but not replace clinical acumen
“Good, comprehensive medical history & physical examination remain

key to paient management”
PURPOSE FOR INVESTIGATIONS
• Confirmation of diagnosis
• Making diagnosis
• Estimate of disease severity
• Monitoring effect of treatment
• Monitoring recurrence
• Screening for disease
Common investigations in obstetrics
Antenatal care (ANC)
• [Hb] & HCT
– To screen or confirm anemia
– Forms a basis for supplementation
• VDRL
– Screening for syphylis – affects fetal outcome
– Specific treponemal tests before treatment (e.g. TPHA)
• Blood group
– Establishes risk of feto-maternal incompartibility & hemolytic disease
– Prepares for transfusion needs
• Urinalysis - Screening for protein, glycosuria, UTI, etc
• HIV - PMTCT; Entry into prevention of transmission; Enables provision of

support - psycho-social & medical
• Obstetric ultrasound - Appraisal of fetal growth; Fetal abnormality screening;

Fetal well-being assessment: BPPS; Doppler studies; PET prediction
Full blood count (FBC)

Has multiplicity of value
Examples of significance:
• [Hb] & HCT
– Presence/absence of anemia; Etiology not implied
• Cell indices - MCV, NCH, MCHC – may allot anemia to broad categories:
– Microcytic
– Hypochromic
– Megaloblastic
– Mixed
• WBC count
– Total count
• Marked elevation - acute infections (bacterial/viral)
• Moderate elevation – chronic infections
– Differential count
• Neutrophilia – acute bacterial infections
• Lymphocytosis –viral or chronic bacterial infections
• Peripheral blood film (PBF)
– RBC’s
• Normocytic normochromic; hypochromic microcytic
• Polychromasia; reticulocytosis;megaloblasts
• Anisocytosis; poikilocytosis;tear drop cells
• Spherocytes; sickle forms
– WBC,s
• Polymorphs – nuclear segmentation
• Toxic granulation
• Malaria parasites (MP,s)
• Erythrocyte sedimentation rate
– None specific
– May indicate infection
• Platelet count
– Absolute count/concentration
Infections in pregnant state
1. Urinary tract infections (UTI)
– Urinalysis:- appearanc; pH; blood; sugar; proteins; nitrites; urobilinogen;

leukocytes; bilirubin; specific gravity; ketones
– Microscopy:- pus cells; epithelial cells;casts; crystals; RBC,s; bacteria;

yeast cells; trichomona vaginalis
– Culture
– sensitivity
2. Respiratory tract infections
– FBC; chest X-ray; sputum – AAFB,s
3. Chorioamnionitis
– FBC +ESR; vaginal swab – M/C/S
4. Malaria
– MP’s
5. Blood coagulation disorders –thrombo-embolic disease & DIC

• Coagulation screen
– Bleeding time; clotting time; APTT/KCCT; PTI/INR; platelet count
• Thrombus localization
– Doppler studies
– Venography; radioisotope studies; thermography
6. Hypertensive disease in pregnancy
• Renal function tests (RFT,s)
– Urinalysis – protein, blood
– U/E; uric acid; creatinine; creatinine clearance
– Renal ultrasound
• Liver function tests (LFT,s)
– Bilirubin, liver enzymes
• Coagulation screen; platelet count
• Obstetric utrasound –FWB; doppler studies
7. Value of ultrasound in obstetrics
• Diagnosis of pregnancy
– Intaruterine; extra-uterine
• Fetal growth monitoring
– Appropriateness of growth (AGA;SGA; LGA)
– IUGR (asymmetrical; symmetrical)
– Fetal weight, sex, viability
• Fetal well-being
– BPPS (fetal tone; fetal movements; respiratory movements; AF volume;
placental echogenicity)
• Pelvimetry
• Gestation estimation-timing of specific epiphyseal plates’ closure
• Diagnosis of twins
• Diagnosis of extra-uterine pregnancy
8. Diabetes mellitus
• Urinalysis
– Glycosuria; ketonuria; proteinuria
• Blood sugar
– RBS; FBS; OGTT; PPBS; Serial BS
• Glycolysated Hb (Hb1c) - [N<6%]
• Obstetric ultrasound – IUGR; Macrosomia; BPPS; Polyhydramnios; etc
9. Rhesus isoimmunization
• Indirect Coombs test (ICT)
• AF spectrophotometry –absobance deviation at 450nm
• Cord blood at birth
– [Hb] + hct
– Direct Coombs test
– Bilirubin
10. Anemia & Antepartum hemorrhage
• Anemia
• FBC+PBF
• Stool o/c
• MPs
• Antepartum hemorrhage (APH)
• Placental localization
• Ultrasound; EUA
• Coagulation screen
• [Hb] = hct
11. Antepartum hemorrhage (APH); Establishment of fetal maturity
Septicemia & endotoxic shock
• RFTs including urine output
• Blood cultures
• Coagulation screen, especially platelet count
• Critical care investigations (spo2, spco2, etc)
Establishment of fetal maturity
• Amniocentesis
– Surfactant or ‘shake’ test
– Lecithin:sphingomyelin (L/S) ratio (N > 1:2)
Common investigations in Gynaecology
• FULL BLOOD COUNT
“Important in differentiating infective from none-infective conditions”
• Value of ultrasound scan in gynecology
• Diagnosis of pelvic masses
– Solid – fibroids; ovarian; other
– Cystic – ovarian; TOM; PCOD
– Fluid in the pelvis – PID; pelvic abscess; ectopic pregnancy
• Management of infertility
– Follicular growth monitoring; TVS for ovum retrieval
• Intrauterine diagnosis
– Endometrial hyperplasia; ‘lost’ IUCD; hematometra
• Radiology in gynecology
• Hysterosalpingogram
– Scope – uterine cavity; endoslpinx; spill
– Pathology:
• Submucous/intramural fibroids
• Tubal block (cornual, mid-section,terminal)
• Tubal loculations/peri-tubal adhesions
• Fimbrial adhesions
• hydrosalpinges
• X-ray sella turcica – hyperprolactinaemic galactorrhoea syndrome
• Erosion of clinoid processes & pituitary fossa
• Embryonal tumours – cystic teratomas
• ‘Lost’ IUCD – tracer IUCD inserted
• Extra-uterine pregnancy
• Infertility –MALE
• Semen analysis
• Appearance
• Volume
• pH
• Liquefaction
• count
• Motility
– Progressive
– Sluggish
– non-progressive
– non-motile
• Vitality
• Morphology
• Agglutination
• Pus cells
• Post-coital test
• Motility; agglutination
• Sperm-mucous interaction tests
• Direct (spouses) or crossed
• Hormonal profile
• Testicular biopsy
• Infertility – FEMALE
• Radiological – HSG; X-ray sella turcica
• Pelvic ultrasound scan
– Uterine pathology (fibroids; adenomyosis)
– ovarian pathology (PCOS)
• Hormonal profile
– FSH; LH; PRL; testosterone; progesterone; estradiol
• PCT
• Sperm-mucus interaction tests
• Visual fields
• CT-scan/MRI
• Karyotype
• Diagnostic endoscopy in gynecology
• Laparoscopy
• Chronic pelvic pain
• Endometriosis
• Infertility
• Ectopic pregnancy
• Pelvic inflammatory disease
• hysteroscopy
• Endometrial pathology
– Submucous myomas; Uterine synachie; Endometrial polyps; abnormal uterine

bleeding
• Culdoscopy
• Carcinoma of the cervix
• Papanicolou (pap) smear
• Colposcopy
• Cone biopsy
• Loop electro-excision procedure (LEEP)
• EUA, bopsy and staging
• Abnormal uterine bleeding
– D&C
– Fractional curettage
– Hysteroscopy
– Hormonal profile
• Gestational trophoblastic disease

• Hydatidiform mole
– PDT/B-hCG
– US scan – ‘snow storm appearance’
• Choriocarcinoma
– B-hCG
– Metastatic disease
• CXR (cannon balls):CT-scan/MRI (liver.renal,brain)
• Lumbar puncture; LFTs; RFTs
• Ectopic pregnancy
• PDT/b-hCG
• Pelvic U/S scan
• Laparoscopy
• Paracentesis
• Culdocentesis
• Sexually transmitted infections (STIs)
• Vaginal swab – M/C/S
– HVS
– Cervical swab
• VDRL
• HIV ELISA
Unit Four Content..
Topic 1: PUBERTY
Period when the endocrine and gametogenic functions of the gonads have first
developed to the point where reproduction is possible
This is characterized by sequence of events by which a child becomes a young

adult:
The beginning of gametogenesis
Secretion of gonadal hormones
Development of secondary sexual characters and reproductive functions
Sexual dimorphism is accentuated.
Factors affecting the onset of puberty
The age of onset of puberty varies and is more closely correlated with osseous
maturation than with chronological age
Genetic/Ethnic factors
Environmental/Geographical factors
Prepubertal stage (8–9 yr of age)
The hypothalamic-anterior pituitary-gonadal axis is suppressed by;
Neuronal restraint pathways
Negative feedback provided by minute amounts of circulating gonadal steroids
Thus there are undetectable serum levels of;
luteinizing hormone (LH)
sex hormones (i.e., estradiol in girls, testosterone in boys)
PREPUBERTY STAGE
Evidence of hypothalamic-anterior pituitary-gonadal interaction during the

prepubertal period resides in the fact that serum follicle-stimulating hormone
(FSH) concentrations are detectable in most children and may be increased
(with serum LH concentrations) in;
Turner syndrome
Anorchia
Peripubertal period (1-3 yr before the onset of puberty)
Pulsatile secretion of low levels of LH during sleep secondary to endogenous

episodic discharge of hypothalamic gonadotropin-releasing hormone (GnRH).
Nocturnal pulses of LH continue to increase in amplitude and, to a lesser extent, in

frequency as clinical puberty approaches.
Serum LH concentrations rise earlier in the course of the pubertal process in boys
than in girls.
This pulsatile secretion of gonadotropins is responsible for;
Enlargement and maturation of the gonads
The secretion of sex hormones
Appearance of the secondary sex characteristics
NB
GnRH is the major, if not the only, hormone responsible for the onset and
progression of puberty.
A second critical event occurs in middle or late adolescence in girls, in whom

cyclicity and ovulation occur.
A positive-feedback mechanism develops whereby rising levels of estrogen in

midcycle cause a distinct increase of LH.
Puberty in Girls (8-13yr)
Thelarche (Development of Breasts) - Breast bud - 10–11 yrs
Pubarche (Development of axillary and pubic hair) - Appearance of pubic hair - 6–12

mo later
Peak height velocity occurs early (at breast stage II–III, typically between 11 and 12
yr of age) in girls and always precedes menarche.
Menarche (first menstrual period) Interval to menarche - 2–2.5 yr but may be as long
as 6 yr after thelarche.
Mean age of menarche - 12.75 yr. (13.5 yrs in rural girls)
Puberty in Boys (9-14yr)
Growth of the testes (>3 mL in volume or 2.5 cm in longest diameter)
Thinning of the scrotum
Pigmentation of the scrotum
Growth of the penis, seminal vesicles and prostrate
Pubic hair then appears
Appearance of axillary hair usually occurs in midpuberty, 2 yr after pubic hair.
In boys, unlike girls, acceleration of growth (5-15cm/yr in early adolescence but later
drops) begins after puberty is well under way and is maximal at genital stage IV–V
(typically between 13 and 14 yr of age).
In boys, the growth spurt occurs approximately 2 yr later than in girls, and growth
may continue beyond 18 yr of age.
Adrenarche
Adrenal cortical androgens also play a role in pubertal maturation.
Serum levels of dehydroepiandrosterone (DHEA) and its sulfate (DHEAS) begin

to rise at approximately 6–8 yr of age, before any increase in LH or sex
hormones and before the earliest physical changes of puberty are apparent.
NB
DHEAS is the most abundant adrenal C-19 steroid in the blood, and its serum
concentration remains fairly stable over 24 hr; a single measurement of this
hormone is commonly used as a marker of adrenal androgen secretion.
Although adrenarche typically antedates the onset of gonadal activity (i.e.,

gonadarche) by a few years, the two processes do not seem to be causally related,
because adrenarche and gonadarche are dissociated in conditions such as;
Central precocious puberty

Adrenocortical failure
ENDOCRINOLOGY IN PUBERTY
The levels of gonadal steroids and gonadotropins are low until the age of 6–8 yrs
This is mainly due to the negative feedback effect of estrogen to the hypothalamic
pituitary system (Gonadostat).
The gonadostat remains very sensitive (6–15 times) to the negative feedback effect,
even though the level of estradiol is very low (10 pg/ml) during that time.
As puberty approaches this negative feedback effect of estrogen is gradually lost.
This results in some significant changes in the endocrine function of the girl.
Hypothalamopituitary gonadal axis
The GnRH pulses from hypothalamus results in pulsatile gonadotropin secretion

(first during the night then by the day time).
GnRH → FSH, LH → Estradiol
The tonic and episodic secretion of gonadotropins in prepubertal period is gradually

changed to one of cyclic release in postpubertal period
..
Adrenal glands (Adrenarche)
increase their activity of sex steroid synthesis (androstenedione, DHA, DHAS) from
about 7 years of age.
Increased sebum formation, pubic and axillary hair and change in voice are primarily
due to adrenal androgen production.
Gonadarche:
Increased amplitude and frequency of GnRH → ↑ secretion of FSH and LH →

ovarian follicular development → ↑ estrogen.
Gonadal estrogen is responsible for the development of uterus, vagina, vulva and
also the breasts
Menarche
The onset of first menstruation in life is called menarche.

It may occur anywhere between 10 and 16 years, the peak time being 13 years.
The first period is usually anovular.
The ovulation may be irregular for a variable period following menarche and may
take about 2 years for regular ovulation to occur.
The menses may be irregular to start with.
ADOLESCENCE
The period of life beginning with puberty and ending with completed growth and
physical maturity.
Between the ages of 10 - 19 yr (WHO), children undergo rapid changes in;
Phenotypic changes: - Body size & Body shape
Neuroendocrine changes - Hormones set the developmental agenda in conjunction

with social structures designed to foster the transition from childhood to adulthood.
Physiology
Psychological functioning
Social functioning
NB: 10-24 yr - Young Adults
Marshall - Tanner Classification of Sex Maturity Stages in Girls
(Tanner JM, Growth of Adolescence, 1962)
SMR = sexual maturity rating.
SMR Stage Pubic Hair Breasts
Preadolescent
1 Preadolescent
2 Sparse, lightly pigmented, straight, medial Breast and papilla

border of labia
elevated as small mound;
areolar diameter
increased
Breast and areola enlarged
3 Darker, beginning to curl, increased amount , no contour
separation
Areola and papilla form
Coarse, curly, abundant but amount less than in
4 secondary mound
adult
Mature; nipple projects,

Adult feminine triangle, spread to medial surface
5 areola part of general
of thighs
breast contour
Marshall - Tanner Classification of Sex Maturity Stages in Boys
SMR Stage PUBIC HAIR PENIS TESTES
1 None Preadolescent Preadolescent
Scanty, long, slightly Enlarged scrotum, pink

2 Slight enlargement
pigmented texture altered
Darker, starts to curl, small

3 Longer Larger
amount
Larger; glans and

Resembles adult type, but less
4 Larger, scrotum dark
in quantity; coarse, curly
breadth increase in size
5 Adult distribution, spread to increase in size Adult size

medial surface of thighs Adult size
Adolescence
Developmental lines occur within three periods of adolescence;
Early Adolescence – 10 – 13YRS
Middle Adolescence – 14-16yrs
Late Adolescence – 17-20 yrs and beyond
Variable Early Adolescence Middle Adolescence Late Adolescence

Age (yr) 10–13 14–16 17–20 and beyond
SMR* 1–2 3–5 5
Height growth peaks;
Secondary sex body shape and
Somatic characteristics; beginning composition change; acne Slower growth
of rapid growth; awkward and odor; menarche;
spermarche
Sexual drive surges;

Sexual interest usually experimentation; Consolidation of sexual
Sexual
exceeds sexual activity questions of sexual identity
orientation
Emergence of abstract
Concrete operations;
Cognitive and moral thought; questioning Idealism; absolutism
conventional morality
mores; self–centered
Preoccupation with Concern with

Relatively stable body
Self–concept changing body; self– attractiveness, increasing
image
conscious introspection
Bids for increased Continued struggle for Practical independence;

Family independence; acceptance of greater family remains secure
ambivalence autonomy base
Peers Same–sex groups; Dating; peer groups less Intimacy; possibly

conformity; cliques important commitment
Gauging skills and Career decisions (e.g.,

Relationship to society Middle–school adjustment
opportunities dropout, college, work)
Common Disorders of Puberty
• Precocious puberty
• Delayed puberty
• Menstrual abnormalities (amenorrhea, menorrhagia, dysmenorrhea)
• Others (infection, neoplasm, hirsutism, etc.)
PRECOCIOUS PUBERTY
The term precocious puberty is reserved for girls who exhibit any secondary sex
characteristics before the age of 8 or menstruate before the age of 10.
Precocious puberty may be isosexual where the features are due to excess
production of estrogen.
It may be heterosexual where features are due to excess production of androgen

(from ovarian and adrenal neoplasm).
FORMS OF PRECOCIOUS PUBERTY
GnRH dependent—80% (complete, central, isosexual or true)
Constitutional—most common
Juvenile primary hypothyroidism
Intracranial lesions—trauma, tumor or infection
Incomplete
Premature thelarche
Premature puberche
Premature menarche
CAUSES OF PRECOCIOUS PUBERTY
GnRH independent (precocious pseudopuberty or peripheral) (Excess estrogen

or androgen)
Ovary
Granulosa cell tumor
Theca cell tumor
Leydig cell tumor
Chorionic epithelioma
Androblastoma
McCune-Albright syndrome
Adrenal
Hyperplasia
Tumor
Liver
Hepatoblastoma
Iatrogenic
Estrogen or androgen intake
Precocious puberty in a girl aged

2 years and 3 months
DIAGNOSIS
History
Basic investigations
X-ray, ct scan, MRI
Serum hCG, FSH, LH
Thyroid profile (TSH, T4)

Serum estradiol, testosterone, 17 OH progesterone, dehydroepiandrosterone
(DHEA).
Electroencephalogram.
TREATMENT
The goals are:
To reduce gonadotropin secretions.
To suppress gonadal steroidogenesis or counteract the peripheral action of sex

steroids.
To decrease the growth rate to normal and slowing the skeletal maturation.
To protect the girl from sex abuse.
DRUG MNX
GnRH agonist therapy arrests the pubertal precocity and growth velocity

significantly.
The agonists suppress the premature activation of hypothalamopituitary axis due to

down regulation and thereby diminished estrogen secretion.
GnRH agonist therapy is the drug of choice in cases with GnRH dependent
precocious puberty.
GnRH agonist therapy suppresses FSH, lH secretion, reverses the ovarian cycle,
establishes amenorrhea, causes regression of breast, pubic hair changes, and other
secondary sexual characteristics.
This drug should be continued till the median age of puberty
GnRH agonist
• Buserelin nasal spray 100 mg daily. It can slow down the process of skeletal
maturation
• Medroxyprogesterone acetate—30 mg daily orally or 100–200 mg. IM

weekly to suppress gonadal steroids. It can suppress menstruation and breast
development but cannot change the skeletal growth rate.
• Cyproterone acetate—It acts as a potent progestogen, having agonist

effects on progesterone receptors.
Dose—70–100 mg/m2/day orally for 10 days starting from 5th day of cycle.

4. Danazol—It produces amenorrhea and arrest breast development. But there is
no effect on growth rate or skeletal maturation.
2. DELAYED PUBERTY
Puberty is said to be delayed when the breast tissue and/or pubic hair have
not appeared by 13–14 years or menarche appears as late as 16 years.
The normal upper age limit of menarche is 15 years.
CAUSES OF DELAYED PUBERTY
• Hypergonadotropic hypogonadism
Gonadal dysgenesis, 45 XO
Pure gonadal dysgenesis 46 XX, 46 XY
Ovarian failure 46 XX
2. Hypogonadotropic hypogonadism
Constitutional delay
Chronic illness, malnutrition
Primary hypothyroidism
Isolated gonadotropin defi ciency (Kallmann’s syndrome)
Intracranial lesions—tumors: craniopharyngioma, pituitary adenomas
3. Eugonadism
Anatomical causes
Müllerian agenesis
Imperforate hymen
Transverse vaginal septum
Androgen insensitivity syndrome
Menstrual cycle
A periodic physiologic vaginal hemorrhage, occurring at approximately 28 ± 7 days

interval (from the start of one menstrual period to the start of the next), and
having its source from the shedding of uterine mucous membrane
(menstruation); usually the bleeding is preceded by ovulation and predecidual
changes in the endometrium.
This may be teleologically regarded as periodic preparations for fertilization and

pregnancy.
Menstruation is the visible manifestation of cyclic physiologic uterine bleeding due to

shedding of the endometrium following invisible interplay of hormones mainly
through hypothalamo-pituitaryovarian axis.
For the menstruation to occur, the axis must be actively coordinated,

endometrium must be responsive to the ovarian hormones (estrogen and
progesterone) and the outflow tract must be patent.
The first menstruation (menarche) occurs between 11–15 years with a mean of 13
years. It is more closely related to bone age than to chronological age
For the past couple of decades, the age of menarche is gradually declining with
improvement of nutrition and environmental condition.
Physiologically, it is kept in abeyance due to pregnancy and lactation
Women have around 400 menstrual cycles during the course of their lifetimes
Ultimately, it ceases between the ages 45–50 when menopause sets in
The duration of menstruation (menses) is about 4–5 days and the amount of blood
loss is estimated to be 20 to 80mL with an average of 35mL.
Nearly 70% of total menstrual blood loss occurs in the first 2 days.
The menstrual discharge consists mainly of:
dark altered blood,
mucus,
vaginal epithelial cells,
fragments of endometrium,
prostaglandins,
enzymes and bacteria.
Prenatal follicular development
During intrauterine fetal development, the ovary develops through 3 stages;

Genital ridge stage - Sex cells can first be identified and begin as hypertrophy of
the coelomic epithelium (future peritoneum) overlying the developing mesonephroi.
Further growth of the ridges is dependent upon the arrival of germ cells.
Indifferent stage - Proliferation of germinal cells by mitosis and somatic cells
Sexual differentiation stage - Fundamental histologic differences between the

ovary and testis are established
To maintain species-specific chromosome complement;
 the male gametes go through meiosis after puberty and continues throughout life
owing to persistence of mitotically active “stem cells”, (spermatogonia)
 the female gametes undergo meiosis during fetal life and all stem cells are eliminated
during birth when meiosis is suspended in the middle of the first meiotic division to
resume shortly before ovulation in response to LH surge
The normal human menstrual cycle can be divided into two segments:
 the ovarian cycle and
 the uterine cycle, based on the organ under examination
The ovarian cycle
Def: is the cyclic hormonal changes and other series of changes that occur in the
ovary to mature the immature follicle and recruit the oocyte.
It may be further divided into:
Follicular phase extends from the beginning of menstruation (day 1) to the onset of

ovulation. The average length of the human follicular phase ranges from 10 to 14
days, and variability in this length is responsible for most variations in total cycle
length.
Ovulation.
luteal phase (post ovulstory phase) extends from ovulation to the beginning of

menstruation. Unlike the follicular phase this phase is most predictable and
constant (14 days) in length
Ovarian cycle
the ovarian cycle consists of:
Follicular phase:
Recruitment of groups of follicles
Selection of dominant follicle and its maturation.
Ovulation
Luteal phase:
Corpus luteum formation
Demise of the corpus luteum.
Recruitment of groups of follicles (Preantral phase)
The cohort of the growing follicles undergoes a process of development and

differentiation which takes about 85 days and spreads over 3 ovarian cycles.
It is not clear as to how many and which of the primordial follicles amidst several
thousands are recruited for a particular cycle.
It is presumed that about 20 antral follicles (about 5–10 per ovary) proceed to
develop in each cycle.
..
The initial recruitment and growth of primordial follicles are not under the control of
any hormone.
After a certain stage (2–5 mm in size), the growth and differentiation of primordial
follicles are under the control of FSH.
Unless the follicles are rescued by FSH at this stage, they undergo atresia.
..
With FSH, the oocyte is now surrounded by an acellular barrier of glycoprotein

produced by the follicular cells and is called zona pellucida.
The flattened outer single layer pregranulosa cells become cuboidal and multilayered
—now called granulosa cells
Then, there is appearance of channels (gap junctions) between the granulosa cells
and the oocyte.
Through these gap junctions nutrition to the oocyte is maintained.

