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Pathophysiology of reproduction – sterility, infertility

Lecture Outline
The Basics
Gametogenesis
Gender determination
Female Reproductive Pathophysiology
Ovarian Cycle
Uterine Cycle
Hormonal control and changes
Disorders
Male Reproductive Pathophysiology
Infertility

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The Basics
Gametogenesis
Gametes are produced during Meiosis I & II
Meiosis function
Production of 4 haploid (n) gametes from each diploid oögonium (2n) or spermatogonium (2n)
Differences between ♂ (male) and ♀ (female) gamete development
♂
continuous development & production of sperm from onset of puberty until….?
stem cells are retained
Sperm are motile and contain very little cytoplasm
♀
the entire complement of dictyate primary oocytes are formed during development with 10-20
continuing development during each ovarian cycle
Oocytes are surrounded by follicular cells – forms ovarian follicle
stem cells are exhausted
oocytes are among the largest cells and are non-motile

The Basics
Gametogenesis
Sperm Production
During development germ cells are produced
Remain quiescent until puberty
Actions of hormones from pituitary, sertoli cells and Leydig cells
At puberty some spermatogonia will
Undergo mitosis continuously
Enter into meiosis
This ensures a continuous supply of spermatogonia

The Basics
Gametogenesis
Process of sperm production involves three stages
1.Spermatocytogenesis
produces secondary spermatocytes from spermatogoium
2.Spermatidogenesis
stage where meiosis I & II occur
results in spermatid formation
3.Spermiogenesis
final stage of sperm development
spermatid becomes a motile spermatozoa during spermiation

The Basics
Gametogenesis
Spermiation
The spermatozoa that are formed are initially unable to move.
The flagella must become motile
Not used however until ejaculated
Prior movement through the male reproductive tract is via peristalsis
End result!

The Basics
Gametogenesis
Oogenesis
Results in formation of secondary oocyte which is released during ovulation
If no fertilization occurs, meiosis II will not occur.
Stages of oogenesis
1.Oocytogenesis
Forms oögonia
During fetal development starting at week 10 and completing around birth
Results in formation of primary oocytes (~1/2 million)
2.Ootidogenesis
Results in the formation of secondary oocytes
These are dictyate in prophase I
3.Formation of ovum (if fertilization occurs)

The
Basics
Gametogenesis

The Basics
Gender Determination
Chromosomes determine gender
23 donated by egg (n)
23 donated by sperm (n)
Syngamy
The fusion of gametes to form a zygote
Consists of
plasmogamy
union of cell membranes and cytosol
Karyogamy
union of genetic material
Autosomes: 44 or 22 pair
Sex chromosomes: 2 or 1 pair
XX chromosomes = female
XY chromosomes = male
What happens if karyogamy of sex chromosomes is different?

The Basics
Gender Determination
Non-disjunction during meiosis I or II
Monosomy or polyploidy
XO (no Y chromosome, or second X)
Turner’s syndrome
Phonotypical female
What about YO monosomy?

The Basics
Gender Determination
Non-disjunction during meiosis I or II
Polyploidy
The incomplete separation of homologues during meiosis results in a zygote with too many
chromosomes
Regarding the sex chromosomes, it may be
XXY (47 chromosomes total)
Klinefelter syndrome: Male sex organs; unusually small testes, sterile. Breast enlargement and
other feminine body characteristics. Normal intelligence.
XYY
Jacob’s syndrome: Individuals are somewhat taller than average and often have below normal
intelligence. At one time (~1970s), it was thought that these men were likely to be criminally
aggressive, but this hypothesis has been disproven over time.
XXYY – male and very rare (48 chromosomes)
XXX (Trisomy X)
Individuals are female normal, undistinguishable except for by karyotype.