There is noticeable beginning of differentiation of the theca interna layer of ovarian
stroma surrounding the follicle.
The granulosa cells now acquire FSH receptors.
Antrum formation
Then, there is accelerated growth of all the components of the follicles of the prentral
phase.
The granulosa cells grow faster than the theca cells.
There is production of follicular fluid which is primarily an ultrafiltrate of blood from

the vessels within theca interna.
The fluidfilled space is formed amidst the granulosa cells.
The spaces coalesce to form an antrum
Dominant Follicle
As early as day 5–7, one of the follicles out of so many becomes dominant and
undergoes further maturation.
It seems probable that the one with highest antral concentration of estrogen and
lowest androgen and whose granulosa cells contain the maximum receptors for
FSH, becomes the dominant follicle.
The rest of the follicles become atretic by day 8
Further growth of dominant follicle
There is marked enlargement of the granulosa cells.
The granulosa cells surround the ovum to form cumulus oophorus which infact

anchors the ovum to the wall of the follicle.
The cells adjacent to the ovum are arranged radially and is called corona radiata.
At this stage, FSH induces LH receptors on the granulosa cells of the dominant

follicle.
LH receptor induction is essential for the mid-cycle LH surge to induce ovulation,

luteinization of the granulosa cells to form corpus luteum and secretion of
progesterone (two cell, two gonadotropin therapy)
Mature Graafian follicle
The fully mature Graafian follicle just prior to ovulation measures about 20 mm,
and is composed of the following structures from outside inward:
• Theca externa.
• Theca interna.
• Membrana granulosa (limitans).
• Granulosa cell layer.
• Discus proligerus in which the ovum is incorporated with cells arranged

radially (corona radiata).
• Antrum containing vesicular fluid.
NB
it takes 3 months for the follicle to grow and mature to ovulation—2 months to reach
an antral stage measuring 1 mm; 2 weeks to reach 5 mm and another 2 weeks to
reach 20mm before ovulation.
Hormonal changes during follicular phase of ovarian cycle…
At the start of the menstrual cycle, FSH levels begin to rise as the pituitary is
released from the negative feedback effects of progesterone, oestrogen and inhibin.
Rising FSH levels rescue a cohort of follicles from atresia, and

initiate steroidogenesis.
Under influence of FSH, a cavity forms around the ovum (antrum formation).
NB. On steroidogenesis
The basis of hormonal activity in pre-antral to pre-ovulatory follicles is described as

the 'two cell, two gonadotrophin' hypothesis.
Steroidogenesis is compartmentalized in the two cell types within the follicle: the

theca and granulosa cells.
The two cell, two gonadotrophin hypothesis states that these cells are responsive to
the gonadotrophins LH and FSH respectively.
Within the theca cells, LH stimulates the production of androgens from

cholesterol.
Within the granulosa cells, FSH stimulates the conversion of thecally derived
androgens to oestrogens (aromatization).
In addition to its effects on aromatization, FSH is also responsible for the proliferation
of granulosa cells.
Androgen production within the follicle regulate the development of the pre-antral

follicle.
Low levels of androgens enhance aromatization and therefore increase oestrogen

production.
In contrast, high androgen levels inhibit aromatization and produce follicular

atresia.
A delicate balance of FSH and LH is required for early follicular development.
The ideal situation for the initial stages of follicular development is low LH levels
and high FSH levels, as seen in the early menstrual cycle.
If LH levels are too high, theca cells produce large amounts of androgens, causing
follicular atresia.
The selection of the dominant follicle is the result of complex signalling between the
ovary and the pituitary.
Such a follicle has the most efficient aromatase activity and

the highest concentration of FSH-induced LH receptors.
The dominant follicle therefore produces the greatest amount of oestradiol and
inhibin.
Inhibin further amplifies LH-induced androgen synthesis, which is used as a

substrate for oestradiol synthesis.
These features mean that the largest follicle therefore requires the lowest levels of
FSH (and LH) for continued development.
At the time of follicular selection, FSH levels are declining in response to the
negative-feedback effects of oestrogen.
The dominant follicle is therefore the only follicle that is capable of continued
development in the face of falling FSH levels.
in-vitro fertilization (IVF) & multiple pregnancy

During in-vitro fertilization (IVF), the production of many ovulatory follicles is desired
to harvest many oocytes.
with the administration of exogenous gonadotrophins, many follicles continue to

develop and are released at ovulation, with an ensuing multiple gestation rate of
around 30%
INHIBIN & ACTIVIN
Granulosa cell inhibin enhances LH -induced androgen synthesis.
The production of inhibin is a further mechanism by which FSH levels are reduced
below a threshold at vlhich only the dominant follicle can respond, ensuring atresia of
the remaining follicles.
Activin augments pituitary FSH secretion and increases FSH binding to granulosa
cells.
Ovulation
The dominant follicle, shortly before ovulation reaches the surface of the ovary.
The cumulus becomes detached from the wall, so that the ovum with the
surrounding cells (corona radiata) floats freely in the liquor folliculi.
The oocyte completes the first meiotic division with extrusion of the first polar body
which is pushed away.
The follicular wall near the ovarian surface becomes thinner.
Hormonal changes at ovulation
As the dominant follicle develops further, follicular oestrogen production

increases.
Eventually the production of oestrogen is sufficient for it to reach the threshold

required to exert a positive-feedback effect on pituitary LH secretion
LH levels increase, at first quite slowly (day 8 to day 12 of the menstrual cycle) and
then more rapidly (day 12 onwards).
Hormonal changes at ovulation..
During this time, LH induces luteinization of granulosa cells in the dominant follicle,

so that progesterone is produced.
Progesterone further amplifies the positive-feedback effect of oestrogen on pituitary

LH secretion, leading to a surge of LH.
Ovulation occurs 36 hours after the onset of the LH surge.
Hormonal changes at ovulation…
In addition to the rise in LH, FSH and oestrogen that occurs around ovulation, a rise
in serum androgen levels also occurs.
These androgens are derived from the stimulatory effect of LH on theca cells,

particularly those of the non-dominant follicle.
This rise in androgens may have an important physiological effect in the stimulation

of libido, ensuring that sexual activity is likely to occur at the time of ovulation, when
the woman is at her most fertile and enhance the process of atresia of the small
follicles.
Prior to the release of the oocyte at the time of ovulation, the LH surge stimulates the
resumption of meiosis, a process which is completed after the sperm enters the egg
(fertilization)
Additionally, the LH surge stimulates increased follicular leukocytes eg macrophage

chemotactic protein-1 (MCP-I), interleukin 8 (IL-8) & neutrophils into the pre-
ovulatory follicle.
Once activated, these leukocytes secrete mediators which cause the follicle wall to
break down, releasing the oocyte at ovulation.
LUTEAL PHASE
Following ovulation, the follicle is changed to corpus luteum.
The ovum is picked up into the fallopian tube and undergoes either degeneration or
further maturation, if fertilization occurs.
Menstruation is unrelated to ovulation and anovular menstruation is quite

common during adolescence, following childbirth and in women approaching
menopause.
Corpus Luteum
Stage of Proliferation
The opening through which the ovum escapes soon becomes plugged with fibrin.
The granulosa cells undergo hypertrophy without multiplication.
The cells become larger, polyhedral with pale vesicular nuclei and frothy cytoplasm.
The cells are called granulosa lutein cells.
The color of thecorpus luteum at this stage is greyish yellow due to presence of

lipids
Corpus luteum..
Stage of Vascularization
Within 24 hours of rupture of the follicle, small capillaries grow into granulosa layer
towards the lumen accompanied by lymphatics and fibroblasts.
Extensive vascularization within the corpus luteum ensures that the granulosa cells
have a rich blood supply providing the precursors for steroidogenesis.
Corpus luteum..
Stage of Maturation
By 4th day, the luteal cells have attained the maximum size.
Approximately about 7–8 days following ovulation, the corpus luteum attains a size
of about 1–2 cm and reaches its secretory peak.
The lutein cells become greatly enlarged and develop lipid inclusion, giving the cells
a distinctive yellowish color. Cell contain a yellow pigment called lutein
Corpus luteum
Stage of Regression
On the day 22–23 of cycle, retrogression starts.
The first evidence of degeneration is appearance of vacuolation in the cells.
The lutein cells atrophy and the corpus luteum becomes corpus albicans.
Regression of corpus luteum is due to withdrawal of tonic LH support

If, however, fertilization occurs in the particular cycle, regression fails to occur,
instead it is converted into corpus luteum of pregnancy.
Hormonal changes in luteal phase
is characterized by the production of progesterone from the corpus luteum within the
ovary.
The production of progesterone from the corpus luteum is dependent on continued

pituitary LH secretion.
However, serum levels of progesterone are such that LH and FSH production is
relatively suppressed by inhibin.
The low levels of gonadotrophins mean that the initiation of new follicular growth

is inhibited for the duration of the luteal phase.
Hormonal changes in luteal phase
In the absence of pregnancy and the production of human chorionic gonadotrophin

(hCG) from the implanting embryo, the corpus luteum regresses at the end of the
luteal phase, a process known as luteolysis.
As the corpus luteum dies, oestrogen, progesterone and inhibin levels decline.
The pituitary is released from the negative-feedback effects of these hormones, and

gonadotrophins, particularly FSH, start to rise.
A cohort of follicles that happen to be at the pre-antral phase is rescued from atresia
and a further menstrual cycle is initiated.
Corpus Luteum of Pregnancy
There is a surge of hyperplasia of all the layers between 23rd to 28th day due to
chorionic gonadotropin.
hCG, like LH will stimulate the corpus luteum to secrete progesterone.
The growth reaches its peak at about 8th week when it measures about 2–3 cm.
Regression occurs following low levels of chorionic gonadotropin and the

degenerative changes take place most frequently at about 6 months of gestation.
Corpus luteum secretions

predominantly progesterone is secreted by the corpus luteum to support the
endometrium of the luteal phase.
There is also secretion of estrogen, inhibin and relaxin.
Progesterone along with estrogen from corpus luteum maintain the growth of the
fertilized ovum.
This is essential till the luteal function is taken over by the placenta.
This turn over of function from corpus luteum of pregnancy to placenta is

called luteal-placental shift.
This transition period continues from seven weeks to ten weeks.
UTERINE CYCLE
ENDOMETRIUM
The endometrium is the lining epithelium of the uterine cavity above the level of
internal os.
It consists of surface epithelium, glands, stroma and blood vessels.
Two distinct divisions are established:—

basal zone (stratum basalis) and
the superficial functional zone.
BASAL LAYER
It is about one-third of the total depth of the endometrium and lies in contact with the
myometrium.
The base of the endometrial glands extends into the layer.
The zone is uninfluenced by hormone and as such, no cyclic changes are observed.
After shedding of the superficial part during menstruation, the regeneration of all the
components occurs from this zone. It measures about 1 mm.
FUNCTIONAL LAYER
This zone is under the influence of fluctuating cyclic ovarian hormones, estrogen and
progesterone.
The changes in different components during an ovulatory cycle has been traditionally
divided into four stages:
Regenerative phase.
Proliferative phase.
Secretory phase.
Menstruation
STAGE OF REGENERATION
starts even before the menstruation ceases and is completed 2–3 days after the end
of menstruation.
New blood vessels grow from the stumps of the old one.
The glands and the stromal cells are regenerated from the remnants left in the basal
zone.
The glands are lined by the cubical epithelia.
The thickness averages 2 mm.
STAGE OF PROLIFERATION
extends from 5th or 6th day to 14th day (till ovulation).

The proliferative changes occurs due to rise in level of ovarian estrogens.
The glands become tubular and lie perpendicular to the surface.
The epithelium becomes columnar.
Unbranched spiral vessels with capillary congestion
The thickness measures about 3–4 mm.
SECRETORY PHASE
The changes of the components are due to the combined effects of estrogen and
progesterone liberated from the corpus luteum after ovulation.
The endometrium contains receptors for progesterone which are induced by

estrogen.
Thus, the progesterone can only act on the endometrium previously primed by
estrogen.
It begins on day 15 and ceases 5–6 days prior to menstruation.
The surface epithelium becomes more columnar and ciliated at places.
The glands show predominant changes.
The glands increase in size.
The lining epithelium become taller.
There is appearance of vacuoles due to secretion of glycogen between the nuclei

and the basement membrane.
The glands become corkscrew-shaped. The blood vessels undergo marked

spiraling.
The thickness of the endometrium reaches its highest (6–8 mm)
The endometrial growth ceases 5–6 days prior to menstruation (22nd or 23rd day of
cycle) in an infertile cycle.
The subepithelial capillaries and the spiral vessels are engorged.
MENSTRUAL PHASE
It is essentially degeneration and casting off an endometrium prepared for a

pregnancy.
Regression of corpus luteum with fall in the level of estrogen and progesterone is an
invariable preceding feature
Thes marked spiralling of the arteries and the withdrawal of hormones estrogen

and progesterone causes intense spasm of the spiral arterioles at the basal part.
These two lead to stasis and tissue anoxemia.
There are evidences of infiltration of leucocytes and monocytes in the stroma.
Stasis of blood and spasm of the arterioles lead to damage of the arteriolar walls.
There is enzymatic autodigestion of the functional zone.
The bleeding occurs from the broken arteries, veins and capillaries and also from the
stromal hematoma, with the superficial functional layer being shed into the uterine
cavity
The menstrual flow stops as a result of combined effect of prolonged

vasoconstriction, myometrial contraction and local aggregation of platelets with
deposition of fibrin around them.
ANOVULAR MENSTRUATION
In an anovulatory cycle, the follicles grow without any selection of dominant follicle.
The estrogen is secreted in increasing amount.
There may be imbalance between estrogen and FSH or because of temporary

unresponsiveness of the hypothalamus to the rising estrogen, GnRH is suppressed
→ no ovulation.
The net effect is unopposed secretion of estrogen till the follicles exist.
The endometrium remains in either proliferative or at times hyperplastic state.
When the estrogen level falls, there is asynchronus shedding of the endometrium
and menstruation.
The bleeding may be heavy or prolonged and irregular
This type of bleeding is mostly found during adolescence, following childbirth and
abortion and in premenopausal period.
ARTIFICIAL POSTPONEMENT
The hormones used for deferment of the period are—combined oral pill, 2 tablets
daily or progestogen such as norethisterone 5 mg twice daily.
The drug should be taken at least 3–6 days before the expected date of the period
and continued until the crisis is over.
The period is expected 2–3 days after the drug is suspended.
The normal menstrual cycle-clinical features
normal menstrual cycle is 28 days +/- 7days
duration of menstrual flow is 3-7 days.
Menstrual cycles are longest immediately after puberty and in the 5 years leading up
to the menopause, corresponding to the peak incidence of anovulatory cycles.
The length of the menstrual cycle is determined by the length of the follicular phase.
Once ovulation occurs, luteal phase length is fairly fixed at 14 days in almost all
women.
Clinical features
The amount of menstrual flow peaks on the first or second day of menstruation.
The normal volume of menstrual loss is 35 mL per month.
A menstrual loss of greater than 80 mL is considered to be excessive - this level is

rather arbitrary and corresponds to the threshold at which iron deficiency anaemia
may ensue unless treated.
New developments
IVF - exogenous gonadotrophins are administered to stimulate follicular growth

within the ovary
GnRH antagonists
GnRH agonists
Menstrual Disorders

 • Dysmenorrhea, mittelschmerz’s syndrome and Premenstrual
syndrome
• Abnormal uterine bleeding:
• Amenorrhea and Oligomenorrhea

• Polycystic ovarian syndrome
• Dysfunctional uterine bleeding
• Postmenopausal bleeding
1. MITTELSCHMERZ’S SYNDROME (Ovular Pain)
 Ovular pain is not an infrequent complaint.

 It appears in the midmenstrual period.
 The pain is usually situated in the hypogastrium or in either iliac fossa.
 The exact cause is not known.
The probable factors are:
 • Increased tension of the Graafian follicle just prior to rupture,

 • Peritoneal irritation by the follicular fluid following ovulation and
 • Contraction of the tubes and uterus
2. DYSMENORRHEA
 Dysmenorrhea literally means painful menstruation.

 But a more realistic and practical definition includes cases of painful menstruation
of sufficient magnitude so as to incapacitate day-to-day activities.
 Prevalence: Dysmenorrhea is a very common complaint, experienced by 45-95 per
cent of women of reproductive age.
Types:
Primary
Secondary
PRIMARY DYSMENORRHEA (Spasmodic)
 The primary dysmenorrhea is one where there is no identifiable pelvic pathology.

 The incidence of primary dysmenorrhea of sufficient magnitude with incapacitation is
about 15–20%.
 The risk factors for primary dysmenorrhoea include:
 duration of menstrual flow of > 5 days,
 younger than normal age at menarche,
 cigarette smoking.
 There is some evidence to support the assertion that dysmenorrhoea improves after
childbirth, and it also appears to decline with increasing age.
 The severity of pain usually lasts for few hours, may extend to 24 hours but seldom
persists beyond 48 hours.
SECONDARY DYSMENORRHEA
(Congestive)
 is normally considered to be menstruation — associated pain occurring in the

presence of pelvic pathology.
 The pain may be related to increasing tension in the pelvic tissues due to pre-
menstrual pelvic congestion or increased vascularity in the pelvic organs.
Common causes of secondary dysmenorrhea:
 chronic pelvic infection,

 Pelvic endometriosis,
 adenomyosis
 pelvic adhesions / Asherman's syndrome
 Uterine fibroid,
 endometrial polyp,
 IUCD in utero
 Pelvic congestion.
 (rarely) cervical stenosis.
 Obstruction due to mullerian malformations

 NB: some definitions
o Endometriosis: Endometrial stroma & glands remote of the uterine cavity,
responsive to ovarian hormone variations with fibrosis of surrounding tissues
o Sites; Uterine ligaments, bowel, urinary tract, pelvic peritonuem, ovaries,
abdominal wall, perineum & vagina.
o Adenomyosis/endometriosis interna: Extension of endometrial glands and
stroma into the myometrium
Clinical features of secondary dysmenorhea
 The pain is dull, situated in the back and in front without any radiation.
 It usually appears 3–5 days prior to the period and relieves with the start of bleeding.
 The onset and duration of pain depends on the pathology producing the pain.
 There is no systemic discomfort unlike primary dysmenorrhea.
 The patients may have got some discomfort even in between periods
Treatment of dysmenorhea
 NSAIDs, such as naproxen, ibuprofen and mefenamic acid, are reasonably effective.
Aspirin, Mefenamic acid (500mg TID)
 Oral contraceptives are widely used but, surprisingly, there is little evidence.
 Surgical treatments aimed at interrupting the nerve pathways from the uterus have
been employed
 Treat underlying conditions
 Conservative mgt; taking a hot bath, using a hot water bottle and relaxing in bed
3. PREMENSTRUAL SYNDROME (PMS) (Syn : Premenstrual Tension)
 is the occurrence of cyclical psychoneuroendocrine disorder of unknown

etiology, often noticed just prior to menstruation (in luteal phase-premenstrual)
and resolve by the time menstruation ceases.
 Occur during the last 7–10 days of the menstrual cycle.
It should fulfil the following criteria:
 Not related to any organic lesion.

 cyclic symptoms occurring only during luteal phase
 Symptoms must be severe enough to disturb the lifestyle of the woman or she
requires medical help.
 Symptom-free period during rest of the cycle.
 symptoms relieved with onset of menses
 symptoms present for at least 3 cycles
Pathophysiology:
The exact cause is not known but the following hypotheses are postulated :
(a) Alteration in the level of estrogen and progesterone starting from the midluteal
phase. Either there is altered estrogen : progesterone ratio or diminished
progesterone level.
(b) Neuroendocrine factors :
 Serotonin is an important neurotransmitter in the CNS. During the luteal

phase, decreased synthesis of serotonin is observed in women suffering from
PMS.
 Endorphins: The symptom complex of PMS is thought to be due to the
withdrawal of endorphins (neurotransmitters) from CNS during the luteal
phase.
 γ-aminobutyric acid (GABA) suppresses the anxiety level in the brain.
Medications that are GABA agonist, are effective.
(c) Psychological and psychosocial factors may be involved to produce behavioral

changes.
Unfortunately, nothing is conclusive
CLINICAL FEATURES
 Bloating
 cyclical weight gain
 Mastalgia
 abdominal cramps
 Fatigue
 Headache
 depression
 irritability.
TREATMENT OF PMS
 As the etiology is multifactorial and too often obscure, various drugs are used
either on speculation or empirically with varying degrees of success.
 Life style modification and congnitive behavior therapy are important
steps.
 Nonpharmacological:
o Assurance, Yoga, Stress management, Diet manipulation.
o Avoidance of salt, caffeine and alcohol specially in second half of cycle
improves the symptoms.
Nonhormonal :
 Tranquilizers or antidepressant drugs, may be of help logically.

 Pyridoxine 100 mg Bid is helpful by correcting tryptophan
metabolism - depression.
 Diuretics - Frusemide 20 mg OD for consecutive 5 days a week
reduces fluid retention.
 Anxiolytic agents are found to be helpful to women having
persistent anxiety. Alprazolam 0.25 mg, BID) is given during the
luteal phase of the cycle.
 Selective Serotonin Reuptake Inhibitors (SSRI) (eg
Fluoxetine 20mg) and Noradrenaline Reuptake Inhibitors
(SNRI) are found to be very effective.
Hormones:
o Oral contraceptive pills: The idea is to suppress ovulation and to

maintain an uniform hormonal milieu. The therapy is to be continued for
3–6 cycles.
o Progesterone is not effective in treating PMS.
o Spironolactone: It is a potassium sparing diuretic. It has anti-
mineralocorticoid and anti-androgenic effects. It is given in the luteal
phase (25–200 mg/day).
o Bromocriptine: 2.5 mg daily or twice daily may be helpful, at least to
relieve the breast complaints.
o Oophorectomy - primary PMS with recurrence of symptoms and
approaching to menopause, hysterectomy with bilateral oophorectomy
is a last resort
o Suppression of ovarian cycle
 Medical oopherectomy - GnRH agonist for 6 months
 Danazol 200 mg daily is to be adjusted so as to produce
amenorrhea
Menstrual Disorders: Abnormal Uterine Bleeding
Abnormal Uterine Bleeding
Any uterine bleeding outside the normal volume, duration, regularity or

frequency is considered abnormalnuterine bleeding (AUB).
Description of alteration in the normal pattern of menstrual flow
Forms;
Excessive flow
Prolonged flow
Intermenstrual bleeding
Types;
- hypermenorrhoea - metrorrhagia
- polymenorrhoea - amenorrhoea
- menometrorrhagia - menorrhagia
- oligomenorrhoea
1. MENORRHAGIA
(Syn : Hypermenorrhea)
Menorrhagia is defined as cyclic bleeding at normal intervals; the bleeding is either

excessive in amount (> 80 mL) or duration (>7 days) or both.
The term menotaxis is often used to denote prolonged bleeding.
Classification of menorrhagia
Menorrhagia can be classified as:
idiopathic, where no organic pathology can be found: also known as dysfunctional

uterine bleeding-(DUB).
secondary to an organic cause, such as fibroids.
Causes:
1. Organic:
a. Pelvic causes:
 Fibroid uterus
 Adenomyosis
 Pelvic endometriosis
 IUCD inutero
 Chronic tubo-ovarian mass
 Tubercular endometritis (early cases)
 Retroverted uterus—due to congestion
 Granulosa cell tumor of the ovary
b. Systemic:
Liver dysfunction—failure to conjugate and thereby inactivates the estrogens.
 Congestive cardiac failure.

 Severe hypertension
c. Endocrinal
 Hypothyroidism.
 Hyperthyroidism.
d. Hematological
 Idiopathic thrombocytopenic purpura.

 Leukemia. von Willebrand’s disease.
 Platelet deficiency.
2. Functional
 Due to disturbed hypothalamo-pituitary-ovarianendometrial axis.
COMMON CAUSES OF MENORRHAGIA
 Dysfunctional uterine bleeding

 Fibroid uterus
 Adenomyosis
 Chronic tubo-ovarian mass
Diagnosis & treatment
 number of towels and tampons used per day is useful

 irregular, intermenstrual or postcoital bleeding, a sudden change in symptoms,
dyspareunia, pelvic pain or premenstrual pain, and excessive bleeding from other
sites or in other situations (e.g. after tooth extraction).
 Long duration of flow, passage of big clots, use of increased number of thick sanitary
pads, pallor, and low level of hemoglobin give an idea about the correct diagnosis
and magnitude of menorrhagia.
Treatment: The definitive treatment is appropriate to the cause for menorrhagia.
Some Definitive Treatment
Drugs that are compatible with ongoing attempts at conception
 Mefenamic acid and other non-steroidal, anti-inflammatory drugs (NSAIDs)

 Tranexamic acid
 Drugs that are incompatible with ongoing attempts at conception but not licensed for
use as contraceptives
 Danazol
 used as contraceptives that are effective in the treatment of menorrhagia
 Combined oral contraceptive pill
 levonorgestrel intrauterine system.
 Second-line drugs with few advantages over the forgoing, and whose side effects
limit long-term use
 Danazol
 Gestrinone
 Gonadotrophin-releasing hormone analogues
 Medical and surgical treatments that are not effective in the
treatment of menorrhagia
 Ethamsylate
 Luteal phase progestogens
 Uterine curettage
Surgical treatments for menorrhagia
 ablation of the endometrial lining of the uterus to sufficient depth prevents

regeneration of the endometrium.
 Hysterectomy
2. POLYMENORRHEA (SYN : EPIMENORRHEA)
 is defined as cyclic bleeding where the cycle is reduced to an arbitrary limit of less
than 21 days and remains constant at that frequency.
 If the frequent cycle is associated with excessive and or prolonged bleeding, it is
called epimenorrhagia.
Causes & treatment
Dysfunctional:
 It is seen predominantly during adolescence, preceding menopause and following

delivery and abortion.
 Hyperstimulation of the ovary by the pituitary hormones may be the responsible
factor.
Ovarian hyperemia as in PID or ovarian endometriosis.
Treatment:
Persistent dysfunctional type is to be treated by hormone as in DUB
3. METRORRHAGIA
 is defined as irregular, acyclic bleeding from the uterus.

 Amount of bleeding is variable.
 While metrorrhagia strictly concerns uterine bleeding but in clinical practice,
the bleeding from any part of the genital tract is included under the heading.
 Then again, irregular bleeding in the form of contact bleeding
or intermenstrual bleeding in an otherwise normal cycle is also included in
metrorrhagia.
 In fact, it is mostly related to surface lesion in the uterus.
Menometrorrhagia is the term applied when the bleeding is so irregular and

excessive that the menses (periods) cannot be identified at all.
CAUSES OF ACYCLIC BLEEDING
 DUB—usually during adolescence, following childbirth and abortion and

preceding menopause
 Submucous fibroid
 Uterine polyp
 Carcinoma cervix and endometrial carcinoma
CAUSES OF CONTACT BLEEDING
 Carcinoma cervix
 Mucos polyp of cervix
 Vascular ectopy of the cervix especially during pregnancy, pill use cervix
 Infections—chlamydial or tubercular cervicitis
 Cervical endometriosis
CAUSES OF INTERMENSTRUAL BLEEDING
 Apart from the causes of contact bleeding, other causes are:

 Urethral caruncle
 Ovular bleeding
 Breakthrough bleeding in pill use
 IUCD in utero
Treatment of metrorhagia
Treatment is directed to the underlying pathology.
Malignancy is to be excluded prior to any definitive treatmentecubitus ulcer
4. OLIGOMENORRHEA
 Definition: Menstrual bleeding occurring more than 35 days apart and
which remains constant at that frequency is called oligomenorrhea.
COMMON CAUSES OF OLIGOMENORRHEA
 Age-related—during adolescence and preceeding menopause

 Weight-related—obesity
 Stress and exercise related
 Endocrine disorders—PCOS (commonest), hyperprolactinemia,
hyperthyroidism
 Androgen producing tumors—ovarian, adrenal
 Tubercular endometritis—late cases
 Drugs:
 Phenothiazines
 Cimetidine
 Methyldopa
5. AMENORRHOEA
 absence of menstruation.
 It may be classified as either primary or secondary.
 There are, physiological situations in which amenorrhoea is normal, namely:
 pregnancy,
 lactation and
 prior to the onset of puberty.
Classification of amenorrhoea
 Primary amenorrhoea: condition in which girls fail to develop secondary

sexual characteristics by 14 years of age or fail to menstruate by 16 years of
age.
 Secondary amenorrhoea: describes the cessation of menstruation for more
than 6 months in a normal female of reproductive age that is not due to
pregnancy.
Causes of amenorrhoea
 Reproductive outflow tract disorders

 Asherman 's syndrome
 Mullerian agenesis
 Transverse vaginal septum
 Imperforate hymen
 Testicular feminization syndrome
 Ovarian disorders
 Anovulation, e.g. polycystic ovarian synd rome (peaS)
 Gonadal dysgenesis, e.g. Turner's syndrome
 Premature ovarian failure
 Resistant ovary syndrome
 Pituitary disorders
 Adenomas such as prolactinoma
 Pituitary necrosis, e.g. Sheehan's syndrome
 Hypothalamic malfunctions
 Resulting from excessive exercise
 Resulting from weight loss/anorexia nervosa
 Resulting from stress
 Craniopharyngioma
 Kallman 's syndrome
Diagnosis & treatment
 Detailed history and examination

 Investigations
 Initial hormone tests:
o Pregnancy test,
o Prolactin,
o Thyroid function,
o LH and FSH,
o Testosterone – androgen producing tumours
 Treat the cause.
6. HYPOMENORRHEA
Definition: When the menstrual bleeding is unduly scanty and lasts for less than 2
days, it is called hypomenorrhea.
Causes
 The causes may be:

 local (uterine synechiae or endometrial tuberculosis),
 endocrinal (use of oral contraceptives, thyroid dysfunction, and
premenopausal period), or systemic (malnutrition).
7. DYSFUNCTIONAL UTERINE BLEEDING (DUB)
 DUB is defined as a state of abnormal uterine bleeding without any clinically

detectable organic, systemic, and iatrogenic cause (Pelvic pathology, e.g.
tumor, inflammation or pregnancy is excluded).
 NB: Heavy menstrual bleeding (HMB) is defined as a bleeding that
interferes with woman's physical, emotional, social and maternal quality of life.
DUB
 The bleeding may be abnormal in frequency, amount, or duration or

combination of any three.
 As the diagnosis is based with the exclusion of ‘organic
lesion’, Currently DUB is defined as a state of abnormal uterine bleeding
following anovulation due to dysfunction of hypothalamo-pituitary-ovarian axis
(endocrine origin).
Pathophysiology
 The endometrial abnormalities may be primary or secondary

to incoordination in the hypothalamopituitary- ovarian axis.
 It is thus more prevalent in extremes of reproductive period—adolescence
and premenopause or following childbirth and abortion.
 The abnormal bleeding may be associated with or without ovulation and
accordingly grouped into :
 Ovular bleeding
 Anovular bleeding
OVULAR BLEEDING
 Polymenorrhea or polymenorrhagia:
 usually occurs following childbirth and abortion, during adolescence and
premenopausal period, and in pelvic inflammatory disease.
 The follicular development is speeded up with resulting shortening of the
follicular phase.
 This is probably due to hyperstimulation of the follicular growth by FSH.
 Rarely, the luteal phase may be shortened due to premature lysis of the
corpus luteum.
 Sometimes, it is related to stress induced stimulation.

 Oligomenorrhea:
 Primary ovular oligomenorrhea is rare.
 Common in adolescence and premenopause.
 The disturbance may be due to ovarian unresponsiveness to FSH or
secondary to pituitary dysfunction.
 There is undue prolongation of the proliferative phase with normal secretory
phase.
ANOVULAR BLEEDING
 Menorrhagia
 Anovular bleeding is usually excessive.
 In the absence of growth limiting progesterone due to anovulation, the
endometrial growth is under the influence of estrogen throughout the cycle.
 There is inadequate structural stromal support and the endometrium remains
fragile.
 Thus, with the withdrawal of estrogen due to negative feedback action of FSH,
the endometrial shedding continues for a longer period in asynchronous
sequences because of lack of compactness

 Cystic glandular hyperplasia
 This type of abnormal bleeding is usually met in premenopausal women
 There is slow increase in secretion of estrogen but no negative feedback
inhibition of FSH.
 The net effect is gradual rise in the level of estrogen with concomittant phase
of amenorrhea for about 6–8 weeks.
 As there is no ovulation, the endometrium is under the influence of estrogen
without being opposed by growth limiting progesterone for a prolonged period.
diagnosis
 History, physical examination & Investigations aim at:

 To confirm the menstrual abnormality as stated by the patient.
 To exclude the systemic, iatrogenic, and ‘organic’ pelvic pathology.
 To identify the possible etiology of DUB.
 To work out the definite therapy protocol.
MANAGEMENT
 Because of diverse etiopathology of DUB in different phases of woman’s life,

the management protocols have been grouped accordingly.
o Pubertal and adolescent menorrhagia < 20 years.
o Reproductive period (20–40 years).
o Premenopausal (> 40 years).
o Postmenopausal.
Management
General
 Rest is advised during bleeding phase.

 Assurance and sympathetic handling are helpful particularly in adolescents.
 Anemia should be corrected energetically by diet, hematinics, and even by
blood transfusion.
 Clinically evident systemic or endocrinal abnormalities should be investigated
and treated accordingly.
MEDICAL
 potent orally active progestins, are the mainstay in the management of

DUB in all age groups.
 Mechanism of antiestrogenic action of progestins are:
o • It stimulates the enzyme (17-β-hydroxy steroid
dehydrogenase) that converts estradiol to estrone (less potent).
o • Inhibits induction of estrogen receptor.
o • It has antimitotic effect on the endometrium.
 While isolated progestins therapy is highly effective in anovular DUB, in ovular
DUB combined preparations of progestogen and estrogen (combined oral
pills) are effective.
 To stop bleeding and regulate the cycle : Norethisterone preparations (5
mg tab) are used thrice daily till bleeding stops, which it usually does by 3–7
days.
Cyclic Therapy:
 In ovular bleeding, Any low dose combined oral pills are effective when

given 5th to 25th day of cycle for 3 consecutive cycles. It causes endometrial
atrophy. It is more effective compared to progesterone therapy as it suppress
the hypothalamopituitary axis more effectively. Normal menstruation is
expected to resume with restoration of normally functionating pituitary–
ovarian-endometrial axis
 In anovular bleeding: Cyclic progestogen preparation of
medroxyprogesterone acetate (MPA) 10 mg or norethisterone 5 mg is used
from 5th to 25th day of cycle for 3 cycles
NON-HORMONAL MANAGEMENT
 Anti-fibrinolytic agents - Tranexamic acid

 Prostaglandin synthetase inhibitors: eg Mefenamic acid 150-600mg is much
effective in women aged more than 35 years and in cases of ovulatory DUB
during bleeding phase.
 Desmopressin: It is a synthetic analogue of arginine-vasopressin.
indicated in von Willebrand’s disease and factor VIII deficiency. It is given IV
(0.3 μg/kg) or intranasally.
SURGICAL MANAGEMENT OF DUB
 Uterine curettage
 Endometrial ablation/resection
 Hysterectomy
8. POLYCYSTIC OVARIAN SYNDROME
 is a syndrome of ovarian dysfunction along with the cardinal features of

hyperandrogenism and polycystic ovary morphology.
 PCOS remains a syndrome, and as such no single diagnostic criterion (such
as hyperandrogenism or polycystic ovary) is sufficient for clinical diagnosis.
 Its clinical manifestations may include:
 menstrual irregularities,
 signs of androgen excess
 obesity.
 Insulin resistance
 elevated serum LH levels.
 PCOS is associated with an increased risk of type 2
diabetes and cardiovascular events.
Prevalence:
 affects around 5-10% of women of reproductive age.

 The prevalence of polycystic ovaries seen on ultrasound is much higher -
around 25%.
Aetiology:
 remains unclear but is self-perpetuating once starts.

 Women with this syndrome have increased ovarian androgen due partly to
disordered ovarian cytochrome P450 activity and partly to increased LH
stimulation.
 Additionally, increasing evidence suggests a role for (peripheral) insulin
resistance in the pathophysiology, with the resulting hyperinsulinaemia also
promoting ovarian androgen production.
Clinical features
 Oligomenorrhoea/amenorrhoea: this occurs in up to 65-75% and is

predominantly related to chronic anovulation.
 Hirsutism: this occurs in 30-70%.
 Subfertility: up to 75% of women with PCOS who try to conceive have
difficulty doing so.
 Obesity: at least 40% are clinically obese.
 Recurrent miscarriage: is seen in 50-60% of women with more than three
early pregnancy losses.
 Acanthosis nigricans: areas of increased skin pigmentation that are velvety
in texture and occur in the axillae and other flexures occur in around 2% of
women with PCOS.
Diagnosis
 Elevated testosterone levels.= testosterone & androstenedione

 Decreased sex hormone binding globulin (SHBG) levels.
 Elevated LH levels.
 • Elevated LH:FSH ratio. Typically LH:FSH > 2:3.1
 Increased fasting insulin levels.
 Free testosterone is higher than normal, since SHBG levels are low.
Testosterone levels of > 5 nmol/L should prompt a search for an
androgensecreting tumour.
 Transvaginal U/S:
 ≥ 10 peripheral cysts btn 2-8 mm diameter (‘string of pearls’
sign)
 Increased ovarian stromal volume to > 8cm3
Management of PCOS
Aim of Rx depends on main complaint
 Weight loss
 Cyclic progestagens or limited use of COC (menstrual disturbance)
 Anti-androgens; cyproterone acetate, spironolactone,
 cosmetic therapy (waxing, bleaching)
 Induction of ovulation with anti-oestrogens (clomiphene, tamoxifen) and
gonadotropins
 Anti-DM meds; metformin
 **Advise on high risk of dev’pt of type II DM, gestational DM, arterial disease
like HT (androgen), endometrial hyperplasia & CA**
Mnx of pcos
Oligomenorrhoea/amenorrhoea
 tend to be anovulatory, normal or high oestrogen levels.

 endometrium that develops under the influence of oestrogen eventually
becomes unsustainable and sheds.
 For these reasons, cyclical progesterone is often useful in the treatment
 Medroxyprogesterone acetate 10 mg daily for 10 days. The woman will
normally bleed a few days after progesterone treatment stops.
 metformin, increases insulin sensitivity, is partially effective in its treatment.
Hirsutism
 arises from the growth-promoting effects of androgen at the hair follicle.

 Some of these growth-promoting effects are irreversible, even when androgen
levels fall.
 However, lowering free androgen levels will slow the rate of hair growth,
which most patients see as a benefit.
 The possible treatment options include the following.
 Eflornithine cream, applied topically.
 Cyproterone acetate: an anti-androgen that competitively inhibits the
androgen receptor.
 GnRH analogues with low-dose HRT: this regime should be reserved for
women intolerant to other therapies, or for short-term treatment, since bone
loss is an inevitable side effect.
 Surgical treatments aimed at destroying the hair follicle, such as laser or
electrolysis
Subfertility
 may respond to treatment either with clomiphene or with gonadotrophin

therapy.
 there is some evidence that metformin may increase ovulation rates, either
alone or when used in combination with clomiphene.
 metformin has been shown to increase ovulation rates (and therefore
frequency of menses) by around once every 5 months.
ABNORMAL UTERINE BLEEDING (AUB) (FIGO, ACOG-2011)
 Any uterine bleeding outside the normal volume, duration, regularity or

frequency is considered abnormal uterine bleeding (AUB).
NORMAL MENSTRUATION
 Cycle interval =28 days (21–35 days)

 Menstrual flow = 4–5 days
 Menstrual blood loss = 35 mL (20–80 mL)
 Abnormal menstrual bleeding pattern have been traditionally expressed by
terms like menorrhagia, metrorrhagia, polymenorrhea, and oligomenorrhea
AUB
 In order to create an universally accepted nomenclature to describe abnormal

uterine bleeding, International Federation of Gynecology and Obstetrics
(FIGO) and American College of Obstetricians and Gynaecologists (ACOG)
introduced newer system of terminology to describe AUB.
 The newer classification system is known by the acronym PALM–COEIN
(FIGO–2011).
 It is used to classify the abnormal uterine bleeding on the basis of etiology:
 Polyp,
 Adenomyosis,
 Leiomyoma,
 Malignancy and hyperplasia,
 Coagulopathy,
 0vulatory dysfunction,
 Endometrial,
 Iatrogenic, and
 Not yet classified are the different etiological factors
expressed by one (or more) letters.
Etiopathology of AUB
Structural causes (PALM)
 Polyp
 Adenomyosis
 Leiomyoma
 Malignancy and hyperplasia
Nonstructural systemic causes (COEIN)
 Coagulopathy
 Ovulatory dysfunction
 Endometrial
 Iatrogenic
 Not yet identified
Diagnosis of Abnormal Uterine Bleeding
• Detailed history taking and physical examination
History: Age,patterns of abnormal uterine bleeding, severity, associated pain, family

history and use of medication
physical examination: Pallor, edema, neck glands, thyroid, and systemic

examination, and pelvic examination (per speculum, Pap smear, and bimanual
examination) are included
• Laboratory investigations: Complete hemogram, thyroid profile, pregnancy

test, coagulation profile.
• Imaging studies: Ultrasonography (Transvaginal), hysteroscopy
• Magnetic resonance imaging (MRI): second line procedure especially in

cases with adenomyosis.
E. Histological confirmation of pathology
POSTMENOPAUSAL BLEEDING
 Vaginal bleeding after the menopause.

 In women who are not taking HRT, any bleeding is abnormal.
 In women on combined cyclical HRT, bleeding in the progesterone free period
is normal.
 Unscheduled bleeding refers to bleeding at other times, and this is abnormal
and should be investigated.
AETIOLOGY OF PMB
 majority of women have atrophic vaginitis, whereby the vaginal epithelium

thins and breaks down in response to low oestrogen levels.
 This is a benign condition, which is relatively easily treated with topical
oestrogens.
 10% of women with PMB will be found to have endometrial cancer, the risk of
which is greater for those who are not currently taking HRT, and progressively
increases with increasing age.
Differential diagnosis OF PMB
 endometrial carcinoma
 endometrial hyperplasia
 endometrial polyps
 cervical malignancy
 atrophic vaginitis.
 Summary
 AUB
 •In order to create an universally accepted nomenclature to describe
abnormal uterine bleeding, International Federation of Gynecology and
Obstetrics (FIGO) and American College of Obstetricians and Gynaecologists
(ACOG) introduced newer system of terminology to describe AUB.
 •The newer classification system is known by the acronym PALM–COEIN
(FIGO–2011).
 •It is used to classify the abnormal uterine bleeding on the basis of etiology:
 –Polyp,
 –Adenomyosis,
 –Leiomyoma,
 –Malignancy and hyperplasia,
 –Coagulopathy,
 –0vulatory dysfunction,
 –Endometrial,
 –Iatrogenic, and
 –Not yet classified are the different etiological factors expressed by one (or
more) letters.
ENDOMETRIOSIS
DEFINITION
ENDOMETRIOSIS:
Abnormal growths of tissue histologically resembling the endometrium in
locations other than the uterine lining.
ADENOMYOSIS:
 n Presence of endometrial glands and stroma within the myometrium on hitological

examination.
 n Also called endometriosis interna
 n ENDOMETRIOSIS
 n It is a benign but it is locally invasive
 n disseminates widely.
 n Cyclic hormones stimulate growth
 n Does NOT Discriminate by Race
 n The prevalence is about 10 percent.
sites of endometriosis
 Abdominal
 Extra-abdominal:
 – The common sites are abdominal scar of hysterotomy, cesarean section,
tubectomy and myomectomy, umbilicus, episiotomy scar, vagina and cervix.
Commonest sites
 Ovary-50%. Pod, utero-sacral ligaments,posterior visceral surface of the

uterus,broad ligament, bowel,bladder&ureters.
 Rare - deep in the cervix,vaginal fornices,wounds contaminated with endometrial
tissue.
 Distant - out of the pelvis- lungs,brain&kidney.