The Basics
Gender Determination
The embryo exhibits gender bipotential
Around week seven of fetal development the SRY (Sex-determining Region of Y chromosome) gene
becomes activated
The SRY directs the bipotential gonads
The absence of this on the X chromosome causes the gonads to develop into ovaries
Ovaries then produce further gender biased hormones
The presence of this gene and its products causes the gonads to descend and develop into testes
Testes then produce further gender biased hormones
Translocation of the gene to X chromosome results in an  XX individual (genotype) but with XY
characteristics (phenotype)

The Basics
Gender Determination
Effects of SRY on sex organ development

The Basics
Gender Determination
Indirect effects of SRY on male and female genital development

Lecture Outline
The Basics
Gametogenesis
Gender determination
The Pituitary-Gonad Axis
Female Reproductive Physiology
Ovarian Cycle
Uterine Cycle
Hormonal control and changes
Male Reproductive Physiology

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The Pituitary-Gonad Axis



Lecture Outline
The Basics
Gametogenesis
Gender determination
The Pituitary-Gonad Axis
Female Reproductive Physiology
Ovarian Cycle
Uterine Cycle
Hormonal controls & changes
Male Reproductive Physiology

>

Female Reproductive Physiology
Basics
The hypothalamus-pituitary-gonad axis controls the required physiologic changes that occur both in
the ovaries and in the uterus of the menstrual cycle.
The Menstrual Cycle
Duration
Approximately 28 days (ranges 24 – 35 days)
Starts with the removal of the endometrium & release of FSH by the anterior pituitary
The ovarian cycle
Development of ovarian follicle
Production of hormones
Release of ovum during ovulation
The uterine cycle
Removal of endometrium from prior uterine cycle
Preparation for implantation of embryo under the influence of ovarian hormones

Female Reproductive Physiology
The Cycles
Three Phases of the Ovarian Cycle
Follicular phase
Ovulation phase
Luteal phase
Three Phases of the Uterine Cycle
Menses
Proliferative Phase
Secretory Phase
These ovarian and uterine phases are intimately linked together by the production and release of
hormones

Female Reproductive Physiology
The Cycles
Hormonal control of the ovarian cycle

Female Reproductive Physiology
The Cycles
Hormonal control of the uterine cycle

Female Reproductive Physiology
All together


Female Reproductive Physiology
Fertilization Effects
What happens if fertilization occurs?
Uterine endometrium is maintained by
First the release of progesterone from the corpus lutem,
then the release of hCG (human chorionic gonadotropin) which maintains the corpus luteum until the
7th week,
From 7th week on, the placenta produces progesterone which continues to maintain the endometrium &
the corpus luteum degenerates
Placenta also produces estrogen and progesterone which at high levels blocks GnRH
Estrogen is also involved in breast development
Progesterone is also involved in uterine maintenance and relaxation (prevents premature
contractions)
Placenta also produces hPL (human placental lactogen)
Implicated in breast development and milk production
Though determined not the only factor as lack of hPL has no ill effects
More important is the role hPL plays in fetal nutrition by altering maternal glucose and fatty acid
metabolism

Female Reproductive Physiology
Fertilization Effects
What changes occur to allow parturition?
Increasing levels of corticotropin-releasing hormone (CRH) from the placenta a few weeks prior to
delivery
Early deliveries have been linked to early elevated levels of CRH
During delivery
progesterone levels drop off
Oxytocin levels rise
Oxytocin receptors on the uterus are upregulated during gestation
Inhibin levels increase
Relax the cervix and ligaments of the pelvis
Allows for increased stretch of the cervix which triggers additional oxytocin which triggers
stronger uterine contractions which increase stretch of the cervix which triggers oxytocin which
triggers stronger uterine contractions which increases stretch of the cervix which increases
oxytocin release which increases uterine contractions which increases stretch on cervix which….