 Risk factors
 Single/nulliparous
 Early menarche
 Non oral contraception
 Non smoker shorter cycle/longer duration of flow
PATHOGENESIS
 still remains unclear and is full of theories:

 1. Retrograde Menstruation (Sampson’s theory):
 – There is retrograde flow of menstrual blood through the uterine tubes.
Endometrial fragments get implanted in the peritoneal surface of the pelvic organs.
 2. Coelomic metaplasia (Meyer and Ivanoff):
 – Chronic irritation of the pelvic peritoneum by the menstrual blood may cause
coelomic metaplasia which results in endometriosis.
 3. Lymphatic Theory (Halban):
 – It may be possible for the normal endometrium to metastasize the pelvic lymph
nodes through the draining lymphatic channels
 4. Vascular Theory:
 – This is sound at least to explain endometriosis at distant sites such as lungs, arms
or thighs.
 5. others: Genetic and Immunological Factors, Direct Implantation, Environment
theory.
PATHOLOGY
 Endometrial lesions appear as red velvety implants on the peritoneal surface. Further
growth gives them a cystic, darkblue or black appearance. Lesions may grow to 5-10
mm surrounded by extensive adhesions. In the ovaries the cysts may enlarge to
several cm; endometriomas or ‘chocolate cysts’.
CLINICAL FEATURES
 The age is 30–45.

 Infertility,
 patients are mostly nulliparous
 25% have no symptom
 Dysmenorrhea (70%)
 Menorrhagia
 Dyspareunia
 Chronic Pelvic Pain
Other Symptoms
 n Urinary—frequency, dysuria, back pain or even hematuria

 n Sigmoid colon and rectum—painful defecation (dyschezia), diarrhea, constipation,
rectal bleeding or even melena
 n Chronic fatigue, perimenstrual symptoms (bowel, bladder)
 n Hemoptysis (rarely), catamenial chest pain
 n Surgical scars—cyclical pain and bleeding
Diagnosis
 confirm by laparoscopy\ laparotomy and biopsy for histology. (“Gold Standard)

 Inconclusive Ix:
 – CA-125 - moderate elevationin patients with severe endometriosis,
 – History & Pelvic Exam,
 – Imaging Studies
 Ultrasonography is not much helpful to the diagnosis.
 MRI & CT scan
Treatment: Overall Approach
Recognize Goals:
– Pain Management
– Preservation / Restoration of Fertility
Discuss with Patient:
– Disease may be Chronic and Not Curable
– Optimal Treatment Unproven or Nonexistent
TREATMENT
Depends on desire for future fertility, symptoms, disease stage and age of the
patient.
Minimal disease – observe on NSAIDS and prostaglandin inhibitors.
Moderate – pseudo pregnancy – ocps.
Severe disease – pseudomenopause – e.g.. Danazol, gnrh agonists - Buserelin ,

Goserelin, Leuprorelin .
Surgery – excision & adhesionolysis, For those with DFS – TAH + BSO,
Appendicectomy and excision of all lesions.
Pain Management: Medical Therapy
 NSAIDs
 OCPs (Continuous)
 Progestins
 Danazol
 GnRH-a
 GnRH-a + Add-Back Therapy
 Misc: Opoids, TCAs, SSRIs
Surgical Treatment
 (Laparoscopy / Laparotomy
 Excision / Fulgeration
 Resection of Endometrioma
 Lysis of Adhesions, Cul-de-sac Reconstruction
 Uterosacral Nerve Ablation
 Presacral Neurectomy
 Appendectomy
 Uterine Suspension
 Hysterectomy +/- BSO
PROGNOSIS
 Counseling after diagnosis and staging is vital for decision of management mode.
 May reccur even after definitive surgery
ADENOMYOSIS
 Adenomyosis is a condition where there is in-growth of the endometrium, both the

glandular and stromal components, directly into the myometrium.
 The cause of such in-growth is not known.
 It may be related to repeated childbirths, vigorous curettage or excess of estrogen
effect
 It is thought to be direct contamination of endometrial surface where isolate islands
have lost the connection with the surface endometrium from fibrosis or musculature.
CLINICAL FEATURES
 one-third remains asymptomatic
 Menorrhagia (70%) - unresponsive to hormonal therapy or uterine curettage
 Dysmenorrhea (30%)
 Pelvic pain
 Dyspareunia or frequency of urination
 Sub-Infertility & pregnancy loss:
 – abnormal function of the subendometrial myometrium,
 – retrograde myometrial contractions,
 – interference in sperm transport and blastocyst implantation and
 – abnormal endomerial immune respose and nitric oxide level
diagnosis
Ultrasound and Color Doppler (TVS) characteristics are:
 – Myometrium normally has three distinct zones of different echogenecity.

 – The inner layer is hypoechoic relative to the middle and outer layer.
 – This subendometrial halo is characteristic in adenomyosis.
 – Other features are:
 § heterogenous echogenecity,
 § hypoecoic myometrium with multiple small cysts in the myometrium
(honeycomb appearance),
 § increased vascularity within the myometrium
Magnetic Resonance Imaging (MRI)
MRI should be expected to be excellent in recognizing uterine masses like fibroids,

cysts, and adenomyomas if they reach 5 mm. or greater in size.
MRI may be able to lead us to expect adenomyosis if the myometrial thickness is

increased or the consistency of the myometrium is changed.

Hysterography
the presence of ill defined areas of contrast intravasation extending perpendicularly

from the uterine cavity into the myometrium is the most characteristic feature of
adenomyosis on hysterography.
Unfortunately, the sensitivity of this technique is too low for clinical practice.
n TREATMENT:
n The only definitive treatment for adenomyosis is total hysterectomy, with or

without ovarian conservation.
n Chemotherapy – ocps reduce pain and bleeding.
n DXT – destroys ovaries and reduces I.e. for those who cannot stand surgery.
n Prognosis – Hysterectomy is curative.
n Levonorgestrel–releasing-IUS is found to improve the menorrhagia and

dysmenorrhea.
n Danazol—loaded (300–400 mg) intrauterine device (IUD) is also found to improve

the symptoms of menorrhagia and dysmenorrhea.
n .
A good gynecologist may suspect adenomyosis based on the clinical factors, but the final
diagnosis usually has to wait until hysterectomy is performed.
Summary
ENDOMETRIOSIS:
Abnormal growths of tissue histologically resembling the endometrium in locations other

than the uterine lining
Diagnosis: confirm by laparoscopy\ laparotomy and biopsy for histology. (“Gold Standard)
Treatment: Depends on desire for future fertility, symptoms, disease stage and age of the
patient.
 Minimal disease – observe on NSAIDS and prostaglandin inhibitors.

 Moderate – pseudo pregnancy – ocps.
 Severe disease – pseudomenopause – e.g.. Danazol, gnrh agonists - Buserelin ,
Goserelin, Leuprorelin .
 Surgery – excision & adhesionolysis, For those with DFS – TAH + BSO,
Appendicectomy and excision of all lesions.
ADENOMYOSIS:
Presence of endometrial glands and stroma within the myometrium on hitological

examination.
Also called endometriosis interna
The only definitive treatment for adenomyosis is total hysterectomy, with or without ovarian
conservation
A good gynecologist may suspect adenomyosis based on the clinical factors, but the final
diagnosis usually has to wait until hysterectomy is performed.
Unit Five Content..
Topic 1: Fertilization and Implantation
FERTILIZATION
Fertilization is the process of fusion of the spermatozoon with the mature ovum. It
begins with sperm egg collision and ends with production of a mononucleated single
cell called the zygote. Its objectives are:
(1) To initiate the embryonic development of the egg and
(2) To restore the chromosome number of the species.
Almost always, fertilization occurs in the ampullary part of the uterine tube.
Process of Fertilization
After the male ejaculates semen into the vagina during intercourse, a few sperm are
transported within 5 to 10 minutes upward from the vagina and through the uterus
and fallopian tubes to the
ampullae of the fallopian tubes near the ovarian ends of the tubes. This transport of
the sperm is aided by contractions of the uterus and fallopian tubes stimulated by
prostaglandins in the male seminal fluid and also by oxytocin released from the
posterior pituitary gland of the female during her orgasm. Of the almost half a billion
sperm deposited in the vagina, a few thousand succeed in
reaching each ampulla.
· Complete dissolution of the cells of the corona radiata occurs by the chemical
action of the hyaluronidase liberated from the acrosomal cap of the hundreds of
sperm present at the site.
· Penetration of the zona pellucida is facilitated by the release of hyaluronidase

from the acrosomal cap. More than one sperm may penetrate the zona pellucida.
· Out of the many sperms, one touches the oolemma. Soon after the sperm
fusion, penetration of other sperm is prevented by zona reaction (hardening) and
oolemma block. This is due to release of cortical granules by exocytosis from the
oocyte.
· Completion of the second meiotic division of the oocyte immediately follows,

each containing haploid number of chromosomes (23, X). The bigger one is called
the female pronucleus and the smaller one is called second polar body which is
pushed to the perivitelline space.
· In the human, both the head and tail of the spermatozoon enter the cytoplasm
of the oocyte but the plasma membrane is left behind on the oocyte surface. Head
and the neck of the spermatozoon become male pronucleus containing haploid
number of chromosomes (23, X) or (23, Y).
· The male and the female pronuclei unite at the center with restoration of the
diploid number of chromosomes (46) which is constant for the species. The zygote,
thus formed, contains both the paternal and maternal genetic materials. In some
instances, an antigen called fertilizin present on the cortex and its coat of the ovum,
reacts with the antibody called antifertilizin liberated at the plasma membrane of the
sperm head. Thus the union between the two gametes may be an immunological
reaction (chemotaxis).
IMPLANTATION (Nidation)
Implantation occurs in the endometrium of the anterior or posterior wall of the body
near the fundus on the 6th day after fertilization which corresponds to the 20th day of
a regular menstrual cycle. Implantation occurs through four stages e.g. apposition,
adhesion, penetration and invasion.
APPOSITION: Occurs through pinopod formation. Pinopods are long finger like

projections (microvilli) from the endometrial cell surface. These pinopods absorb the
endometrial fluid which is secreted by the endometrial gland cells. This fluid, rich in
glycogen and mucin provides nutrition to the blastocyst initially. Unless this fluid is
absorbed, adhesion phase cannot occur.
ADHESION of blastocyst to the endometrium occurs through the adhesion

molecules like integrin, selectin and cadherin (glycoproteins).
PENETRATION AND INVASION: Actual penetration and invasion occur through the

stromal cells in between the glands and is facilitated by the histolytic action of the
blastocyst. With increasing lysis of the stromal cells, the blastocyst is burrowed more
and more inside the stratum compactum of the decidua. Vacuoles appear in the
advancing syncytium which fuse to form large lacunae. These are more evident at
the embryonic pole. Concurrently, the syncytial cells penetrate deeper into the
stroma and erode the endothelium of the maternal capillaries. The syncytium by
penetrating the vessels, not only becomes continuous with the endothelial lining but
permits the maternal blood to enter into the lacunar system. Ultimately erosion of few
maternal arteries with formation of blood space (lacunae) occurs. Nutrition is now
obtained by aerobic metabolic pathway from the maternal blood. Further penetration
is stopped probably by the maternal immunological factor and the original point of
entry is sealed by fibrin clot and later by epithelium. The process is completed by
10th or 11th day which corresponds to D 24-25 from LMP. This type of deeper
penetration of the human blastocyst is called interstitial implantation and the
blastocyst is covered on all sides by the endometrium (decidua). Occasionally, there
may be increased blood flow into the lacunar spaces at the abembryonic pole. This
results in disruption of the lacunae and extravasation of blood into the endometrial
cavity. This corresponds approximately to 13th day after fertilization (at about the
expected day of the following period). This may produce confusion in determination
of the expected date of delivery.
Normal Pregnancy and the Fetus
Normal Pregnancy
Pregnancy (gestation) is the physiologic process of a developing fetus within the

maternal body.
Several terms are used to define the developmental stage of human conception and
the duration of pregnancy. For obstetric purposes, the gestational age or menstrual
age is the time elapsed since the first day of the last normal menstrual period
(LNMP), which actually precedes the time of oocyte fertilization. The gestational age
is expressed in completed weeks. The start of the gestation (based on the LNMP) is
usually 2 weeks before ovulation, assuming a 28-day regular menstrual cycle. The
developmental or fetal age is the age of the conception calculated from the time of
implantation, which is 4 to 6 days after ovulation is completed. The menstrual
gestational age of pregnancy is calculated at 280 days or 40 completed weeks. The
estimated due date (EDD) may be estimated by adding 7 days to the first day of the
last menstrual period and subtracting 3 months plus 1 year (Naegele’s rule).
The period of gestation can be divided into units consisting of 3 calendar months
each or 3 trimesters.
Three periods are distinguished in the prenatal development of the fetus. (1) Ovular
period or germinal period—which lasts for first 2 weeks following ovulation. In spite
of the fact that the ovum is fertilized, it is still designated as ovum. (2) Embryonic
period—begins at 3rd week following ovulation and extends up to 10 weeks of
gestation (8 weeks post conception). The crown-rump length (CRL) of the embryo is
4 mm. (3) Fetal period begins after 8th week following conception and ends in
delivery. The chronology in the fetal period is henceforth expressed in terms of
menstrual age and not in embryonic age. The principal events of embryonic and
fetal development are shown in the table below:
THE FETUS
GROWTH OF THE FETUS
Normal fetal growth is characterized by cellular hyperplasia followed by hyperplasia

and hypertrophy and lastly by hypertrophy alone. The fetal growth increases linearly
until 37th week. It is controlled by genetic factor in the first half and by environmental
factors in the second half of pregnancy. The important physiological factors
are: Race (European babies are heavier than Indians); Sex (male baby weighs >
female); Parental height and weight (tall and heavier mother have heavier babies);
Birth order (weight rises from first to second pregnancy) and Socioeconomic factors
(heavier babies in social class I and II). Fetal growth is predominantly controlled by
IGF-1, insulin and other growth factors. Growth hormone is essential for postnatal
growth. At term, the average fetal weight in India varies from 2.5 kg to 3.5 kg.
FETAL NUTRITION
There are three stages of fetal nutrition following fertilization:
(1) Absorption: In the early postfertilization period, nutrition is stored in deutoplasm

within cytoplasm and the very little extra nutrition needed is supplied from the tubal
and uterine secretion.
(2) Histotrophic transfer: Following nidation and before the establishment of
uteroplacental circulation, nutrition is derived from eroded decidua by diffusion and
later on from the stagnant maternal blood in the trophoblastic lacunae.
(3) Hematotrophic: With the establishment of the fetal circulation, nutrition is

obtained by active and passive transfer from the 3rd week onwards.
The fetus is a separated physiological entity and it takes what it needs from the
mother even at the cost of reducing her resources. While all the nutrients are
reaching the fetus throughout the intrauterine period, the demand is not squarely
distributed. Two-thirds of the total calcium, three-fifths of the total proteins and
four-fifths of the total iron are drained from the mother during the last 3
months. Thus, in preterm births, the store of the essential nutrients to the fetus is
much low. The excess iron reserve is to compensate for the low supply of iron in
breast milk which is the source of nutrients following birth.
THE FETAL CIRCULATION
The umbilical vein carrying the oxygenated blood (80% saturated) from the
placenta, enters the fetus at the umbilicus and runs along the free margin of the
falciform ligament of the liver. In the liver, it gives off branches to the left lobe of the
liver and receives the deoxygenated blood from the portal vein. The greater portion
of the oxygenated blood, mixed with some portal venous blood, short circuits the
liver through the ductus venosus to enter the inferior vena cava (IVC) and thence to
right atrium of the heart. The O2 content of this mixed blood is thus reduced.
Although both the ductus venosus and hepatic portal/fetal trunk bloods enter the
right atrium through the IVC, there is little mixing. The terminal part of the IVC
receives blood from the right hepatic vein.
In the right atrium, most of the well oxygenated (75%) ductus venosus blood is
preferentially directed into the foramen ovale by the valve of the inferior vena cava
and crista dividens and passes into the left atrium. Here it is mixed with small
amount of venous blood returning from the lungs through the pulmonary veins. This
left atrial blood is passed on through the mitral opening into the left ventricle.
Remaining lesser amount of blood (25%), after reaching the right atrium via the
superior and inferior vena cava (carrying the venous blood from the cephalic and
caudal parts of the fetus respectively) passes through the tricuspid opening into the
right ventricle.
During ventricular systole, the left ventricular blood is pumped into the ascending
and arch of aorta and distributed by their branches to the heart, head, neck, brain
and arms. The right ventricular blood with low oxygen content is discharged into the
pulmonary trunk. Since the resistance in the pulmonary arteries during fetal life is
very high, the main portion of the blood passes directly through the ductus
arteriosus into the descending aorta bypassing the lungs where it mixes with the
blood from the proximal aorta. 70% of the cardiac output (60% from right and 10%
from left ventricle) is carried by the ductus arteriosus to the descending aorta. About
40% of the combined output goes to the placenta through the umbilical arteries. The
deoxygenated blood leaves the body by way of two umbilical arteries to reach
the placenta where it is oxygenated and gets ready for recirculation. The mean
cardiac output is comparatively high in fetus and is estimated to be 350
mL/kg/min.
Common Pregnancy Complaints and Questions
First Trimester
What are the first symptoms of pregnancy?

Missing a period is usually the first signal of a new pregnancy, although women with
irregular periods may not initially recognize a missed period as pregnancy. During
this time, many women experience a need to urinate frequently, extreme fatigue,
nausea and/or vomiting, and increased breast tenderness. All of these symptoms
can be normal. Most over-the-counter pregnancy tests are sensitive 9-12 days after
conception, and they are readily available at most drug stores. Performing these
tests early helps to allay confusion and guesswork. A serum pregnancy test
(performed in a provider's office or laboratory facility) can detect pregnancy 8-11
days after conception.
How long after conception does the fertilized egg implant?
The fertilized conceptus enters the uterus as a 2- to 8-cell embryo and freely floats in
the endometrial cavity about 90-150 hours, roughly 4-7 days after conception. Most
embryos implant by the morula stage, when the embryo consists of many cells. This
happens, on average, 6 days after conception. However, there is great variance in
the time of implantation. It can occur on days 16-30 of the menstrual cycle. The new
embryo then induces the lining changes of the endometrium, which is called
decidualization. It then rapidly begins to develop the physiologic changes that
establish maternal-placental exchange. Prior to this time, medications ingested by
the mother typically do not affect a pregnancy.
Is cramping during pregnancy normal?
Early in pregnancy, uterine cramping can indicate normal changes of pregnancy

initiated by hormonal changes; later in pregnancy, it can indicate a growing uterus.
Cramping that is different from previous pregnancies, worsening cramping, or
cramping associated with any vaginal bleeding may be a sign of ectopic
pregnancy, threatened abortion, or missed abortion.
Other physical effects that are normal during pregnancy, and not necessarily signs of
disease, include nausea, vomiting, increase in abdominal girth, changes in bowel
habits, increased urinary frequency, palpitations or more rapid heartbeat, upheaving
of the chest (particularly with breathing), heart murmurs, swelling of the ankles, and
shortness of breath.
Why do pregnant women feel tired?
Fatigue in early pregnancy is very normal. Many changes are occurring as the new
pregnancy develops, and women experience this as fatigue and an increased need
for sleep. Lower blood pressure level, lower blood sugar levels, hormonal changes
due to the soporific effects of progesterone, metabolic changes, and the physiologic
anemia of pregnancy all contribute to fatigue. Women should check with their health
care provider to determine if an additional work up, prenatal vitamin changes, and/or
supplemental iron would be beneficial.
Second Trimester
When do the postural changes of pregnancy occur?

Women experience a progressive increase in the anterior convex shape of the
lumbar spine during pregnancy. This change, termed lordosis, helps keep the center
of gravity stable and over the legs as the uterus enlarges. Late in pregnancy, aching,
weakness, and numbness of the arms may occur secondary to compensatory
anterior positioning of the neck and hunching of the shoulders in positional response
to exaggerated lordosis. These positional responses put traction on the ulnar and
median nerves, resulting in the previously mentioned symptoms.
In pregnancy, relaxin is secreted by the corpus luteum, the placenta, and part of the
decidual lining of the uterus. It is thought to cause remodeling of the connective
tissue of the reproductive tract and especially induce biochemical changes of the
cervix.
When is fetal movement usually felt?
Most women feel the beginnings of fetal movement before 20 weeks' gestation. In a
first pregnancy, this can occur around 18 weeks' gestation, and in following
pregnancies it can occur as early as 15-16 weeks' gestation. Early fetal movement is
felt most commonly when the woman is sitting or lying quietly and concentrating on
her body. It is usually described as a tickle or feathery feeling below the umbilical
area. The point at which a woman feels the baby move is termed quickening.
Placental location can impact the timing of quickening. An anterior placenta can
"cushion" against fetal movement and delay maternal detection of fetal movements.
As the fetus grows larger, the fetal movement feelings become stronger, regular, and
easier to detect. While there is no absolute number that indicates fetal well-being,
typical guidance may include that fetuses should move approximately 4 times an
hour as they get larger, and some clinicians advise patients to count fetal
movements to follow fetal well-being.
What kind of breast changes are normal during pregnancy?
Pregnancy-related breast changes include growth and enlargement, tenderness,

darkening of the nipples, and darkened veins due to increased blood flow. In
addition, small raised bumps (Montgomery tubercles) appear around the areola in
mid-pregnancy.
Third Trimester
How much does the uterus grow during pregnancy?
The uterus grows from an organ that weighs 70 g with a cavity space of about 1 mL
to an organ that weighs more than 1000 g that can accumulate a fluid area of almost
20 L. The shape also evolves during pregnancy from the original pearlike shape to a
more round form, and it is almost a sphere by the early third trimester. By full term,
the uterus becomes ovoid. The uterus is completely palpable in the abdomen (not
just by pelvic examination) at about 12-14 weeks' gestation. After 20 weeks'
gestation, most women begin to appear pregnant upon visual examination.
Is it normal to secrete milk from the breast prior to delivery?

Galactorrhea (milk secretion from the nipple) is the product of the combined effects
of prolactin, glucocorticoids, progesterone, and human placental lactogen.
Galactorrhea is not uncommon in the first trimester, although it usually does not
occur until milk let-down soon after delivery. At that time, the high levels of
progesterone, which block milk excretion, drop with the delivery of the placenta. In
mid-pregnancy a woman reaches lactogenesis stage I and she is able to secrete
colostrum.
Early galactorrhea does not mean that a woman will produce less milk after delivery.
Some women notice secretions beginning before the fifth month of pregnancy. Many
women find they spontaneously leak or express some fluid by the ninth month.
Early milk secretion, known as colostrum, is watery and pale. Colostrum has more
protein and lower fat levels than mature milk.
Lactogenesis stages II and III occur postpartum and form more mature milk.
Nutrition in Pregnancy
What are the most common dietary complaints during pregnancy?
During early pregnancy, most women experience an increased appetite, with extra
caloric needs of approximately 300 kcal/d. Stomach motility decreases, probably due
to decreased production of motilin. A decreased incidence of peptic ulcer disease is
due to a reduction in gastric acid secretion. Prolonged transit times through the colon
are also reported, with transit from the stomach to the cecum occurring in about 58
hours instead of 52 hours.
Some women have nonfood cravings, known as pica.
Women who experience nausea or hyperemesis may develop ptyalism (spitting).

Reported fluid losses of 1-2 L/d can occur in these women.
Should certain foods be avoided during pregnancy?
Pregnant women are at increased risk of bacterial food poisoning. For the safety of
both mother and fetus, it is important to take steps to prevent foodborne illnesses,
including the following:
 Properly cook food to kill bacteria. Use a meat thermometer to determine the
appropriate temperature, although cooking until well done is safe for most
meat. Ground beef should be cooked to at least 160°F, roasts and steaks to
145°F, and whole poultry to 180°F.
 Cook eggs until they have a firm yolk and are white. Eggnog and hollandaise
sauce have raw or partially cooked eggs and are not considered safe.
 Eat liver in moderation. Liver can contain extremely high levels of vitamin A.
 Avoid products containing unpasteurized milk, including soft cheeses like brie,
feta, and blue cheese. Also avoid unpasteurized juice.
 Carefully wash all fruits and vegetables to eliminate harmful bacteria. Avoid
raw sprouts altogether.
 Limit caffeine intake. Caffeine crosses the placenta and can affect fetal heart
rate. Some clinicians recommend limiting caffeine to less than 200 mg/day
(about 2 cups of coffee).
Can women safely eat fish while pregnant?
The American College of Obstetricians and Gynecologists (ACOG) issued a warning

regarding eating fish in response to the US FDA's consumer advisory about the
dangers of eating fish for nursing mothers and women who are or who may become
pregnant. The fish themselves are not harmful, but extensive fish consumption
increases exposure to the naturally occurring compound methylmercury, levels of
which have been increasing in the waters because of industrial pollution. Mercury is
very toxic and can cause danger to the fetus and to the newborn nursing infant.
Mercury exposure can actually occur via inhalation and/or skin absorption, and all
fish contain trace amounts. However, longer-lived and larger fish, such as shark,
swordfish, king mackerel, and tilefish, have increased mercury levels and cause the
most concern for consumption by pregnant women.
Other Questions Related to Pregnancy
What is the recommended weight gain in pregnancy?
Important variables to consider regarding weight gain recommendations include the

presence of twin or triplet pregnancies, maternal age, and maternal prepregnancy
weight. These variables can add to the burden of chronic disease for the mother and
baby; excessive weight gain is associated with an increased risk for gestational
diabetes, pregnancy-associated hypertension, and delivery of large-for-gestational-
age (LGA) infants.
Guidelines for weight gain during pregnancy* are as follows:
 Underweight women (BMI < 18.5) should gain 12.5-18 kilograms.

 Normal-weight women (BMI, 18.5-24.9) should gain 11-16 kilograms.
 Overweight women (BMI, 25-29.9) should gain 6.8-11 kilograms.
 Obese women (BMI, 30 or higher) should gain 5-9 kilograms.
*Weight gain guidelines are for singleton pregnancy; weight gain should be higher for
multiple pregnancies but the ideal amounts are unknown.
Clinicians are urged to supplement these guidelines with individualized counseling

about diet and exercise, and preconception counseling should emphasize the
importance of conceiving when the mother is at a normal body mass index (BMI). To
help mothers attain these goals, dietary, lifestyle, and exercise interventions have
been shown to be safe and effective at reducing excessive weight gain in pregnancy
Do older fathers have an increased risk of fathering children with birth

defects?
No medical information exists to support the hypothesis that increased paternal age
causes increased numerical chromosomal abnormalities in the manner that
increased maternal age does. However, as males age, structural spermatozoa
abnormalities increase, and affected sperm usually cannot fertilize eggs.
The literature suggests a 0.3%-0.5% risk of autosomal dominant disease in offspring

of fathers aged 40 years or older. Autosomal dominant disorders
include neurofibromatosis, Marfan syndrome, achondroplasia, and polycystic kidney
disease.
Should women wear seatbelts during pregnancy?
Seatbelts should absolutely be worn during pregnancy. Trauma to the mother is

more devastating to the child than any potential entrapment of the pregnant
abdomen in the seatbelt. The seatbelt should be placed low, across the hip bones
and under the pregnant abdomen. The shoulder strap should be placed to the side of
the abdomen, between the breasts, and over the midportion of the clavicle. No
information indicates that air bags are unsafe during pregnancy. Pregnant women
should try to keep their abdomen 10 inches from the airbag.
Can pregnant women go to the dentist?
Dental care during pregnancy is an important part of overall healthcare. During

pregnancy, the gums naturally become more edematous and may bleed after
brushing. Epulis gravidarum, a type of gingivitis with violaceous pedunculated
lesions, can occur. If treatment of cavities, surgery, or infection care is required, be
sure the dentist is aware of the pregnancy. Most antibiotics and local anesthetics are
safe to use during pregnancy. Radiographs can be obtained with abdominal
shielding but are best avoided during pregnancy because a small, but statistically
significant, increase in childhood malignancies exists in children exposed to in-utero
radiographic irradiation.
Why is heartburn more common during pregnancy?
Stomach emptying was thought to be retarded during pregnancy, but hormonal

influences of increased progesterone and/or decreased levels of motilin may be
more responsible for pyrosis (heartburn) than the actual mechanical obstruction in
the third trimester. Some studies have also shown decreased lower esophageal
sphincter tone, which can lead to an excess of gastric acid in the esophagus.
Why is back pain prevalent during pregnancy and can it be treated?
Half of women report having back pain at some point during pregnancy. The pain
can be lumbar or sacroiliac. The pain may also be present only at night. Back pain is
thought to be due to multiple factors, which include shifting of the center of gravity
caused by the enlarging uterus, increased joint laxity due to an increase in relaxin,
stretching of the ligaments (which are pain-sensitive structures), and pregnancy-
related circulatory changes.
Treatment is heat and ice, acetaminophen, massage, proper posturing, good support
shoes, and a good exercise program for strength and conditioning. Pregnant women
may also relieve back pain by placing one foot on a stool when standing for long
periods of time and placing a pillow between the legs when lying down.
Is sexual intercourse safe during pregnancy?
Research indicates that sexual intercourse is safe in the absence of ruptured

membranes, bleeding, or placenta previa, but pregnant women engage in sex less
often as their pregnancy progresses. ACOG states that sexual activity during
pregnancy is safe for most women right up until labor, unless there is a specific
contraindication.
ACOG specifically cautions that a woman should limit or avoid sex if she has a
history of preterm labor or birth, more than one miscarriage, placenta previa,
infection, bleeding, and/or breaking of the amniotic sac or leaking amniotic fluid.
ACOG discusses that, as part of natural sexuality, couples may need to try different
positions as the woman's stomach grows. Vaginal penetration by the male is not as
deep with the male facing the woman's back, and this may be more comfortable for
the pregnant woman.
Why do women get varicose veins during pregnancy?
Varicose veins are more common as women age; weight gain, the pressure on major
venous return from the legs, and familial predisposition increase the risk of
developing varicose veins during pregnancy. These can occur in the vulvar area and
be fairly painful. Rest, leg elevation, acetaminophen, topical heat, and support
stockings are typically all that is necessary. Determining that the varicosities are not
complicated by superficial thrombophlebitis is important. Having a venous
thromboembolism in association with superficial thrombophlebitis is rare.
Hemorrhoids, essentially varicosities of the anorectal veins, may first appear during
pregnancy for the same reasons and are aggravated by constipation during
pregnancy.
Why are urinary tract infections more common during pregnancy?
Pregnancy predisposes women with bacteriuria, which in the nonpregnant state is

usually self-limiting, to developing urinary tract infections (UTIs). Normal pregnancy-
related physiologic changes contribute to UTIs, including dilatation of the upper
collecting systems, hypotonic renal pelvises, increases in urinary tract dead space
and vesicoureteral reflux, and reductions in the natural antibacterial activity in the
urine and in the phagocytic activity of leukocytes at the mucosal surfaces. UTIs in
pregnant women usually do not present with typical symptoms, and they may be
asymptomatic. All of these factors increase the likelihood for infections to ascend to
the kidneys; pyelonephritis is a serious complication of UTIs.
How can stretch marks be prevented?
Unfortunately, striae (stretch marks) cannot be prevented. The degree to which a

woman experiences stretch marks is determined genetically. Stretch marks usually
occur when weight is lost or gained quickly. Using creams and gels rarely make a
difference. Fortunately, striae fade with time and marks become silvery white, but
they do not tan. Striae managed early can be reduced with new medical laser
technology.
Work and Exercise During Pregnancy
What kind of exercise can women engage in during pregnancy?
Regular physical activity during pregnancy is felt to improve or maintain physical

fitness as well as assisting with weight management, decreasing gestational
diabetes in obese women and enhancing well-being. A goal for pregnancy exercise
would include working up to moderate-intensity exercise for at least 20-30 minutes
daily on most days of the week. Although some preexisting conditions such as
chronic bronchitis and heavy smoking call for cautionary increases in activity, the
majority of women in pregnancy would benefit from becoming or remaining active.
Contact sports such as boxing as well as those with a high risk of falling (such as
downhill snow skiing) should be avoided. Walking, swimming and stationary cycling
are well suited to pregnancy. Running, racquet sports and strength training can be
safe in pregnancy, especially when these were done regularly prior to
pregnancy. Women doing these for the first time should use caution due to the
pregnancy causing a change in their center of balance and more laxity in their joints.
Should women restrict work during pregnancy?
Maintaining an active and productive lifestyle helps make time pass faster and adds
to a feeling of accomplishment. Working during pregnancy is usually not a problem
unless a woman has risk factors or a complicated pregnancy. Women should check
with their healthcare providers for specific restrictions. With an uncomplicated
pregnancy, working close to or near the due date should not be a problem. Pregnant
women should wear comfortable clothing, move around frequently if sedentary, drink
plenty of fluids, and have time to rest and take breaks. Women with strenuous jobs,
those who work with heavy machinery, or those who work with toxic chemicals
should consult their healthcare providers and their job's occupational department for
restrictions or concerns.
Postpartum
When will the uterus return to normal size?
The uterus returns to prepregnancy size after approximately 6 weeks. This is

accomplished through a process called involution. During involution, the uterus has
contractions that women may be able to feel, especially during breastfeeding.
When can women resume sexual intercourse after pregnancy?
Women usually can resume sexual intercourse when they feel ready, typically 4-6
weeks after delivery and when bleeding has substantially decreased. Clinically, this
is the period when the cervix has closed, which usually occurs at 4 weeks
postpartum, and when uterine bleeding is minimal.
The following are other issues to consider:

 Breastfeeding may cause increased vaginal dryness due to slightly decreased
estrogen levels.
 Women who have had an episiotomy need at least 2-3 weeks to heal before
intercourse.
 An ACOG bulletin indicated that some women may find that they do not have
much interest in sex after giving birth because of fatigue, stress, fear of pain,
lack of opportunity, and/or lack of desire. This lack of postpartum sexual
interest is usually temporary.
Reference: Medscape (WebMD LLC)

Diagnosis of Pregnancy
DIAGNOSIS OF PREGNANCY
It is crucial to diagnose pregnancy as soon as possible in order to initiate appropriate

prenatal care, avoid teratogen (an agent that can cause a deleterious fetal effect)
exposure, and diagnose nonviable or ectopic pregnancies.
Clinical Findings
A. Symptoms & Signs
A number of clinical signs and symptoms may presumptively indicate pregnancy.
1. Amenorrhea—Cessation of menses is caused by hormones (estrogen and

progesterone) produced by the corpus luteum. The abrupt cessation of menses in a
healthy reproductive-aged female with predictable cycles is highly suggestive of
pregnancy.
2. Nausea & vomiting—This is a common symptom (50% of pregnancies) that

begins as early as 2 weeks’ gestational age and customarily resolves at between 13
and 16 weeks’ gestation. Hyperemesis gravidarum is an extreme form of nausea and
vomiting and is characterized by dehydration, weight loss (up to 5%), and ketonuria.
In extreme cases of hyperemesis gravidarum, hospitalization, intravenous therapy,
antiemetics, and, if needed, parenteral nutrition are given. Uncomplicated nausea
and vomiting is treated with frequent small meals, a dry diet, and emotional support.
3. Breast changes
A. MASTODYNIA—Breast tenderness may range from tingling to pain caused by

hormonal changes affecting the mammary duct and alveolar system.
B. BREAST ENGORGEMENT—Breast engorgement and periareolar venous

prominences are also seen early in pregnancy, especially in primiparous patients.
Montgomery’s tubercles are the portion of the areolar glands visible on the skin
surface. These tubercles can be more pronounced during pregnancy secondary to
hormonal changes occurring as early as 6–8 weeks’ gestation.
C. COLOSTRUM SECRETION—Protein and antibody production may occur during
pregnancy as early as 16 weeks’ gestation. This secretion is not associated with
preterm delivery.
D. DEVELOPMENT OF SECONDARY BREAST TISSUE—Development of

secondary breast tissue may occur across the nipple line. Hypertrophy of secondary
breast tissue may occur in the axilla and cause a symptomatic mass.
4. Fetal movement—The initial perception of fetal movement occurs at 18–20

weeks’ gestation in primiparous patients and as early as 14 weeks’ gestation in
multiparous patients. Maternal perception of movement is called quickening, but this
is not a dependable sign of pregnancy.
5. Elevated basal body temperature—Progesterone produces a 0.5°F increase in

the basal body temperature, which persists after the missed menses. The rise in
temperature occurs within the luteal phase of the menstrual cycle.
6. Skin changes
A. CHLOASMA—The mask of pregnancy is skin darkening of the forehead, bridge of

the nose, or cheek bones. This pregnancy-associated change is linked to genetic
predisposition and usually occurs after 16 weeks’ gestation. Chloasma is
exacerbated by sunlight.
B. LINEA NIGRA—Melanocyte-stimulating hormone increases, causing darkening of

the nipples and the lower midline from the umbilicus to the pubis (linea nigra). This
skin change is genetically based; skin lightens slightly after delivery of the fetus.
C. STRIAE—Striae marks of the breast and abdomen appear as irregular scars. The
striae appear late in pregnancy and are caused by collagen separation.
D. SPIDER TELANGIECTASIA—These are common skin lesions of pregnancy that

result from elevated plasma estrogen. Both the vascular stellate skin lesions as well
as palmar erythema may be seen in pregnancy and also occur in patients with liver
failure.
7. Pelvic organ changes
A. CHADWICK’S SIGN—Congestion of the pelvic vasculature causes bluish

discoloration of the vagina and the cervix. This is a presumptive sign of pregnancy.
B. HEGAR’S SIGN—There is widening and softening of the body or isthmus of the

uterus. This occurs at 6–8 weeks’ menstrual age or gestational age. Estrogen and
progesterone cause increased cervical softening and dilation at the external os.
C. LEUKORRHEA—There is an increase in vaginal discharge, containing epithelial

cells and cervical mucous, secondary to hormonal changes.
D. PELVIC LIGAMENTS—There is relaxation of the sacroiliac and pubic symphysis

during pregnancy. Relaxation is pronounced at the pelvic symphysis.
E. ABDOMINAL ENLARGEMENT—There is progressive abdominal enlargement
with growth of uterus during pregnancy. From 18 to 34 weeks there is a good
correlation between the uterine fundal measurement in centimeters and the
gestational age in weeks.
F. UTERINE CONTRACTIONS—Painless uterine contractions (Braxton Hick’s

contractions) are felt as tightening or pressure. They usually begin at approximately
28 weeks’ gestation and increase in regularity with advancing gestational age. These
contractions usually disappear with walking or exercise, whereas true labor
contractions become more intense.
Diagnosis
A. Fetal Heart Tones
Fetal heart tones (FHTs) are detectable by handheld Doppler (after 10 weeks’
gestation) or by fetoscope (after 18–20 weeks’ gestation). The normal heart rate is
110–160 beats per minute, with a higher fetal heart rate observed early in
pregnancy.
B. Uterine Size/Fetal Palpation
Uterine size can be used to diagnose pregnancy secondary to uterine enlargement.

Later in pregnancy, the fetus can be palpated through the maternal abdominal wall
(after 22 weeks), and the position can be determined by Leopold’s maneuvers.
C. Imaging Studies
Sonography is one of the most useful technical aids in diagnosing and monitoring
pregnancy. Cardiac activity is discernible at 5–6 weeks via transvaginal sonogram,
limb buds at 7–8 weeks, and finger and limb movements at 9–10 weeks. At the end
of the embryonic period (10 weeks by LNMP), the embryo has a human appearance.
The gestational age can be determined by the crown rump length between 6 and 13
weeks’ gestation, with a margin of error of approximately 8% or 3–5 days.
D. Pregnancy Tests
Sensitive, early pregnancy tests measure changes in the level of human chorionic
gonadotropin (hCG). There is a small degree of cross-reactivity between luteinizing
hormone, follicle-stimulating hormone, and thyrotropin, which all share an α subunit
with hCG. The β submit of hCG is produced by the syncytiotrophoblast 8 days after
fertilization and may be detected in the maternal serum 8–11 days after conception
or as early as 21–22 days after the LNMP. β-hCG levels peak at 10–12 weeks’
gestation and decrease afterward. The half-life of hCG is 1.5 days. Generally, serum
and urine levels return to normal (<5 mIU/mL), 21–24 days after delivery or after a
fetal loss.
1. Home pregnancy test—hCG is a qualitative test that is performed on the first

voided morning urine sample. A positive test is usually indicated by a color change.
Because the accuracy of the home pregnancy test depends on technique and
interpretation, it should always be repeated in the office.
2. Urine pregnancy test—An antibody assay recognizing the β-hCG subunit is the
initial lab test performed in the office to diagnose pregnancy. The test is reliable,
rapid (1–5 minutes), and inexpensive, with a positive test threshold between 5 and
50 mIU/mL, characterized by a color change. This is the most common method to
confirm pregnancy.
3. Serum pregnancy test—β-hCG can be detected within 7 days after conception or

at a menstrual age of 21 days’ gestation. The threshold for a positive test can be as
low as 2–4 mIU/mL. Serial quantitative tests of β-hCG are be used to evaluate
threatened abortion, ectopic pregnancy, or a molar pregnancy.
Maternal Physiological Changes in Pregnancy
Introduction
v Maternal physiology undergoes many changes during pregnancy.
v These changes, which are largely secondary to the effects of progesterone and
estrogen, begin as early as 4 weeks gestation and are progressive.
v These changes both enable the fetus and placenta to grow and prepare the
mother and baby for childbirth.
Reproductive System Changes
Ø In the non-pregnant woman, the uterus weighs approximately 70g and is almost

solid, except for a cavity of 10 mL or less.
Ø By the end of pregnancy, the uterus has achieved a capacity that is 500 to 1000
times greater (approx. 5L) & weighs about 1100g!
Ø The size of the uterus increases 5-6 times (from 7x5x3 cm to 35x25x22 cm)
mostly due to hypertrophy of muscle cells.
Ø Uterine ligaments show hypertrophy.
Ø There is dextrorotation of the uterus (twisting to the right) in 80% of cases.
Ø Blood flow to the uterus increases 10-fold (from 50-500 ml/min)
Ø The shape of the uterus changes from its original pear shape to be spherical by
week 12 and finally attains an ovoid shape towards term.
Ø By the end of week 12, the enlarged uterus extends out of the pelvis and starts
displacing abdominal organs upwards and outwards.
Ø The lower uterine segment (LUS) starts forming at 4 months gestation and
reaches full development (10 cm) at full term.
Ø The uterine walls thin up but are supported by fibrous tissue.
Ø As early as 1 month after conception, the cervix begins to soften and gain bluish
tones. These result from increased vascularity and edema of the entire cervix; and
from changes in its collagen network.
Ø Cervical glands undergo marked proliferation, and there is increased cervical

secretions.
Ø A tenacious mucus plug that obstruct the cervical canal forms soon after
conception. This mucus is rich in immunoglobulins and cytokines and may act as an
immunological barrier to protect the uterine contents against infection.
Ø The fallopian tube elongates and its musculature undergoes little hypertrophy

during pregnancy.
Ø The ovaries show increased vascularity and one ovary contains the active corpus
luteum in early pregnancy.
Ø Ovulation is suspended during pregnancy because of pituitary inhibition.
Ø The vulva becomes edematous and more vascular; superficial varicosities may

appear especially in multiparae.
Ø Vaginal walls become hypertrophied, edematous and more vascular.
Ø The vaginal secretion becomes copious, thin and curdy white due to marked
exfoliated cells and bacteria.
Ø The vaginal pH becomes more acidic (3.5–6), which prevents bacterial infections
but promotes yeast infection.
Ø The changes in the breasts are best evident in a primigravida.
Ø In early pregnancy there is breast tenderness. After the second month, the
breasts grow in size, and delicate veins are visible just beneath the skin.
Ø The nipples become considerably larger, more deeply pigmented, and more

erectile.
Ø The areolae become broader and more deeply pigmented. Secondary areola

may appear.
Ø Tubercles of Montgomery (sebaceous glands) enlarge and secrete a substance

to maintain areolar suppleness.
Ø A thick, yellowish colostrum-like fluid can be expressed from the breast starting
from around the third month of pregnancy.
Cardiovascular System Changes
· The heart is displaced upward and outward making the apex beat to be

shifted to the 4th ICS about 2.5 cm outside the midclavicular line.
· Pulse rate is slightly raised (by 10-15 bpm), often with extrasystoles.
· A systolic murmur may be audible in the apical or pulmonary area due to

decreased blood viscosity and torsion of the great vessels.
· The cardiac output (CO) increases and reaches its peak (of 40–50% increase)
at about 30–34 weeks.
· Systemic vascular resistance (SVR) decreases (–21%) due to smooth muscle

relaxing effect of progesterone, NO, prostaglandins or ANP.
· Diastolic blood pressure (BP) and mean arterial pressure (MAP) decrease by

5–10 mm Hg.
· Systolic arterial pressure declines slightly during pregnancy, reaching a nadir

at 24–28 weeks of gestation.
· Supine hypotension syndrome occurs in 8% of women in the latter half of

pregnancy.
Hematological System Changes
o Blood (mostly Plasma) volume increases by 40-45% reaching a peak between

32-34 weeks.
o Circulating RBCs mass increases by 20-30% (more in multiple pregnancy and

with iron supplementation).
o The disproportionate increase in plasma and RBC volume produces a state of

hemodilution (fall in hematocrit) during pregnancy.
o Erythropoietin rises esp. with no iron supplementation
o Reticulocyte count increases by 2%
o Human placental lactogen (HPL) may stimulate hemopoiesis
o Erythrocyte Sedimentation Rate (ESR) level rises.

o WBC count rises (increase in polymorphonuclear leucocytes)
o Neutrophil count rises with estrogen levels and peaks at 33 weeks. It stabilizes

thereafter until the puerperium when it rises sharply.
o T and B lymphocytes counts do not change but their function is suppressed