Pathophysiology of female reproduction
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Infertility definition
Infertility is defined as the inability of couples to have a baby after one year of regular
unprotected intercourse, affecting 10–15 percent of couples. According to the latest WHO
statistics, about 50–80 million people worldwide suffer from infertility. Large-scale studies have
shown that about half of all cases of infertility occur due to female factors, 20 to 30 percent
male factors, and 20 to 30 percent due to common causes of both gender. Recent meta-analysis
studies by researchers show that male’s factors are present in 20–70 percent of infertility cases.
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PATHOLOGICAL PROCESSES, THEIR IMPLICATIONS, AND THERAPEUTIC OPTIONS
A. Folliculogenesis
1. Genetic
Premature ovarian insufficiency (POI) occurs in ∼1% of women and is defined as the cessation of
menstrual cycles under 40 years of age in the presence of an elevated serum FSH measured on two
separate occasions. The causes may be genetic, environmental, infective (subsequent to mumps
infection), associated with autoimmune conditions, metabolic [due to biochemical damage in the
presence of galactossaemia], and subsequent to cancer therapy or surgery; however, in the majority
of cases no cause is determined.
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Turner syndrome
Possibly the most common genetic cause of POI is Turner syndrome characterized by the loss of all,
or part of an X chromosome, occurring in ∼1 in 3,000 female births. Approximately half due to X
chromosome monosomy and the majority of the remainder due to mosaicism. This is a condition with
several phenotypic features characterized by short stature, cardiac and renal abnormalities,
hypothyroidism, webbed-neck, and otological and ophthalmological abnormalities are all common in
childhood.
The ovarian insufficiency commonly found in this condition relates to disruption of the BMP15 gene
locus located at Xp11.2, within a critical region related to ovarian failure.
Spontaneous puberty occurs in approximately one quarter of girls, more commonly in mosaics;
however, premature ovarian failure is universal.
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B. Ovulation
1. Hypogonadotrophic hypogonadism
Insufficient ovarian stimulation with gonadotrophins LH and FSH results in the condition of
hypogonadotrophic hypogonadism (HH), either due to insufficient hypothalamic GnRH stimulation of
the pituitary or due to insufficient secretion due to pituitary compromise. After exclusion of
excessive exercise, extreme stress, or an eating disorder, and after ensuring pituitary function,
other than secretion of LH and FSH, is normal, and pituitary imaging is normal the condition is
considered idiopathic HH (IHH). The most common cause of GnRH insufficiency is the failure of
migration of the GnRH secretory neurons to the forebrain which may also result in olfactory
disorder (Kallman's syndrome); in the absence of olfactory, the condition is described as normosmic
IHH.
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2. Hyperprolactinemia
Other central causes of HH can be caused by systemic disease, medication (such as opioids and
psychotropic medication), hypothalamic or pituitary compression, or infiltration; however, the most
common cause is probably hyperprolactinemia. Hyperprolactinemia may be caused by physiological
states such as pregnancy, breastfeeding, stress, exercise, and some medications as well as patients
with chronic hypothyroidism. Kidney disease may predispose a patient to hyperprolactinemia due to
reduced clearance and altered prolactin metabolism. As prolactin secretion is suppressed by
hypothalamic dopamine secretion, interruption or compression of the pituitary stalk by a
non-prolactin-secreting pituitary tumor will lead to hyperprolactinemia.
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3. Polycystic ovary syndrome
The polycystic ovary syndrome (PCOS) is a collection of signs and symptoms related to ovarian
dysfunction, found within a phenotypically heterogeneous group of women. It is classically
described by the Rotterdam criteria as a syndrome consisting of two of three criteria related to
infrequent or absent ovulation, a morphological description of the ovaries by ultrasound
assessment, and hyperandrogenism. Other groups suggest that the excessive androgen secretion is the
most significant underlying pathology as this is believed to lead to ovarian dysfunction and the
longerterm metabolic consequences these women experience, and they consequently adopt a more
stringent definition of PCOS.
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PCOS
It is believed that oocyte developmental competence and the embryos resulting from fertilization
are altered in women with PCOS, compared with women without PCOS. There are multiple serum and
follicular factors that are reportedly altered in women with PCOS that may be responsible for this
poor embryonic development and reduced implantation) although it is not clear whether this is
associated with an increase in the rate of embryo aneuploidy. Not only is the systemic and
follicular environment different in PCOS, the gene expression profile of oocytes derived from women
with PCOS are distinctly different.
These genes relate to signal transduction, transcription, RNA and DNA processing, and the
regulation of the cell cycle.
Of particular importance in the acquisition of oocyte developmental competence is GDF-9 expression,
which is reduced in the oocytes of women with PCOS.
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Ovarian hyperstimulation syndrome
OHSS is triggered by the systemic release of inflammatory cytokines, particularly VEGF which leads
to endothelial cell damage and increased vascular permeability and the rapid development of
ascites, and potentially pleural and pericardial effusion. OHSS is a significant cause of morbidity
and in Australia and New Zealand is reported to complicate 0.6% of IVF cycles. Adjuvant therapies
that have been demonstrated to significantly reduce the incidence are the use of an GnRH antagonist
for pituitary downregulation, particularly with the use of an GnRH agonist trigger, the VEGF
receptor blocker cabergoline, and by combing the ovarian stimulation with metformin administration.
Other strategies include using low doses of gonadotrophin drugs for stimulation or omitting
completely, cancelling the IVF cycle prior to oocyte retrieval, omitting the gonadotrophin drugs
for a few days–“coasting” and not proceeding to an embryo transfer (so-called “freeze-all”
approach). A further innovation is to use a different stimulation approach called in vitro
maturation of oocytes (IVM) where no final trigger for oocyte maturation is administered prior to
oocyte retrieval and oocyte maturation is performed in the laboratory with some centers reporting
similar pregnancy rates as their standard IVF approach  without the risk of OHSS. The evidence for
some of the therapeutic interventions employed for women with OHSS is not robust and hence for the
prevention of OHSS clinicians are advised to follow guidelines provided by consensus statements
after systematic review of the literature.
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C. Fallopian Tube Function
1. Disorders of ciliary action
2. Inflammatory disorders: endometriosis and infection
3. Other gynecological conditions
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D. Implantation
1. Systemic
It is generally believed that severe systemic illness, such as sepsis or severe renal disease, will
prevent embryonic implantation, although infection is an unusual cause of early pregnancy failure.
A comprehensive list of all systemic conditions that have been demonstrated to have a significant
negative influence on embryonic implantation is difficult to compile; however, conditions such as
unstable diabetes, subclinical hypothyroidism, periodontal disease, and uncontrolled celiac disease
have been demonstrated to reduce rates of conception, and it is believed that low serum vitamin D
and active autoimmune conditions are also associated with a reduced chance of conception, and
strategies to control these conditions may improve conception chances. Due to their high prevalence
and ease of correction of the abnormality, celiac disease and subclinical hypothyroidism are
discussed further.
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2. Celiac disease
In a population of women experiencing unexplained infertility or recurrent miscarriage, celiac
disease is five times more prevalent than in the general population. A meta-analysis of patients
with celiac disease found that the risk of miscarriage is 40% greater with increased risks in the
pregnancy for growth restriction and premature delivery, and the effect is tempered if a
gluten-free diet is observed.
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3. Subclinical hypothyroidism
Overt thyroid disorder must be appropriately managed prior to conception; however, more subtle
perturbations in thyroid function are also associated with reproductive disorder. Approximately 1
in 25 women have subclinical hypothyroidism, and thyroid antibodies are present in up to one in
eight of women. The presence of thyroid antibodies in a woman with normal thyroid function is
believed to be associated with difficulty conceiving, recurrent implantation failure of embryos,
and early pregnancy loss, potentially due to an unrecognized thyroid hormone deficiency or due to a
potential autoimmune cause. Treatment of subclinical hypothyroidism is believed to potentially
improve embryo development and is recommended for women prior to conception; however, whether to
treat a woman prior to conception, who is euthyroid in the presence of thyroid antibodies, is
contentious.
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4. Thrombophilia
It has been unclear whether an inherited thrombophilia leading to microthrombi within the decidua
are associated with implantation failure of the embryo as the intervillous spaces are not developed
until 10 wk of gestation. Although it is tempting to speculate that perturbations in the clotting
system may influence implantation and early embryonic development, for example, factor XII gene
expression is increased in endometrial stromal cells during in vitro decidualization, this is
believed to lead to an activation of the kallikrein-kininogen-kinin system during the implantation
of human embryos.
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5. Natural killer cells
There has been substantial interest in the assessment of blood and uterine natural killer cell
populations in women with poor embryo implantation. Evidence would appear to suggest that women
with unexplained implantation failure may have an abnormal population of natural killer (NK) cells
in the blood and in the endometrium in the mid-luteal phase of the menstrual cycle, although