(making pregnant women more susceptible to viral infections, malaria and leprosy)
o Platelet count and platelet functions are largely unchanged.
o There is increased concentrations of all clotting factors except

factors XI and XIII.
o Plasma fibrinolytic activity decreases during pregnancy and labor and returns

to normal within 1 hour of delivery of the placenta.
o Antithrombin III level falls.
o Because of all the above changes, pregnancy is considered as

a procoagulant state.
Respiratory System Changes
§ As the uterus enlarges, the diaphragm is elevated by as much as 4 cm. The rib

cage is displaced upward, increasing the angle of the ribs with the spine. May cause
dyspnea.
§ Abdominal muscles have less tone and activity during pregnancy, causing

respiration to be more diaphragm dependent.
§ Respiratory dead space volume increases because of relaxation of the

musculature of conducting airways.
§ Tidal volume & inspiratory reserve volume rise by 30-40%.
§ Elevation of the diaphragm is associated with reduction in total lung capacity,

expiratory reserve volume and functional residual capacity.
§ Increased levels of progesterone appear to have a critical role in

the hyperventilation of pregnancy, which develops early in the first trimester.
§ The overall respiratory effect appears to be a decrease in the threshold and an

increase in the sensitivity of central chemoreflex responses to CO2.
§ Respiratory rate does not change.
§ Carbon dioxide production rises sharply in the third trimester as fetal metabolism
increases.
Increased alveolar ventilation due to rise in PaCO2 from 96.7 mmHg to 101.8
§
mmHg.
§ Increase in oxygen consumption of about 16% by term.
§ Fall in arterio-venous oxygen difference.
§ Pregnancy places a greater demand on the cardiovascular system than on the

respiratory system.
Gastrointestinal System Changes
The gums may become hypertrophic and hyperemic (epulis); often, they are

so spongy and friable that they bleed easily.
Increased salivation (ptyalism)
Taste is often altered in early pregnancy
Increased appetite and thirst leading to frequent snacking
Heart burn (pyrosis) due to relaxation of the cardiac sphincter under the

influence of progesterone and relaxin
Emesis gravidarum [NVP] occurs in 70-80% of pregnancies.
Decreased gastric acidity which interferes with iron absorption
Constipation due to reduced gut motility caused by progestin
Hepatic synthesis of albumin, plasma globulin and fibrinogen increase
Gall bladder increases in size and empties more slowly
Relaxation of the gall bladder wall increases the tendency of gall stone

(cholelithiasis) formation
Secretion of bile is unchanged
Renal System Changes
ü During pregnancy, the length of the kidneys increases by 1–1.5 cm, with a

proportional increase in weight.
ü The renal calyces and pelves are dilated in pregnancy, with the volume of the
renal pelvis increased up to 6-fold.
ü The ureters are dilated above the brim of the bony pelvis, with more prominent
effects on the right.
ü The ureters elongate, widen, and become more curved.
ü The entire dilated collecting system may contain up to 200 mL of urine, which

predisposes to ascending urinary infections.
ü GFR increases reaching a peak increment of 40–65% by the end of the first

trimester and remains high until term.
ü 100 extra liters (40-60% increase) of fluid passes through the kidneys during

pregnancy
ü There is increased frequency of micturition due to pressure of the gravid

uterus on the bladder in the first trimester and pressure of the engaging
head towards term.
Endocrine System Changes
v The anterior pituitary gland increases in size and activity
v The posterior pituitary gland remains unchanged. It releases oxytocin at the

onset of labor.
v The thyroid gland increases in size (in 50%) and activity
v Most pregnant women are euthyroid
v The parathyroid glands increase in size and activity to regulate calcium

metabolism
v Adrenals increase in size and activity and increase total cortisol levels (free
cortisol levels remain the same)
v Progesterone is initially produced by the corpus luteum and later by the placenta.
v Its levels rises steadily throughout the pregnancy to a maximum of 250mg/day
v Its actions during pregnancy include: reduces gut motility, causes nausea and

constipation, reduces bladder and ureteric tone, causes vascular and bronchial
dilatation and raises body temperature.
v Estrogen is produced by the ovary in early pregnancy and then by the placenta
and fetal adrenals later in pregnancy. Levels of different estrogens peak during
pregnancy to between 100- and 1000-fold above normal non-pregnant values.
v The major actions of estrogen during pregnancy include the following: induce
growth of the uterus and development of the breasts; alter chemical composition of
connective tissues of the cervix to become more pliable; causes water retention and
reduce sodium excretion.
Musculoskeletal System Changes
Ø Increased lumbar lordosis. Compensating for the anterior position of the

enlarging uterus, lordosis shifts the center of gravity back over the lower extremities.
Ø Increased relaxation of pelvic joints and ligaments due
to progesterone and relaxin hormones.
Ø Joint strengthening begins immediately following delivery and is usually

complete within 3 to 5 months.
Skin Changes
· Increased skin pigmentation due to high melanocyte stimulating hormone
· Linea nigra: pigmentation of the linea alba that is more marked below the
umbilicus
· Chloasma gravidarum: butterfly pigmentation of the face
· Striae gravidarum: stretch marks of the abdominal wall or breasts due to

rupture of subcutaneous elastic fibres.
Weight Changes
o There is an overall increase in weight of approximately 12.5Kg on average at

term.
o There is a slight loss of weight during early pregnancy if the patient experiences

much nausea and vomiting.
o She then gains 1 to 2 Kgs by the end of the first trimester.
o The major increase occurs in the second half of the pregnancy at a rate of

approx. 0.5Kg/week.
Metabolic Changes
§ Basal metabolic rate is increased to the extent of 30% higher than that of the
average for the nonpregnant women.
§ Carbohydrate Metabolism: Normal pregnancy is characterized by mild fasting

hypoglycemia, postprandial hyperglycemia, and hyperinsulinemia.
§ This response reflects a pregnancy-induced state of peripheral insulin resistance,

which ensures a sustained postprandial supply of glucose to the fetus. The
mechanisms responsible for this reduced insulin sensitivity include numerous
endocrine and inflammatory factors.
§ In particular, pregnancy related hormones such as progesterone, placentally

derived growth hormone, prolactin, and cortisol; cytokines such
as tumor necrosis factor; and hormones derived from central adiposity,
particularly leptin and its interplay with prolactin, all have a role in the insulin
resistance of pregnancy.
§ Fat Metabolism: The concentrations of lipids, lipoproteins, and apolipoproteins in

plasma rise appreciably during pregnancy.
§ Augmented lipid synthesis and food intake contribute to maternal fat accumulation
during the first two trimesters. In the third trimester, however, fat storage declines or
ceases. This transition to a catabolic state favors maternal use of lipids as an energy
source and spares glucose and amino acids for the fetus.
§ Protein Metabolism: There is a positive nitrogenous balance throughout

pregnancy.
§ At term, the fetus and the placenta contain about 500 g of protein and the
maternal gain is also about 500 g chiefly distributed in the uterus, breasts and the
maternal blood.
§ As the breakdown of amino acid to urea is suppressed, the blood urea level falls
to 15–20 mg/dL. Blood uric acid and creatinine level, however, either remain
unchanged or fall slightly.
§ Pregnancy is an anabolic state.
Nervous System Changes
Women often report problems with attention, concentration,

and memory throughout pregnancy and the early puerperium.
Beginning as early as 12 weeks’ gestation and extending through the first 2

months postpartum, women have difficulty with falling asleep, frequent
awakenings, fewer hours of night sleep, and reduced sleep efficiency.
The greatest disruption of sleep is encountered postpartum and may
contribute to postpartum blues or to frank depression.
Psychological Changes
ü Maternal Emotional Responses include:
• Ambivalence
• Introversion (nervousness)
• Acceptance
• Mood Swings
• Changes in Body Image
ü A woman’s attitude toward a pregnancy depends a great deal on psychological

aspects such as the environment in which she was raised, the messages about
pregnancy her family communicated to her as a child, the society and culture in
which she lives as an adult, and whether the pregnancy has come at a good time or
less than a good time in her life (Darby, 2007).
ü Social Influences: How well a pregnant woman and her partner feel during
pregnancy and childbirth is related to their cultural background, their personal
experiences, and the experiences of friends and relatives, as well as that taught by
childbirth educators, and the current public philosophy of childbirth.
ü Individual Influences: A woman’s ability to cope with or adapt to stress plays a

major role in how she will resolve conflict and adapt to the new life contingencies that
are coming.
ü Family Influences: The family in which a woman was raised can be influential to

her beliefs about pregnancy because it is part of her cultural environment.
ü Cultural Influences: A woman’s cultural background may strongly influence how

active a role she wants to take in her pregnancy, because certain beliefs and taboos
may place restrictions on her behavior and activities (Andrews & Boyle, 2007).
Emotional Changes
v Emotional changes during pregnancy may include feeling uncomfortable with

having a baby, feeling anxious about caring for the new baby and even negative
emotions about the baby from time to time as sleep deprivation takes its toll on the
new mother and father.
v Feeling sad at times throughout pregnancy is completely normal.
v Mood Swings occur during pregnancy because of the overwhelming amount of

emotion. This is as a result of the progesterone hormone.
Antenatal Care (Concept and Practice)
Pregnancy is a normal physiologic process; however, complications that increase the

mortality or morbidity to the mother and/or fetus occur in 5–20% of pregnancies. The
present system of antenatal care focuses on prevention.
Antenatal care (ANC) is the medical care given to a pregnant woman from the
moment she realizes she is pregnant until she delivers. The purpose of antenatal
care is to ensure a successful pregnancy outcome when possible, including the
delivery of a live, healthy fetus. It’s proven that mothers receiving antenatal care
have a lower risk of complications, and one of the principal aims of antenatal care is
the identification and special treatment of the high-risk patient—the one whose
pregnancy, because of some factor in her medical history or an issue that develops
during pregnancy, is likely to have a poor outcome. Antenatal care providers must be
familiar with the normal changes of pregnancy and the possible pathologic changes
that may occur so that therapeutic measures can be initiated to reduce any risks to
the mother or fetus.
Antenatal care aims to make the woman the focus. Women should be treated with
kindness and dignity at all times, and due respect given to personal, cultural and
religious beliefs. Services should be readily accessible and there should be
continuity of care. There is a need for high-quality, culturally appropriate, verbal and
written information on which women can base their choices, through a truly informed
decision-making process, which is led by them.
ANC Schedule Models

1. High risk ANC model: The high risk approach intended to classify pregnant
women as “low risk” or “high risk” based on predetermined criteria and involved
many ANC visits. This approach was hard to implement effectively since many
women had at least one risk factor and not all developed complications; at the same
time, some low risk women did develop complications, particularly during childbirth.
2. Focused antenatal care (FANC) model: Focused or goal oriented ANC

services provides specific evidence-based interventions for all women, carried out at
certain critical times in the pregnancy. The essential elements of this package are
outlined in the boxes below:
3. The standard ANC model: The frequency of office visits is dependent on the
gestational age, maternal condition, and any fetal complications. The standard
schedule for prenatal office visits in uncomplicated patients is every 4 weeks from 0
to 32 weeks’ gestation, every 2 weeks from 32 to 36 weeks’ gestation, and weekly
visits after 36 weeks’ gestation. At each visit, maternal weight, uterine fundal height,
maternal blood pressure, and urinalysis by dipstick are documented. The FHTs
should be documented. All findings should be recorded and compared with those
from previous visits.
4. Revised WHO (2016) ANC model: Antenatal care models with a minimum of

eight contacts are recommended to reduce perinatal mortality and improve women’s
experience of care. The table below compares the FANC model and the revised
WHO (2016) ANC model:
FANC model WHO (2016) ANC model

First trimester
Visit 1: 8–12 weeks Contact 1: up to 12 weeks
Second trimester
Contact 2: 20 weeks
Visit 2: 24–26 weeks
Contact 3: 26 weeks
Third trimester
Contact 4: 30 weeks
Contact 5: 34 weeks
Visit 3: 32 weeks
Contact 6: 36 weeks
Visit 4: 36–38 weeks
Contact 7: 38 weeks
Contact 8: 40 weeks
Return for delivery at 41 weeks if not given birth.

WHO RECOMMENDATIONS ON ANTENATAL CARE
A. Nutritional interventions
Dietary interventions
A.1.1: Counselling about healthy eating and keeping physically active during

pregnancy is recommended for pregnant women to stay healthy and to prevent
excessive weight gain during pregnancy
A.1.2: In undernourished populations, nutrition education on increasing daily energy

and protein intake is recommended for pregnant women to reduce the risk of low-
birth-weight neonates.
A.1.3: In undernourished populations, balanced energy and protein dietary

supplementation is recommended for pregnant women to reduce the risk of stillbirths
and small-for-gestational-age neonates.
A.1.4: In undernourished populations, high-protein supplementation is not

recommended for pregnant women to improve maternal and perinatal outcomes.
Iron and folic acid supplements
A.2.1: Daily oral iron and folic acid supplementation with 30 mg to 60 mg of

elemental iron and 400 g (0.4 mg) of folic acid is recommended for pregnant women
to prevent maternal anaemia, puerperal sepsis, low birth weight, and preterm birth.
A.2.2: Intermittent oral iron and folic acid supplementation with 120 mg of elemental
iron and 2800 g (2.8 mg) of folic acid once weekly is recommended for pregnant
women to improve maternal and neonatal outcomes if daily iron is not acceptable
due to side-effects, and in populations with an anaemia prevalence among pregnant
women of less than 20%.
Calcium supplements
A.3: In populations with low dietary calcium intake, daily calcium supplementation
(1.5–2.0 g oral elemental calcium) is recommended for pregnant women to reduce
the risk of pre-eclampsia.
Vitamin A supplements
A.4: Vitamin A supplementation is only recommended for pregnant women in areas

where vitamin A deficiency is a severe public health problem, to prevent night
blindness.
Zinc supplements
A.5: Zinc supplementation for pregnant women is only recommended in the context

of rigorous research.
Restricting caffeine intake
A.10: For pregnant women with high daily caffeine intake (more than 300 mg per
day), lowering daily caffeine intake during pregnancy is recommended to reduce the
risk of pregnancy loss and low-birth-weight neonates.
B. Maternal and fetal assessment
B.1: Maternal assessment
Anaemia
B.1.1: Full blood count testing is the recommended method for diagnosing anaemia
in pregnancy. In settings where full blood count testing is not available, on-site
haemoglobin testing with a haemoglobinometer is recommended over the use of the
haemoglobin colour scale as the method for diagnosing anaemia in pregnancy.
Asymptomatic bacteriuria (ASB)
B.1.2: Midstream urine culture is the recommended method for diagnosing

asymptomatic bacteriuria (ASB) in pregnancy. In settings where urine culture is not
available, on-site midstream urine Gram staining is recommended over the use of
dipstick tests as the method for diagnosing ASB in pregnancy.
Intimate partner violence (IPV)
B.1.3: Clinical enquiry about the possibility of intimate partner violence (IPV) should
be strongly considered at antenatal care visits when assessing conditions that may
be caused or complicated by IPV in order to improve clinical diagnosis and
subsequent care, where there is the capacity to provide a supportive response
(including referral where appropriate) and where the WHO minimum requirements
are met.
Gestational diabetes mellitus (GDM)
B.1.4: Hyperglycaemia first detected at any time during pregnancy should be

classified as either gestational diabetes mellitus (GDM) or diabetes mellitus in
pregnancy, according to WHO criteria.
Tobacco use
B.1.5: Health-care providers should ask all pregnant women about their tobacco use
(past and present) and exposure to second-hand smoke as early as possible in the
pregnancy and at every antenatal care visit.
Substance use
B.1.6: Health-care providers should ask all pregnant women about their use of
alcohol and other substances (past and present) as early as possible in the
pregnancy and at every antenatal care visit.
Human immune deficiency virus (HIV) and syphilis
B.1.7: In high-prevalence settings, provider-initiated testing and counselling (PITC)

for HIV should be considered a routine component of the package of care for
pregnant women in all antenatal care settings. In low-prevalence settings, PITC can
be considered for pregnant women in antenatal care settings as a key component of
the effort to eliminate mother-to-child transmission of HIV, and to integrate HIV
testing with syphilis, viral or other key tests, as relevant to the setting, and to
strengthen the underlying maternal and child health systems.
Tuberculosis (TB)
B.1.8: In settings where the tuberculosis (TB) prevalence in the general population is
100/100 000 population or higher, systematic screening for active TB should be
considered for pregnant women as part of antenatal care.
B.2: Fetal assessment
Daily fetal movement counting
B.2.1: Daily fetal movement counting, such as with “count-to-ten” kick charts, is only
recommended in the context of rigorous research.
Symphysis-fundal height (SFH) measurement
B.2.2: Replacing abdominal palpation with symphysis-fundal height (SFH)

measurement for the assessment of fetal growth is not recommended to improve
perinatal outcomes. A change from what is usually practiced (abdominal palpation or
SFH measurement) in a particular setting is not recommended.
Ultrasound scan
B.2.4: One ultrasound scan before 24 weeks of gestation (early ultrasound) is

recommended for pregnant women to estimate gestational age, improve detection of
fetal anomalies and multiple pregnancies, reduce induction of labour for post-term
pregnancy, and improve a woman’s pregnancy experience.
C. Preventive measures
Antibiotics for asymptomatic bacteriuria (ASB)
C.1: A seven-day antibiotic regimen is recommended for all pregnant women with
asymptomatic bacteriuria (ASB) to prevent persistent bacteriuria, preterm birth and
low birth weight.
Antibiotic prophylaxis to prevent recurrent urinary tract infections
C.2: Antibiotic prophylaxis is only recommended to prevent recurrent urinary tract

infections in pregnant women in the context of rigorous research.
Antenatal anti-D immunoglobulin administration
C.3: Antenatal prophylaxis with anti-D immunoglobulin in non-sensitized Rh-negative

pregnant women at 28 and 34 weeks of gestation to prevent RhD alloimmunization is
only recommended in the context of rigorous research.
Preventive anthelminthic treatment
C.4: In endemic areas, preventive anthelminthic treatment is recommended for

pregnant women after the first trimester as part of worm infection reduction
programmes.
Tetanus toxoid vaccination
C.5: Tetanus toxoid vaccination is recommended for all pregnant women, depending

on previous tetanus vaccination exposure, to prevent neonatal mortality from
tetanus.
Malaria prevention: intermittent preventive treatment in pregnancy (IPTp)
C.6: In malaria-endemic areas in Africa, intermittent preventive treatment with

sulfadoxine-pyrimethamine (IPTp-SP) is recommended for all pregnant women.
Dosing should start in the second trimester, and doses should be given at least one
month apart, with the objective of ensuring that at least three doses are received.
Pre-exposure prophylaxis (PrEP) for HIV prevention
C.7: Oral pre-exposure prophylaxis (PrEP) containing tenofovir disoproxil fumarate

(TDF) should be offered as an additional prevention choice for pregnant women at
substantial risk of HIV infection as part of combination prevention approaches.
D. Interventions for common physiological symptoms
Nausea and vomiting
D.1: Ginger, chamomile, vitamin B6 and/or acupuncture are recommended for the

relief of nausea in early pregnancy, based on a woman’s preferences and available
options.
Heartburn
D.2: Advice on diet and lifestyle is recommended to prevent and relieve heartburn in

pregnancy. Antacid preparations can be offered to women with troublesome
symptoms that are not relieved by lifestyle modification.
Leg cramps
D.3: Magnesium, calcium or non-pharmacological treatment options can be used for

the relief of leg cramps in pregnancy, based on a woman’s preferences and available
options.
Low back and pelvic pain
D.4: Regular exercise throughout pregnancy is recommended to prevent low back

and pelvic pain. There are a number of different treatment options that can be used,
such as physiotherapy, support belts and acupuncture, based on a woman’s
preferences and available options.
Constipation
D.5: Wheat bran or other fibre supplements can be used to relieve constipation in

pregnancy if the condition fails to respond to dietary modification, based on a
woman’s preferences and available options.
Varicose veins and oedema
D.6: Non-pharmacological options, such as compression stockings, leg elevation

and water immersion, can be used for the management of varicose veins and
oedema in pregnancy, based on a woman’s preferences and available options.
ELIMINATION OF MOTHER TO CHILD TRANSMISSION OF HIV AND SYPHILIS
Mother-to-child transmission (MTCT) of HIV is a significant contributor to the HIV

pandemic, accounting for 9% of new infections globally. The Joint United Nations
Programme on HIV/AIDS (UNAIDS) reported that in 2016 an estimated 160 000
children were newly infected with HIV, and an estimated 3.1 million children were
living with HIV globally. Although this is still a large number of new infections, at the
peak of the HIV epidemic, there were close to 500 000 children infected with HIV
through MTCT each year.
MTCT of HIV occurs when HIV is transmitted from a woman living with HIV to her
baby during pregnancy, labour or delivery, or after delivery through breastfeeding.
Without treatment, approximately 15–30% of infants born to HIV-positive women will
become infected with HIV during gestation and delivery, with a further 5–15%
becoming infected through breastfeeding. HIV infection of infants results in early
mortality for many or creates a lifelong chronic condition that greatly shortens life
expectancy and contributes to substantial human, social and economic costs.
Globally, an estimated 1.3 million women living with HIV become pregnant every
year. Primary prevention of HIV, prevention of unintended pregnancies, effective
access to HIV testing and counselling, initiation of lifelong antiretroviral therapy
(ART) with support for adherence, retention and viral suppression for mothers living
with HIV, safe delivery practices, optimal infant feeding practices and access to
postnatal antiretroviral (ARV) prophylaxis for infants all contribute to the prevention
of mother-to-child transmission (PMTCT), thereby reducing maternal and child
mortality. With the global shift to highly effective and simplified interventions based
on lifelong maternal ART, it is now feasible to virtually eliminate new HIV infections in
infants, while assuring the health of the mother.
In 2012, WHO estimated that over 900 000 pregnant women were infected with
syphilis. These maternal infections resulted in more than 350 000 estimated adverse
pregnancy outcomes, over 200 000 of which were stillbirths or neonatal deaths.
Syphilis is caused by the Treponema pallidum bacterium, renowned for its
invasiveness. It can be transmitted via sexual exposure or vertically from mother to
child early in pregnancy (in utero infection). If the infection remains untreated,
adverse pregnancy outcomes are frequent. Indeed, over half of the pregnancies
among women with active syphilis will result in stillbirth, early neonatal death, a
preterm or low-birth-weight infant, or serious neonatal infection. Screening for
maternal syphilis early in pregnancy and prompt treatment of seropositive mothers
with intramuscular benzathine benzylpenicillin, a long-acting penicillin, cures syphilis
in both mother and infant, and prevents most complications associated with MTCT of
syphilis.
Dual elimination serves to improve a broad range of maternal and child health (MCH)
services and outcomes. This achievement directly contributes to Sustainable
Development Goals (SDGs) 3, 5 and 10, which aspire to ensure health and well-
being for all, achieve gender equality and empower women and girls, and reduce
inequalities in access to services and commodities. Additionally, the similarity of the
control interventions necessary to prevent transmission of HIV and syphilis in
pregnancy adds to the feasibility and benefit of such an integrated approach to the
elimination of MTCT (EMTCT) of both infections.
The following strategies are important components of successful EMTCT

programmes:
• interruption of transmission through quality ANC and prevention services that

provide timely identification and treatment of pregnant women infected with HIV or
syphilis, their sexual partners, and their infants;
ü reduction in the number of HIV and/or syphilis infections among pregnant women
through:
prevention of HIV and/or syphilis infection in women of reproductive age, including in
HIV negative pregnant and breastfeeding women and their sexual partners;
ü promotion of a healthy reproductive life, including prevention of unintended

pregnancies and support for safer conception among women with known HIV
infection;
ü control of HIV and syphilis in the general and key populations (including sex
workers, drug users, men who have sex with men) to decrease prevalence.
• promotion and protection of the human rights and gender equality of women living
with HIV;
• greater engagement of women living with HIV in HIV programming, decision-
making and service delivery.
SPECIFIC EMTCT MEASURES
Guidelines on infant feeding for mothers living with HIV
WHO bases its recommendations on infant feeding for mothers living with HIV on the
comparative risk of infants acquiring HIV through breastfeeding with the increased
risk of infants dying from illnesses such as malnutrition, diarrhea and pneumonia,
which increases if they are not breastfed.
In 2016, WHO released guidelines recommending that mothers living with HIV who
are on treatment and are being fully supported to adhere to it should exclusively
breastfeed their infants for the first six months of life, then introduce appropriate
complementary foods while continuing to breastfeed for at least 12 months and up to
24 months or longer (similar to the general population).
When ARV drugs are not immediately available, the WHO guidelines still
recommend mothers exclusively breastfeed for the first six months of an infant’s life
and continue, unless environmental and social circumstances are safe for, and
supportive of, replacement feeding. This decision should be based on international
recommendations and consideration of:
 the socioeconomic and cultural contexts of the population groups served by

maternal and child health services
 the availability and quality of health services
 the local epidemiology (which diseases are common and who they affect),
including HIV prevalence among pregnant women
 the main causes of under-nutrition among mothers and children, and infant
and child mortality.
When ARV drugs are unlikely to be available, such as in acute emergencies,

mothers living with HIV are still recommended to breastfeed their infants to increase
their chances of survival.
Currently, most high-income countries recommend women living with HIV do not
breastfeed whether they are virally suppressed or not. This is because formula feed
and clean, boiled water are widely accessible. So any risks around dirty water or
malnutrition have been eliminated. In low- and middle-income countries this risk is
far greater, leading WHO’s advice on infant feeding to differ.
Guidelines for HIV-exposed infants
If an HIV-exposed infant is given ART within the first 12 weeks of life, they are 75%
less likely to die from an AIDS-related illness. The treatment should be linked to the
mother's course of ARV drugs and would vary according to the infant feeding method
as follows:
 breastfeeding: the infant should receive once-daily nevirapine from birth for

six weeks
 replacement feeding: the infant should receive once-daily nevirapine (or
twice-daily zidovudine) from birth for four to six weeks.
This is one of the reasons WHO recommends that infants born to mothers living with
HIV are tested between four and six weeks old. This is often referred to as ‘early
infant diagnosis’.
WHO further recommends that another HIV test is carried out at 18 months and/or
when breastfeeding ends to provide the final infant diagnosis. As proportionally more
infant infections are now occurring during breastfeeding these tests are becoming
increasingly important.
According to WHO guidelines, all infants who test positive for HIV should be
immediately initiated on treatment (full HAART).
unit six content