strategies to improve the systemic and endometrial environment to facilitate conception have not
been proven.
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6. Endometrial and myometrial (endometriosis, leiomyomas, hydrosalpines, PCOS, obesity, endometrial
polyps)
As evidenced by IVF success rates, embryonic implantation potential is decreased in the presence of
endometriosis, leiomyomas, dilated fallopian tubes (hydrosalpines), and PCOS and have been linked
to reduced endometrial expression of HOXA10 and HOXA11. In addition, women with endometriosis have
reduced expressions of endometrial integrin αvβ3 and LIF, hypermethylation leading to silencing of
the HOXA10 gene and endometrial progesterone resistance leading to a reduction in the chance of
conception which may potentially be improved by surgical intervention or by use of prolonged
downregulation with a GnRH analog prior to the initiation of an IVF cycle. Similarly to integrin
αvβ3 expression normalizing with surgical intervention in the presence of endometriosis, the
surgical removal of hydrosalpinges (salpingectomy) will restore the expression of integrin αvβ3 and
LIF improving conception.
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7. Embryonic
With the advent of genetic testing of blastomeres from embryos of women undergoing IVF treatment,
it has become evident that a significant cause of embryos failing to implant is due to chromosomal
rearrangements developing within the embryo as described above. With the ability to perform a
low-resolution genome-wide survey of either single blastomeres from a three-day-old embryo or by
the study of several cells from the trophectoderm of a five- or six-day-old blastocyst, it has
become evident that in addition to the common occurrence of aneuploidy within the embryo, usually
arising during meiosis, the embryo is predisposed to segmental chromosomal imbalances which arise
during programmed DNA breakage and repair by homologous recombination during prophase I of meiosis.
These rearrangements may lead to a failure to develop and implant, but also lead to phenotypic
variability and hence ultimately genome evolution [for a detailed description of the origin of
chromosomal rearrangement, see Voet et al.]. Hence, in IVF programs the majority of apparently
morphologically normal embryos fail to implant as aneuploidy is such a frequent occurrence,
occurring more frequently in an older woman, and a woman with a history of failed embryonic
implantation.
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F. Early Pregnancy Failure
The causes of early pregnancy failure overlap with the causes of embryo implantation failure and
hence are not reiterated here. The discussion is limited to a description of possible associations
of genetic variations which may influence implantation and predispose to early pregnancy loss.
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1. Genetic polymorphisms
Genetic polymorphisms associated with recurrent early pregnancy loss suggest that genes regulating
oxidative stress may be involved . Single nucleotide polymorphisms of genes associated with oxygen
free radical metabolism, ABCB1, COMT, GPX4, and OGG1, have been reported to lead to a doubling of
the risk of recurrent miscarriage. In addition, polymorphism of genes that regulate the complement
cascade, such as membrane cofactor protein and C4 binding protein, have a putative role in
recurrent early pregnancy loss. HLA-G, part of the major histocompatibility complex class I group,
has been linked to the success of IVF and is believed to have an immune modulatory role, and
potentially lower expression of HLA-G is associated with reduction in embryo implantation and early
pregnancy failure.
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IV. LIFESTYLE INFLUENCES INFLUENCING OVULATION, FALLOPIAN TUBE FUNCTION, IMPLANTATION, AND
MISCARRIAGE
A. Delayed Childbearing
1. Ovulatory frequency
2. Oocyte quality
a)Aneuploidy
b)oocyte mitochondrial function
c)embryo metabolism
d)epigenetic alterations.
3. Fallopian tube function
B. Dietary Restriction and Over-exercise
C. Stress
D. Obesity
E. Cigarette Smoking
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Stress
Due to central neuronal corticotrophin releasing hormone (CRH) projection to GnRH cells and
CRH-induced β-endorphin inhibition of GnRH secretion, stress may exert a modulating effect on
subsequent pituitary LH and FSH pulsatility, which may be overcome by modified behavior restoring
ovulation. Higher daily reported stress levels in a cohort of normal healthy women were associated
with a reduction in serum estradiol, LH, and luteal phase progesterone concentrations as well as a
predisposition to anovulation. Furthermore, while it is known that an elevated serum cortisol
concentration is related to FHA, women with FHA who resume ovulation have serum cortisol
concentrations similar to eumenorrheic women, suggesting that by reducing stress levels by
therapeutic interventions normal ovulation may return . The Nurses' Health Study demonstrated that
working longer hours (over 40 h/wk) and also lifting heavy loads were associated with increased
time to conceive, suggesting a relation to tiredness or stress may impact upon conception.
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Lecture Outline
The Basics
Gametogenesis
Gender determination
The Pituitary-Gonad Axis
Female Reproductive Physiology
Ovarian Cycle
Uterine Cycle
Hormonal control and changes
Male Reproductive Physiology

>

Male Reproductive Physiology
Basic Functions
Function
Produce, maintain & transport viable spermatozoa
Testes
Epididymis
Ductus deferens
Accessory glands
Prostate
Seminal vesicles
Bulbourethral glands
Hormone production that
develops secondary sexual characteristics
Involved in feedback mechanisms relating to spermatogenesis

Male Reproductive Physiology
Testes
Site of Sperm production
Divided into lobules, each with seminiferous tubules.
Seminiferous tubule functions to
Maintain environment for spermatogonia by the basal lamina and the Sertoli cells
Sertoli cells separate the lumen from the basal lamina and create a blood-testis barrier
Creates three compartments
Lumen – low glucose, high K+
& steroid hormones
Basal compartment – the baso-
lateral side of the sertoli cells &
containing the developing
spermatogonia
Interstitial fluid space – below the
basal lamina and contains the Leydig
cells
Produce hormones/paracrines
From Sertoli cells
From Leydig cells

Male Reproductive Physiology
Testis
Sertoli cells
Produce hormones & paracrines involved with control of hypothalamus-pituitary-gonad axis and the
testes directly
Anti-Müllerian Hormone (AMH)
Secreted during embryogenesis
Prevents development of the Müllerian ducts
Inhibin & activin
Regulate FSH release from anterior pituitary
inhibin decreases FSH release
activin increases LH function & increases FSH release
Androgen Binding Protein (ABP)
Binds to testosterone and DHT, reduces the loses due to diffusion resulting in an increase in
testicular testosterone levels
Estradiols & Aromatase
Support spermatogenesis

Male Reproductive Physiology
Testis
Sertoli cells, cont…
GDNF (glial derived neurotrophic factor) & ERM transcription factor
Maintenance of the stem cell line
Leydig cells
Produce androgens
testosterone, androstenedione and dehydroepiandrosterone (DHEA)
Increase spermatogenesis
Influence secondary sexual characteristics
Stimulated to produce androgens by luteinizing hormone (LH)
FSH increases the response to LH by Leydig cells

Male Reproductive Phsyiology
Testes


Male Reproductive Physiology
Testes
Spermatogenesis Hormonal Control Flow Chart

[USEMAP]
What does testosterone do ?
A. It or its DHT metabolite bind to Androgen Receptors [AR]
1. ANDROGENS
1. Cytosolic –GENOMIC Action –mediates cell growth & differentation in AR responsive tissues;
reproductive, those of 2ndry male sex characters, muscles …
* Binding & Activation
* Nuclear translocation
* Dimerization on SRE
* Gene Transcription
* mRNA Translation
* New Protein Formation
TESTOSTERONE
PROTEIN
Like all other steroid hormones they act on;

C:\Users\Administrator\Pictures\AND.jpg
2. Membranous –
NON-GENOMIC Action – mediates rapid responses –  on some brain, CVS, T cells functions
B. It aromatize to estradiol and binds to Estrogen Receptors [ER]
http://www.clevelandclinicmeded.com/medicalpubs/diseasemanagement/endocrinology/male-hypogonadism/i
mages/hypercalcemiafig2_large.jpg
Like all other steroid receptors
CNS; -ve loop
CVS;  protection
AR
AR
ER
  CNS; libido
Estradiol rather than testosterone; 1.Responsible for feedback inhibition on hypothalamus
(specially –ve LH secretion)
2. Induce maturation of cartilage
– leading to closure of
 epiphyses & conclusion
 of growth.
3. Some CVS protective actions
1. ANDROGENS