Topic 1: Ectopic Pregnancy
ECTOPIC PREGNANCY
Ectopic pregnancy refers to the implantation of a fertilized egg in a location outside

of the uterine cavity, including the fallopian tubes (approximately 97.7%), cervix,
ovary, cornual region of the uterus, and abdominal cavity. Of tubal pregnancies, the
ampulla is the most common site of implantation (80%), followed by the isthmus
(12%), fimbria (5%), cornua (2%), and interstitia (2-3%).
Ectopic pregnancy is the result of a flaw in human reproductive physiology that

allows the conceptus to implant and mature outside the endometrial cavity, which
ultimately ends in the death of the fetus. Without timely diagnosis and treatment,
ectopic pregnancy can become a life-threatening situation. As the gestation
enlarges, it creates the potential for organ rupture, because only the uterine cavity is
designed to expand and accommodate fetal development. Ectopic pregnancy can
lead to massive hemorrhage, infertility, or death
Etiology
An ectopic pregnancy requires the occurrence of 2 events: fertilization of the ovum

and abnormal implantation. Many risk factors affect both events; for example, a
history of major tubal infection decreases fertility and increases abnormal
implantation.
Multiple factors contribute to the relative risk of ectopic pregnancy. In theory,

anything that hampers or delays the migration of the fertilized ovum (blastocyst) to
the endometrial cavity can predispose a woman to ectopic gestation. The following
risk factors have been linked to ectopic pregnancy:
1. Tubal damage - Which can be the result of infections such as pelvic inflammatory
disease (PID) or salpingitis (whether documented or not) or can result from
abdominal surgery or tubal ligation or from maternal in utero diethylstilbestrol (DES)
exposure
2. History of previous ectopic pregnancy
3. Smoking - A risk factor in about one third of ectopic pregnancies; smoking may
contribute to decreased tubal motility by damage to the ciliated cells in the fallopian
tubes
4. Altered tubal motility - As mentioned, this can result from smoking, but it can also
occur as the result of hormonal contraception; progesterone-only contraception and
progesterone intrauterine devices (IUDs) have been associated with an increased
risk of ectopic pregnancy
5. History of 2 or more years of infertility (whether treated or not) - Women using
assisted reproduction seem to have a doubled risk of ectopic pregnancy (to 4%),
although this is mostly due to the underlying infertility
6. History of multiple sexual partners
7. Maternal age - Although this is not an independent risk factor
Clinical Presentation
The classic clinical triad of ectopic pregnancy is pain, amenorrhea, and vaginal
bleeding; unfortunately, only about 50% of patients present with all 3 symptoms.
About 40-50% of patients with an ectopic pregnancy present with vaginal bleeding,
50% have a palpable adnexal mass, and 75% may have abdominal tenderness. In
one case series of ectopic pregnancies, abdominal pain presented in 98.6% of
patients, amenorrhea in 74.1% of them, and irregular vaginal bleeding in 56.4% of
patients.
Patients may present with other symptoms common to early pregnancy, including
nausea, breast fullness, fatigue, low abdominal pain, heavy cramping, shoulder pain,
and recent dyspareunia. Painful fetal movements (in the case of advanced
abdominal pregnancy), dizziness or weakness, fever, flulike symptoms, vomiting,
syncope, or cardiac arrest have also been reported. Shoulder pain may be reflective
of peritoneal irritation.
The physical examination of patients with ectopic pregnancy is highly variable and
often unhelpful. Patients frequently present with benign examination findings, and
adnexal masses are rarely found. Patients in hemorrhagic shock from ruptured
ectopic may not be tachycardic.
Some physical findings that have been found to be predictive (although not
diagnostic) for ectopic pregnancy include the following:
 Presence of peritoneal signs

 Cervical motion tenderness
 Unilateral or bilateral abdominal or pelvic tenderness - Usually much worse on the
affected side
Abdominal rigidity, involuntary guarding, and severe tenderness, as well as evidence

of hypovolemic shock, such as orthostatic blood pressure changes and tachycardia,
should alert the clinician to a surgical emergency; this may occur in up to 20% of
cases. However, midline abdominal tenderness or a uterine size of greater than 8
weeks on pelvic examination decreases the risk of ectopic pregnancy.
On pelvic examination, the uterus may be slightly enlarged and soft, and uterine or
cervical motion tenderness may suggest peritoneal inflammation. An adnexal mass
may be palpated but is usually difficult to differentiate from the ipsilateral ovary.
The presence of uterine contents in the vagina, which can be caused by shedding of
endometrial lining stimulated by an ectopic pregnancy, may lead to a misdiagnosis of
an incomplete or complete abortion and therefore a delayed or missed diagnosis of
ectopic pregnancy.
Diagnosis
Serum β-HCG levels
In a normal pregnancy, the β-HCG level doubles every 48-72 hours until it reaches
10,000-20,000mIU/mL. In ectopic pregnancies, β-HCG levels usually increase less.
Mean serum β-HCG levels are lower in ectopic pregnancies than in healthy
pregnancies.
No single serum β-HCG level is diagnostic of an ectopic pregnancy. Serial serum β-

HCG levels are necessary to differentiate between normal and abnormal
pregnancies and to monitor resolution of ectopic pregnancy once therapy has been
initiated.
The discriminatory zone of β-HCG (ie, the level above which an imaging scan should
reliably visualize a gestational sac within the uterus in a normal intrauterine
pregnancy) is as follows:
 1500-1800 mIU/mL with transvaginal ultrasonography, but up to 2300 mIU/mL with

multiple gestates
 6000-6500 mIU/mL with abdominal ultrasonography
Absence of an intrauterine pregnancy on a scan when the β-HCG level is above the
discriminatory zone represents an ectopic pregnancy or a recent abortion.
Ultrasonography
Ultrasonography is probably the most important tool for diagnosing an extrauterine

pregnancy.
Visualization of an intrauterine sac, with or without fetal cardiac activity, is often

adequate to exclude ectopic pregnancy.
Transvaginal ultrasonography, or endovaginal ultrasonography, can be used to

visualize an intrauterine pregnancy by 24 days post ovulation or 38 days after the
last menstrual period (about 1 week earlier than transabdominal ultrasonography).
An empty uterus on endovaginal ultrasonographic images in patients with a serum β-
HCG level greater than the discriminatory cut-off value is an ectopic pregnancy until
proved otherwise.
Color-flow Doppler ultrasonography improves the diagnostic sensitivity and

specificity of transvaginal ultrasonography, especially in cases in which a gestational
sac is questionable or absent.
Laparoscopy
Laparoscopy remains the criterion standard for diagnosis; however, its routine use
on all patients suspected of ectopic pregnancy may lead to unnecessary risks,
morbidity, and costs. Moreover, laparoscopy can miss up to 4% of early ectopic
pregnancies.
Laparoscopy is indicated for patients who are in pain or hemodynamically unstable.
Management
Therapeutic options in ectopic pregnancy are as follows:
 Expectant management
 Methotrexate
 Surgery
Expectant management
Candidates for successful expectant management should be asymptomatic and

have no evidence of rupture or hemodynamic instability. Candidates should
demonstrate objective evidence of resolution (eg, declining β-HCG levels).
Close follow-up and patient compliance are of paramount importance, as tubal

rupture may occur despite low and declining serum levels of β-HCG.
Methotrexate
Methotrexate is the standard medical treatment for unruptured ectopic pregnancy. A
single-dose IM injection is the more popular regimen. The ideal candidate should
have the following:
 Hemodynamic stability
 No severe or persisting abdominal pain
 The ability to follow up multiple times
 Normal baseline liver and renal function test results
Absolute contraindications to methotrexate therapy include the following:
 Existence of an intrauterine pregnancy

 Immunodeficiency
 Moderate to severe anemia, leukopenia, or thrombocytopenia
 Sensitivity to methotrexate
 Active pulmonary or peptic ulcer disease
 Clinically important hepatic or renal dysfunction
 Breastfeeding
 Evidence of tubal rupture
Surgical treatment
Conservative Surgery: The procedure can be done either laparoscopically or by

microsurgical
laparotomy.
Indications: (a) Cases not fulfilling the criteria of medical therapy. (b) Cases where
b-hCG levels are not decreasing despite medical therapy. (c) persistent fetal cardiac
activity.
1. Linear Salpingostomy: A longitudinal incision is made on the antimesenteric

border directly over the site of ectopic pregnancy. After removing the products (by
fingers, scalpel handle or by suction), the incision line is kept open to be healed later
on by secondary intention. Hemostasis is achieved by electrocautery or laser.
2. Linear Salpingotomy: The procedures are the same as those of salpingostomy.

But the incision line is closed in two layers with 7-0 interrupted vicryl sutures. This is
not commonly done.
3. Segmental Resection: This is of choice in isthmic pregnancy. End-to-end

anastomosis can be done immediately or at a later date after appropriate counseling
of the patient.
4. Fimbrial Expression: This is ideal in cases of distal ampullary (fimbrial)

pregnancy and is done digitally.
Salpingectomy is done when (i) whole of the affected tube is damaged, (ii)
contralateral tube is normal or (iii) future fertility is not desired.
Following conservative surgery or medical treatment, estimation of b-hCG should be

done weekly
till the value becomes less than 5.0 mlU/mL. Additional monitoring by TVS is
preferred. Following laparoscopic salpingostomy, persistent ectopic pregnancy
ranges between 4% and 20%.
Persistent ectopic pregnancy is due to incomplete removal of trophoblast. It is high

after fimbrial
expression and in cases where initial serum b-hCG level is greater than 3,000 IU/L.
Prophylactic single dose MTX (1 mg/kg) IM is effective to resolve the problem.
GESTATIONAL TROPHOBLASTIC DISEASES (GTDs)
Gestational trophoblastic disease (GTD) refers to a spectrum of interrelated but

histologically distinct tumors originating from the placenta. These diseases are
characterized by a reliable tumor marker, which is the β-subunit of human chorionic
gonadotropin (β-hCG), and have varied tendencies or local invasion and spread.
Gestational trophoblastic neoplasia (GTN) refers to the subset of GTD that develops
malignant sequelae. These tumors require normal staging and typically respond
favorably to chemotherapy. Most commonly, GTN develops after a molar pregnancy
but may follow any gestation. The prognosis or most GTN cases is excellent, and
patients are routinely cured, even with widespread
metastases. The outlook or preservation of fertility and or successful subsequent
pregnancy outcomes is equally bright. Accordingly, although GTD is uncommon,
because the opportunity or cure is great, clinicians should be familiar with its
presentation, diagnosis, and management.
Classification of GTD
1. Hydatidiform mole: – Complete – Partial

2. Invasive mole
3. Placental site trophoblastic tumor (PSTT)
4. Choriocarcinoma
5. Epithelioid trophoblastic tumor (ETT)
RISK FACTORS
· Maternal age at the upper and lower extremes carries a higher risk of GTD.
This association is much greater for complete moles, whereas the risk of partial
molar pregnancy varies relatively little with age.
· A history of prior unsuccessful pregnancies also increases the risk of GTD.
For example, previous spontaneous abortion at least doubles the risk of molar
pregnancy. More significantly, a personal history of GTD increases the risk of
developing a molar gestation in a subsequent pregnancy at least 10-fold.
· Prior COC use approximately doubles the risk, and longer duration of use also
correlates positively with risk.
· Some epidemiologic characteristics differ markedly between complete and
partial moles. For example, vitamin A deficiency and low dietary intake of carotene
are associated only with an increased risk of complete moles. Partial moles have
been linked to higher educational levels, smoking, irregular menstrual cycles, and
obstetric histories in which only male infants are among the prior live births. Many of
these associations, however, are weak and could be explained by confounding
factors other than causality.
HYDATIDIFORM MOLE (MOLAR PREGNANCY)
Hydatidiform moles are abnormal pregnancies characterized histologically by

aberrant changes within the placenta. Classically, the chorionic villi in these placenta
show varying degrees of trophoblast proliferation and edema o the stroma within villi.
Hydatidiform moles are categorized as either complete hydatidiform moles or partial
hydatidiform moles. Chromosomal abnormalities play an integral role in hydatidiform
mole development.
Complete Hydatidiform Mole
These molar pregnancies differ from partial moles with regard to their karyotype,
their histologic appearance, and their clinical presentation. First, complete moles
typically have a diploid karyotype, and 85 to 90 percent of cases are 46,XX. The
chromosomes, however, in these pregnancies are entirely of paternal origin, and
thus, the diploid set is described as diandric. Specifically, complete moles are formed
by androgenesis, in which the ovum is fertilized by a haploid sperm that then
duplicates its own chromosomes after meiosis. The ovum fails to contribute
chromosomes. Most of these moles are 46,XX, but dispermic fertilization of a single
ovum, that is, simultaneous fertilization by two sperm, can produce a 46,XY
karyotype.
Microscopically, complete moles display enlarged, edematous villi and abnormal

trophoblastic proliferation. These changes diffusely involve the entire placenta.
Macroscopically, these changes transform the chorionic villi into clusters of vesicles
with variable dimensions. Indeed, the name hydatidiform mole literally stems from
this “bunch of grapes” appearance. In these pregnancies, no fetal tissue or amnion is
produced. As a result, this mass of placental tissue completely fills the endometrial
cavity.
More than half of affected patients present with anemia and uterine sizes in excess
of that predicted or their gestational age. In addition, hyperemesis gravidarum,
preeclampsia, and theca-lutein cysts develop in approximately one quarter of
women. These cysts range in size from 3 to 20 cm, and most regress with falling β-
hCG titers after molar evacuation. If such cysts are present, and especially if they
are bilateral, the risk of postmolar GTN is increased.
Vaginal bleeding remains the most common presenting symptom, and β-hCG levels
are often greater than expected.
Partial Hydatidiform Mole

These moles differ from complete hydatidiform moles clinically, genetically, and
histologically. The degree and extent of trophoblastic proliferation and villous edema
are decreased compared with those of complete moles. Moreover, most partial
moles contain fetal tissue and amnion, in addition to placental tissues. As a result,
patients with partial moles typically
present with signs and symptoms of an incomplete or missed abortion. Many women
will have vaginal bleeding. However, because trophoblastic proliferation is slight and
only focal, uterine enlargement in excess of gestational age is uncommon. Similarly,
preeclampsia, theca-lutein cysts, hyperthyroidism, or other dramatic clinical features
are rare.
Preevacuation β-hCG levels are typically much lower than those or complete moles
and o ten do not exceed 100,000 mIU/mL. For this reason, partial moles are o ten
not identified until after a histologic review of a curettage specimen.
Partial moles have a triploid karyotype (69, XXX, 69,XXY, or less commonly 69,XYY)
that is composed of one maternal and two paternal haploid sets of chromosomes.
The coexisting fetus present with a partial mole is nonviable and typically has
multiple malformations with abnormal growth.
Clinical Findings
A. Symptoms & Signs
Abnormal uterine bleeding, usually during the first trimester, is the most common
presenting symptom, occurring in more than 90% of patients with molar pregnancies.
Three-fourths of these patients present before the end of the first trimester. Nausea
and vomiting have been reported in 14–32% of patients with hydatidiform mole and
may be confused with nausea and vomiting of pregnancy or hyperemesis
gravidarum. Ten percent of these patients may have nausea and vomiting severe
enough to require hospitalization. About half of patients will have a uterine size that
is greater than expected for their gestational age.
However, in one-third of patients, the uterus may be smaller than expected. Multiple
theca lutein cysts causing enlargement of one or both ovaries are seen in 15–30% of
women with molar pregnancies. In about half of these cases, both ovaries are
enlarged and may be a source of pain. Involution of the cysts proceeds over several
weeks and usually parallels the decline of hCG values. In studies, patients with theca
lutein cysts appear to have a greater likelihood of developing malignant sequelae of
gestational trophoblastic neoplasia.
Preeclampsia in the first trimester or early second trimester—an unusual finding in

normal pregnancies—has been said to be pathognomonic for a molar pregnancy.
Hyperthyroidism from stimulation of thyrotropin receptors by hCG can also occur in
10% of patients, although the disease is usually subclinical, and most patients
remain asymptomatic. Treatment involves evacuation of the mole. An occasional
patient may require brief antithyroid therapy.
B. Laboratory Findings
The principal characteristic of gestational trophoblastic neoplasms is their capacity to
produce hCG. This hormone may be detected in the serum or urine of virtually all
patients with hydatidiform mole or malignant trophoblastic disease, and its levels
correlate closely with the presence of viable tumor cells. Consequently, monitoring of
hCG levels is a necessary tool for the diagnosis, treatment, and surveillance of the
disease process.
The usefulness of a serum gonadotropin assay depends on the hCG titer and the
sensitivity of the test. Today, sensitive and specific immunoassays are available to
differentiate hCG from luteinizing hormone by measuring the β chain of hCG. Serial
β-hCG levels are best monitored in the same laboratory using the same
immunoassay technique.
The rate of decline in hCG titers is also important. Normal postmolar pregnancy hCG
regression curves highlighting the weekly hCG levels in patients undergoing
spontaneous remission have been constructed, hence providing a reference for the
comparison of random or serial values. In most instances, the hCG values exhibit a
progressive decline to non-detectable levels within 14 weeks after evacuation of a
molar pregnancy. If the hCG titer rises or plateaus, it must be concluded that viable
tumor continues to persist. If the levels of hCG are very low and not responsive to
treatment, a false positive hCG result or “phantom hCG,” caused by cross-reaction of
heterophilic antibodies with the hCG test, should be considered.
C. Ultrasonographic Findings
The simplicity, safety, and reliability of ultrasonography define it as the diagnostic

method of choice for patients with suspected molar pregnancy. In a complete molar
pregnancy, the characteristic ultrasound pattern consists of multiple hypoechoic
areas corresponding to hydropic villi, at times described as a “snowstorm” pattern. A
normal gestational sac or fetus is not present. Theca lutein cysts may be visualized.
In a partial mole, focal areas of trophoblastic changes and fetal tissue may be noted.
Focal cystic changes in the placenta are also a hallmark finding. On the other hand,
an ultrasonogram of a choriocarcinoma may reveal an enlarged uterus with a
necrotic and hemorrhagic pattern, whereas that of PSTT may show an intrauterine
mass.
Complications
The maternal–fetal barrier contains leaks large enough to permit passage of cellular
and tissue elements. As a result, deportations of trophoblastic tissue to the lungs are
frequent. Spontaneous regression of these ectopic trophoblastic tissues can occur.
Less commonly, this results in a syndrome of acute pulmonary insufficiency.
Symptoms of dyspnea and cyanosis, due to massive deportation of trophoblasts to
the pulmonary vasculature and subsequent formation of pulmonary emboli, can
present within 4–6 hours after evacuation of a molar pregnancy. Pulmonary edema
leading to high-output congestive heart failure may complicate excessive fluid
administration, preeclampsia, anemia, or hyperthyroidism.
Treatment
After the diagnosis has been confirmed, blood type, hematocrit, and thyroid, liver,
and renal function tests should be obtained. A chest radiograph can rule out
metastasis to the lungs. Subsequently, the molar pregnancy should be terminated.
Suction curettage under general anesthesia is the method of choice once the patient
is deemed stable. This can be safely accomplished even when the uterus is the size
of a 28-week gestation. Local or regional anesthesia may be an option for the stable,
cooperative patient with a small uterus. Intravenous oxytocin should be administered
after dilation of the cervix but before the start of evacuation and may be continued, if
necessary, for 24 hours post-evacuation. Tissue should be submitted for pathologic
study. Blood loss usually is moderate, but precautions should be taken for the
possibility of hemorrhage requiring a transfusion.
When a large hydatidiform mole (>12 weeks in size) is evacuated by suction

curettage, a laparotomy setup should be readily available, as hysterotomy,
hysterectomy, or bilateral hypogastric artery ligation may be necessary if perforation
or hemorrhage occurs. After the completion of the evacuation, all Rh-negative
patients should receive Rh immune globulin. Hysterectomy continues to remain an
option for good surgical candidates not desirous of future pregnancy and for older
women (who are more likely to develop malignant sequelae). If theca lutein cysts are
encountered at laparotomy, the ovaries should remain intact, as regression to normal
size will occur with diminishing hCG titers. Surgical treatment of these cysts is
indicated only if rupture, torsion, or hemorrhage occurs or if the enlarged ovaries
become infected.
Follow-up
Despite earlier diagnosis of molar pregnancies, the incidence of persistent