1. ANDROGENS
ACTIONS DIVIDED INTO
¡Anabolic Steroids
Not used in infertility
¡ Testosterone & Synthetic Androgens

Male Reproductive Physiology
Accessory Gland Function
Job of the accessory glands is to
Secrete seminal fluid (99% of semen volume)
Components of seminal fluid
Mucus
Water
Nutrients
Buffers
Enzymes
Prostaglandins
Zinc?
Accessory Glands
Prostate
Seminal vesicles
Bulbourethral glands

Male Reproductive Physiology
Accessory Gland Function
Seminal Fluid Components, Function and Location (source)
From Table 26-3

Male Reproductive Physiology
The sexual response
Remember
Function of the reproductive system is to reproduce
Males contribution is
Deliver viable sperm into the vagina
Requires a complex neural reflex – the erection reflex
Creates changes in vascular condition within the penile arterioles
Initiated by erotic stimuli (visual, auditory, tactile, cerebral)
the parasympathetic division of the ANS causes vasodilation of the penile arterioles
Erectile tissue fills with blood creating an erection

Male Reproductive Physiology
The sexual response
Remember
Function of the reproductive system is to reproduce
Males contribution is
Deliver viable sperm into the vagina
Requires a complex neural reflexes
Starts with the erection reflex which creates changes in vascular condition within the penile
arterioles
Initiated by erotic stimuli (visual, auditory, tactile, cerebral)
the parasympathetic division of the ANS causes vasodilation of the penile arterioles
Erectile tissue fills with blood creating an erection
Emission & Ejaculation during climax
Emission is the movment of sperm from vas deferens into the urethra adding seminal fluid along the
way, this is under sympathetic control
Ejaculation is the expulsion of semen due to strong muscular contractions – this is a spinal reflex

Male Reproductive Pathophysiology
The sexual response
Emission & Ejaculation during climax
Emission is the movement of sperm from vas deferens into the urethra adding seminal fluid along the
way, this is under sympathetic control
Ejaculation is the expulsion of semen due to strong muscular contractions – this is a spinal reflex
Started with the contraction of the bulbospongiosus muscle
Disorders
Erectile dysfunction (ED)
Premature ejaculation
Prolonged ejaculation / anorgasmic