gestational trophoblastic disease has not decreased. Three-fourths of patients with
malignant nonmetastatic trophoblastic disease and half of patients with malignant
metastatic disease develop these tumors following a hydatidiform mole. In the
remainder, disease arises subsequent to a term pregnancy, abortion, or ectopic
pregnancy. Several clinical features of hydatidiform moles are recognized as having
a high association with malignant trophoblastic neoplasia. In general, at diagnosis,
the larger the uterus and the higher the hCG titer, the greater the risk for malignant
gestational trophoblastic disease. The combination of theca lutein cysts and uterine
size excessive for gestational age is associated with an extremely high risk of
malignant sequelae. Pathologic specimens with marked nuclear atypia, necrosis,
hemorrhage, or trophoblastic proliferation may also increase the risk of persistent
disease.
Regardless of the method of termination (suction curettage or hysterectomy) or

presence of high risk features, close monitoring with serial hCG titers is essential for
every patient, as the incidence of malignant sequelae approaches 20–30%. After
evacuation of the molar pregnancy, the patient should undergo serial hCG
determinations, beginning within 48 hours after evacuation and then at weekly
intervals until hCG values decline to undetectable levels (<5 mIU per milliliter) on
three successive assays. If titer remission occurs spontaneously within 14 weeks
and without a titer plateau, the hCG titer should then be repeated monthly for at least
6 months to 1 year before the patient is released from close medical supervision.
Thereafter, the patient may enter into a routine gynecologic care program.
A gynecologic examination should be done 1 week after evacuation, at which time
blood may be taken for the hCG titer. Estimates of uterine size, presence of adnexal
masses (theca lutein cysts) and presence of vulvar, vaginal, or cervical lesions
should be noted. Unless symptoms develop, the examination may be repeated at 4-
week intervals throughout the observation period. If pre-evacuation chest
radiography has revealed pulmonary metastases, chest radiographs should be
repeated at 4-week intervals until spontaneous remission is confirmed, then at 3-
month intervals during the remainder of the surveillance period.
Effective contraceptive measures should be implemented and maintained throughout

the period of surveillance. Studies have not shown an increased risk of persistent
gestational trophoblastic neoplasia after a molar pregnancy with the use of oral
contraceptives. Therefore, they remain the most widely used method of birth control.
A patient who has entered into spontaneous remission with negative titers,
examinations, and chest radiographs for 6 months to 1 year and who is desirous of
becoming pregnant may terminate contraceptive practices. Successful pregnancy is
the norm, and complications are similar to those of the general population.
Abortion/Miscarriage
ABORTION
An abortion is the spontaneous or induced loss of an early pregnancy. The period of

pregnancy prior to fetal viability outside of the uterus is considered early pregnancy.
Most (following the WHO definition of abortion) consider early pregnancy to end at
20 weeks' gestation or when the fetus weighs 500 grams. In Kenya and most of sub-
Saharan Africa, the age of fetal viability is 28 weeks. Therefore, our definition of
abortion is ‘the loss of a pregnancy before 28 complete weeks of gestation.’
Spontaneous abortion (commonly termed miscarriage in layman language) is

the most common complication of pregnancy and is defined as the passing of a
pregnancy at less than 28 weeks of gestation. It implies the spontaneous loss of an
embryo or fetus weighing less than 500 g. Threatened abortion is bleeding arising
from within the uterus that occurs before the 28th completed week in a viable
pregnancy. The patient may or may not experience pain or cramping; however, there
is no passage of products of conception and no cervical dilation. Complete
abortion is the expulsion of all of the products of conception before the 28th
completed week of gestation, whereas incomplete abortion is the expulsion of
some, but not all, of the products of conception. Inevitable abortion refers to
bleeding from within the uterus before the 28th week, with dilation of the cervix but
without expulsion of the products of conception. The term missed
abortion describes a nonviable pregnancy that has been retained in the uterus
without cervical dilation and without the spontaneous passage of products of
conception. In septic abortion, embryonic or fetal demise has occurred, and
intrauterine infection has developed, which has the potential risk of spreading
systemically.
Although the true incidence of spontaneous abortion is unknown, approximately 15%
of clinically evident pregnancies and up to 50% of chemically evident pregnancies
end in spontaneous abortion. Eighty percent of spontaneous abortions occur before
12 weeks’ gestation.
The incidence of abortion is influenced by the age of the mother and by a number of
pregnancy-related factors, including the number of previous spontaneous abortions,
a previous intrauterine fetal demise, and a previous infant born with malformations or
known genetic defects. Additionally, chromosomal abnormalities in either parent,
such as balanced translocations, and medical comorbidities, such as thyroid disease
and diabetes mellitus, may influence the rate of spontaneous abortion.
Pathogenesis
An abnormal karyotype is present in as many as 50% of spontaneous abortions
occurring during the first trimester. The incidence decreases to 20–30% of second-
trimester losses and to 5–10% of thirdtrimester losses. The majority of chromosome
abnormalities are trisomies (56%), followed by polyploidy (20%) and monosomy X
(18%).
Other suspected causes of spontaneous abortion are less common, and these
include infection, anatomic defects, endocrine factors, immunologic factors, and
exposure to toxic substances. In a significant percentage of spontaneous abortions,
the etiology is unknown, even with genetic testing.
Prevention
Some miscarriages can be prevented by early obstetric care and even preconception
care, with adequate treatment of maternal comorbidities such as diabetes and
hypertension, and by protection of pregnant women from environmental hazards and
exposure to infectious diseases.
Clinical Findings
A. Threatened Abortion
Approximately 25% of pregnant women experience first-trimester bleeding. In most
cases, this bleeding is caused by implantation into the endometrium. The cervix
remains closed, and slight bleeding with or without cramping may be noted.
Resolution of the bleeding and cramping carries a favorable prognosis; however,
these women are at increased risk for subsequent miscarriage. First trimester
bleeding has also been associated with preterm premature rupture of membranes
and preterm labor. Other causes, such as ectopic pregnancy and molar gestation,
should also be considered.
B. Inevitable Abortion
Bleeding with cervical dilation, often with back or abdominal pain, indicate impending
abortion. Unlike an incomplete abortion, the products of conception have not passed
from the uterine cavity.
C. Incomplete Abortion
Incomplete abortion is defined as the passage of some but not all of the products of
conception from the uterine cavity. Bleeding and cramping usually continue until all
products of conception have been expelled. In general, severe pain and heavy
bleeding occur and often require medical evaluation.
D. Complete Abortion
In a complete abortion, all of the products of conception have passed from the
uterine cavity and the cervix is closed. Slight bleeding and mild cramping may
continue for several weeks.
E. Missed Abortion
Missed abortion is defined as a pregnancy that has been retained within the uterus
after embryonic or fetal demise. Cramping or bleeding may be present, but often
there are no symptoms. The cervix is closed, and the products of conception remain
in situ.
F. Anembryonic Pregnancy
Anembryonic pregnancy (previously called blighted ovum) is an ultrasound
diagnosis. It is a pregnancy in which the embryo fails to develop or is resorbed after
loss of viability. On ultrasound, an empty gestational sac is seen without a fetal pole.
Clinical presentation is similar to that of a missed or threatened abortion: Mild pain or
bleeding may be present; however, the cervix is closed, and the nonviable
pregnancy is retained in the uterus.
Laboratory Findings
A. Complete Blood Count
If significant bleeding has occurred, the patient will be anemic. Both the white blood
cell count and the sedimentation rate may be elevated, even without the presence of
infection.
B. Pregnancy Tests
Falling or abnormally rising serum levels of β-human chorionic gonadotropin (hCG)
are diagnostic of an abnormal pregnancy, either a failed intrauterine gestation or an
ectopic pregnancy.
Ultrasound Findings
Transvaginal ultrasound is an essential diagnostic tool in diagnosing early normal
and abnormal pregnancies. As early as 4–5 weeks of gestation, a gestational sac
may be visualized in the uterus. In a normal intrauterine pregnancy, the sac is
spherical and is eccentrically placed within the endometrium. At 5–6 weeks’
gestation, a yolk sac will be present. In general, a gestational sac with a mean sac
diameter (MSD) of ≥8 mm should contain a yolk sac. Similarly, a gestational sac with
an MSD of >16 mm should also contain an embryo. Pregnancies with a large
gestational sac and no embryo are typically anembryonic gestations and are
managed in a similar manner as a missed abortion. Fetal heart motion is expected in
embryos with a crown to rump length of >5 mm or at 6–7 weeks’ gestation. If a
repeat ultrasound in 1 week does not show embryonic cardiac activity, the diagnosis
of embryonic demise is made.
In threatened abortion, ultrasound will reveal a normal gestational sac and a viable
embryo. However, a large or irregular sac, an eccentric fetal pole, and/or a slow fetal
heart rate (<85 beats/min) carry a poor prognosis. Miscarriage becomes increasingly
less likely the further the gestation progresses. If a viable fetus of 6 weeks or less is
seen on ultrasound, the risk of miscarriage is approximately 15–30%. The risk
decreases to 5–10% at 7–9 weeks’ gestation and to less than 5% after 9 weeks’
gestation.
In an incomplete abortion, the gestational sac usually is irregularly shaped. The
diagnosis of complete abortion is also based on clinical findings. On ultrasound, the
endometrial lining appears thin, and no products of conception are visible within the
cavity. Importantly, a complete abortion is only diagnosed with certainty if a previous
intrauterine gestation was documented on ultrasound. Otherwise, hCG levels must
be followed to confirm the absence of ectopic pregnancy.
When findings on ultrasound are nonspecific, correlation with hCG levels can
improve the ability to distinguish normal and abnormal pregnancies. In a normal
pregnancy, the minimal rise in hCG is 53% over 48 hours. hCG values that rise
slower than expected may be consistent with a failed intrauterine or ectopic
pregnancy. Decreasing levels of hCG are also diagnostic of an abnormal pregnancy.
In spontaneous abortion, the hCG values are expected to drop 21–35% in 2 days
(depending on the initial hCG value). A slower decline is suggestive of an ectopic
pregnancy.
Complications
Severe or persistent bleeding during or after spontaneous abortion may be life-
threatening. The more advanced the gestation, the greater the likelihood of
excessive blood loss. Infection, intrauterine adhesions (Asherman’s syndrome), and
infertility are other complications of abortion.
Perforation of the uterus may occur during procedures to remove retained products
of conception, namely dilatation and curettage (D&C). The rate of perforation during
the first and second trimesters is approximately 0.5% for both induced and
spontaneous abortions. Uterine perforation is more common during D&C performed
in pregnancy because of the soft uterine wall and may be accompanied by injury to
the bowel and bladder, hemorrhage, and infection. Surgical evacuation may also
lead to cervical trauma and subsequent cervical insufficiency.
Treatment of Abortions
Successful management of spontaneous abortion depends on early diagnosis. Every
patient should have a complete history taken and a physical examination performed.
Laboratory studies include a complete blood count, blood type, and cervical cultures
to determine pathogens in case of infection.
If the diagnosis of threatened abortion is made, pelvic rest can be recommended,
although it has not been shown to prevent subsequent miscarriage. Prognosis is
good when bleeding and/or cramping resolve.
If the diagnosis of a missed or incomplete abortion is made, options include surgical,
medical, or expectant management. In the past, surgery was the standard of care
because of concern that medical or expectant management would lead to higher
rates of retained pregnancy tissue and subsequent infection. More recently,
expectant or medical management are acceptable alternatives and have even shown
lower rates of infection despite their higher rates of retained products of conception.
These patients also avoid the risks of surgery, including uterine perforation,
intrauterine adhesions, and cervical insufficiency. The advantages of performing a
manual vacuum aspiration (MVA) include convenient timing and low rates of retained
products of conception.
Expectant management allows the spontaneous passage of products of conception
and avoids risks of surgery. Risks and side effects include unpredictable timing until
the abortion is completed with the possibility of significant pain and bleeding,
occasionally requiring emergent dilatation and curettage (D&C) or MVA. Expectant
management also has the highest rates of retained pregnancy tissue, necessitating
treatment with misoprostol (prostaglandin E1) or MVA.
Patients who choose medical management are given misoprostol, a drug that
induces uterine contractions and expulsion of the products of conception. The risk of
retained products is lower than with expectant management; however, repeat doses
of medication may be needed to complete the abortion. As with expectant
management, timing can be unpredictable, and symptoms of pain and/or bleeding
may necessitate emergent D&C. Expectant or medical management of abortion
assumes that prompt medical evaluation is available. Those options should not be
considered if medical care is not easily accessible.
If the diagnosis of complete abortion is made, the patient should be observed for
further bleeding. If bleeding is minimal, no further treatment is necessary. All
products of conception should be examined and sent for pathologic examination to
confirm an intrauterine pregnancy. If an intrauterine pregnancy was not previously
seen on ultrasound and no pathology specimen is available, serial hCG levels are
followed to confirm spontaneous abortion. If hCG levels decline more slowly than
expected (eg, <21–35%), an ectopic pregnancy or retained products of conception
must be considered. Molar gestation is also a possible diagnosis if hCG levels
plateau or rise abnormally without an intrauterine pregnancy.
If a complete or partial hydatidiform molar pregnancy is diagnosed, surgical
evacuation with suction D&C should be performed. As long as hCG levels are
decreasing and remain undetectable after molar evacuation, there is no need for
chemotherapy. However, if hCG levels start rising, plateau, or are persistent for more
than 6 months, evaluation for malignant postmolar gestational trophoblastic disease
is indicated.
Treatment of Complications
Uterine perforation may result in intraperitoneal bleeding, as well as injury to the
bladder and/or bowel. In many cases, uterine perforation is asymptomatic and goes
unrecognized. When perforation and bowel or bladder injury is suspected or when
heavy bleeding is encountered, laparoscopy and/or laparotomy are indicated to
determine the extent of the perforation and to evaluate for injury to other adjacent
organs.
A Rh-negative patient without antibody in her system should be protected by anti-D

gamma globulin 50 μg or 100 μg intramuscularly in cases of early miscarriage or late
miscarriage respectively within 72 hours. However, anti-D may not be required in a
case with complete miscarriage before 12 weeks of gestation where no
instrumentation has been done.
SEPTIC ABORTION
In septic abortion, infection usually begins as endometritis involving the endometrium

and any retained products of conception. These patients present with fevers, chills,
abdominal pain, vaginal bleeding, and malodorous vaginal discharge. Without
treatment, endometritis may spread beyond the uterus, leading to peritonitis,
bacteremia, and sepsis.
The 2 most common causes of septic abortion are retained products of conception
and bacteria that have been introduced into the uterus via ascending infection.
Pathogens that cause septic abortion are usually those seen in normal vaginal flora
as well as sexually transmitted bacteria. Before performing D&C, screening for
sexually transmitted infections is essential.
In evaluating septic abortion, a complete blood count, urinalysis, endocervical
cultures, blood cultures, and abdominal x-ray to rule out uterine perforation should
be obtained. Ultrasound should be performed to look for retained products of
conception.
Treatment
Treatment of septic abortion involves hospitalization and intravenous antibiotic
therapy. Selection of antibiotic agents should provide for both anaerobic and aerobic
coverage. If retained products of conception are diagnosed, a D&C is indicated.
RECURRENT/HABITUAL MISCARRIAGE
Recurrent miscarriage is defined as 3 or more consecutive pregnancy losses

before 28 weeks of gestation, each with a fetus weighing less than 500 g. Recurrent
pregnancy loss affects up to 5% of couples, often with no identifiable cause. The
prognosis for a successful subsequent pregnancy correlates with the number of
previous miscarriages. The risk of spontaneous abortion in a first pregnancy is
approximately 15%, and this risk is at least doubled in women experiencing recurrent
pregnancy loss.
Overall, the prognosis after repeated losses is good, with most couples having an
approximately 60% chance of a viable pregnancy. The table below shows the
evaluation and management of recurrent early pregnancy loss:
Hyperemesis Gravidarum (HEG)
HYPEREMESIS GRAVIDARUM
Nausea and vomiting in pregnancy are extremely common; 70–80% of women

experience these symptoms early in their pregnancy. Mild to moderate nausea and
vomiting are especially common in pregnant women until approximately 16 weeks’
gestation.
Hyperemesis gravidarum (HEG) is defined as unexplained intractable nausea,

retching, or vomiting beginning in the first trimester, resulting in dehydration,
ketonuria, and typically a weight loss of more than 5% of prepregnancy weight.
Severe HEG requiring hospital admission occurs in 0.3-2% of pregnancies.
Etiology
The pathogenesis is largely unknown, with possible contributing factors being

increased levels of human chorionic gonadotropin (hCG), estradiol, and possible
progesterone. It is more common among younger mothers and those with a history
of motion sickness, migraines, and nausea and vomiting associated with oral
contraceptives. It is more commonly seen in women carrying multiple gestations, and
patients with siblings or a mother with HEG are more likely to be affected.
Other factors that increase the risk for admission include hyperthyroidism, previous
or concurrent molar pregnancy, diabetes, gastrointestinal illnesses, some restrictive
diets, and asthma and other allergic disorders. An association of Helicobacter pylori
infection has been proposed, but evidence is not conclusive. Chronic marijuana use
may cause the similar cannabinoid hyperemesis syndrome. And for unknown
reasons—perhaps estrogen related—a female fetus increases the risk by 1.5-fold.
Symptoms & Signs

HEG is associated with severe nausea and vomiting that may result in dehydration,
weight loss, and frequently social isolation and negative impacts on relationships
with family and friends. Patients with HEG, rather than nausea and vomiting of
pregnancy, tend to have an earlier onset and longer duration. Excess salivation
(ptyalism) may also be seen in a subset of women with HEG.
On examination features of dehydration and ketoacidosis may be present such

as: dry coated tongue, sunken eyes, acetone smell inbreath, tachycardia,
hypotension, rise in temperature may be noted, jaundice is a late feature.
Complications
Maternal complications of HEG can include Wernicke’s encephalopathy (due to

thiamine deficiency), acute tubular necrosis/acute kidney injury (due to severe
dehydration), central pontine myelinolysis, Mallory-Weiss tear of the esophagus,
pneumomediastinum, and splenic avulsion. Additionally, significant psychological
burden of the disease has been reported, with depression, anxiety, and lost work
frequently seen among those with persistent or severe HEG. Fortunately, no clear
fetal complications have been associated with HEG. Fetal risks may be due to low
birth weight.
Diagnosis
The pregnancy is to be confirmed first. Suppressed thyroid-stimulating

hormone/elevated free thyroxine and elevated liver enzymes, bilirubin, amylase, and
lipase may all be noted in patients with severe nausea and vomiting; these are
transiently abnormal and resolve with improvement of HEG. Other initial laboratory
studies in the evaluation of women with HEG are:
v Urinalysis for ketones and specific gravity
v Serum levels of electrolytes and ketones
v Urine culture
v Calcium level
v Hematocrit level
Differential Diagnoses
The differential diagnosis for late (onset after 9 weeks gestation) HEG should include
gastroenteritis, gastroparesis, biliary tract disease, hepatitis, acute febrile infection,
peptic ulcer disease, pancreatitis, appendicitis, pyelonephritis, ovarian torsion,
diabetic ketoacidosis, migraines, drug toxicity or withdrawal, psychological
conditions, acute fatty liver of pregnancy, and preeclampsia.
Management
Initial management of pregnant women with HEG should be conservative and may
include reassurance, dietary recommendations and support. Dietary modifications in
patients with HEG or morning sickness may include the following:
Ø Eat when hungry, regardless of normal meal times
Ø Eat frequent small meals
Ø Avoid fatty and spicy foods and emetogenic foods or smells. Increase intake of
bland or dry foods.
Ø Eliminate pills with iron
Ø High protein snacks are helpful
Ø Crackers in the morning may be helpful
Ø Other suggested foods include herbal teas containing peppermint or ginger, other
ginger-containing beverages, broth, unbuttered toast, gelatin or frozen desserts.
If pharmacologic therapy is necessary, treatment is given using the algorithm below

that balances safety and efficacy:
If medications and outpatient hydration fail or if severe electrolyte disturbance
persist, inpatient admission for IV hydration may be necessary. In some refractory
severe cases of HEG, if maternal survival is threatened, or if HEG is causing severe
physical and psychological burden, termination of pregnancy should be considered.
Prognosis
More than 50% of women have resolution of symptoms by 16 weeks of gestational
age and 80% by 20 weeks. However, approximately 10% will be affected to some
degree with severe nausea and vomiting for the duration of the pregnancy. HEG has
been shown to recur in up to 80% of subsequent pregnancies, although earlier
aggressive medical therapy prior to significant symptoms has been demonstrated to
reduce both the severity and recurrence rate overall in future pregnancies.

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REPRODUCTIVE HEALTH

Unit one Content..

Topic one: Standards of Reproductive health care in Kenya, Policies and

 · Reproductive Health is a state of complete physical, mental,

Basic Elements in Reproductive Health

 · Ability - to reproduce, regulate fertility and enjoy healthy relationships

Components of Reproductive Health

o · Reproductive health is a right

 · Kenya has made steady progress in improving reproductive, maternal and

1. sub-optimal functioning of the health system with uneven

o · Sociocultural and economic barriers and constraints in physical

Status of Key Indicators

Key indicators KDHS KDHS Sub-Saharan

currently married women (%)

Direct Causes of Maternal Mortality

 These result from obstetric complications of pregnancy, labour and the

o Complications of abortion and

Causes of Maternal Morbidity

 Underlying Causes of Maternal & Neonatal Mortality (The Three Delays)

 Risk factors affecting maternal health

Causes of Maternal Morbidity

 Underlying Causes of Maternal & Neonatal Mortality (The Three Delays)

 Risk factors affecting maternal health

The Kenya Maternal and Newborn Health Model (2009)

The Kenya Maternal and Newborn Health (MNH) Pillars

 To ensure effective and efficient service delivery, the skilled attendant

Community Action, Partnerships

 Involving community members (particularly women and their families,

Male Involvement and Participation

 it is evident that for successful programme implementation, male participation

Equity for All

 Rights based perspective helps legitimize prioritization of women’s health.

Emergency Obstetric Care

 Emergency Obstetric Care refers to a set of minimal health care elements,

 Comprehensive Emergency Obstetric Care

Policies and initiatives related to Reproductive health

THE SAFE MOTHERHOOD INITIATIVE (SMI)

Summary of SMI Events

 International Conference for Population and Development (ICPD)

International Conference For Population and Development (ICPD)

National Reproductive Health Policy 2007

The KEPH Life-Cycle Cohorts

 · They are delineated in the NHSSP II as follows

Levels of Care in KEPH

 · The KEPH approach is not only limited to a definition of the target

o Level 6 : tertiary hospitals

o Level 5: secondary hospitals

o Level 4: primary hospitals

o Level 3: health centres,

o Level 2: dispensaries / clinics

 · As a result of the implementation of the constitution of Kenya 2010,

Annual Operational Plans (AOPs)

The Community Strategy

 The community-based approach, is the mechanism through which households

Assignment: study the following policies/initiatives

Millennium Development Goals (MDGs)

 MDGs were set by all Government leaders at the UN Millennium Summit,

Why the MDGs ?

 The 1990s was a decade of faltering progress on:

Millennium Development Goals (MDGs)