Male infertility
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Male infertility - causes
There are multiple causes for male infertility, which can be broadly classified due to their
general underlying etiology.  These include endocrine disorders (usually due to hypogonadism) at an
estimated 2% to 5%, sperm transport disorders (such as vasectomy) at 5%, primary testicular defects
(which includes abnormal sperm parameters without any identifiable cause) at 65% to 80% and
idiopathic (where an infertile male has normal sperm and semen parameters) at 10% to 20%. These are
broad estimates only as accurate statistics are unavailable due to general underreporting, cultural
factors, and regional variations.  Patients sent to a tertiary referral center are more likely to
have their condition reported, while private patients may never have their data collected.
The causes underlying male infertility are numerous and best categorized by effects at one or more
of the following levels: pretesticular, testicular, and posttesticular.
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Pretesticular causes of male infertility
Hypothalamic Disease
Gonadotropin Deficiency (Kallmann Syndrome)
Kallmann syndrome (1:30,000) is characterized by central hypogonadism, delayed in puberty, and
infertility. Other clinical features include anosmia, small testes and occasionally renal agenesis,
bimanual synkinesia, cleft lip, and dental agenesis. When anosmia is not present, the condition is
termed idiopathic hypogonadotrophic hypogonadism (IHH). The clinical diagnosis of Kallmann syndrome
is confirmed by hormonal assessment revealing low testosterone, low LH, low FSH, and normal
prolactin levels. Infertility is treatable with gonadotropin (LH and FSH) replacement over 12–18
months, which induces sperm in the ejaculate in 80% of men. The condition is inherited as a
familial disorder in one-third of cases and both X-linked and autosomal inheritance patterns have
been described.
Isolated Gonadotropin Deficiencies
These deficiencies are rare. As the result of a partial LH deficit, there is enough LH to stimulate
intratesticular testosterone production and spermatogenesis but insufficient testosterone to
promote virilization. The results are a eunuchoid body habitus, variable virilization, and
gynecomastia. These men usually have normal size testes, but sperm concentration is low. Plasma FSH
levels are normal, but serum LH and testosterone levels are low normal.
With insufficient FSH production by the pituitary, patients are normally virilized, testicular size
is normal, and LH and testosterone levels are normal. FSH levels are uniformly low and do not
respond to stimulation with GnRH. Sperm counts range from azoospermia to severely low numbers
(oligospermia).
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Congenital Hypogonadotrophic Syndromes
Several syndromes may be associated with secondary hypogonadism. Prader–Willi syndrome (1:20,000)
is characterized by obesity, mental retardation, small extremities, and hypogonadism and is caused
by a deficiency of hypothalamic GnRH. The cause of this condition appears to be a single gene
deletion on chromosome 15. Similar to Kallmann syndrome, spermatogenesis can be induced by
treatment with FSH and LH. Bardet–Biedl syndrome is an autosomal recessive form of
hypogonadotrophic hypogonadism that also results from GnRH deficiency. It is characterized by
mental retardation, retinitis pigmentosa, polydactyly, and hypogonadism. The presentation is
similar to Kallmann syndrome but includes obesity and may also be treated with gonadotropin
administration. Cerebellar ataxia can be associated with hypogonadotrophic hypogonadism. Cerebellar
involvement includes abnormalities of speech and gait and these patients can have a eunuchoid
appearance with atrophic testes. Hypothalamic–pituitary dysfunction due to pathologic changes in
cerebral white matter is thought to underlie infertility.
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Pituitary Disease
Pituitary Insufficiency
Pituitary insufficiency may result from tumors, infarcts, surgery, radiation, or infiltrative and
granulomatous processes. In sickle cell anemia, pituitary and testicular microinfarcts result from
sickling of red blood cells potentially leading to both hypogonadism and spermatogenic failure. Men
with sickle cell anemia have decreased testosterone and variable LH and FSH levels.
Beta-thalassemia occurs primarily in patients of Mediterranean or African origin and is caused by
mutations in the beta-globulin that leads to abnormal hemoglobin composition and subsequent red
cell lysis. Infertility results from the deposition of hemosiderin in the pituitary gland and
testes. Similarly, hemochromatosis results in iron deposition within the liver, testis, and
pituitary and is associated with testicular dysfunction in 80% of cases.
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Exogenous or Endogenous Hormones
Estrogens
An excess of sex steroids, either estrogens or androgens, may cause infertility due to an imbalance
of the testosterone estrogen ratio, which is normally 10:1. Liver cirrhosis increases endogenous
estrogens due to augmented aromatase activity within the diseased liver. Likewise, obesity may be
associated with testosterone and estrogen imbalance owing to increased peripheral aromatase
activity in adipocytes. Less commonly, adrenocortical tumors, Sertoli cell tumors, and interstitial
testis tumors may produce estrogens. Excess estrogens cause spermatogenic failure by decreasing
pituitary gonadotropin secretion, thus inducing secondary testis failure.
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Exogenous or Endogenous Hormones
Androgens
An excess of androgens can suppress pituitary gonadotropin secretion and lead to secondary testis
failure. The use of exogenous androgenic steroids (anabolic steroids) by as many as 15% of high
school athletes, 30% of college athletes, and 70% of professional athletes may result in temporary
sterility due to suppression of the normal HPG axis. Treatment includes immediate discontinuation
of steroids and reevaluation of semen quality every 3–6 months until spermatogenesis returns. The
most common reason for excess endogenous androgens is congenital adrenal hyperplasia caused by
21-hydroxylase deficiency. The resultant absence of cortisol synthesis and excessive
adrenocorticotropic hormone production leads to elevated androgenic steroids by the adrenal cortex.
High androgen levels in prepubertal boys result in precocious puberty, with premature development
of secondary sex characteristics and abnormal enlargement of the phallus. The testes are
characteristically small because of central gonadotropin inhibition by androgens. In young girls,
virilization occurs with clitoral enlargement. In cases of classic congenital adrenal hyperplasia
that presents in childhood, normal sperm counts and fertility have been reported, even without
glucocorticoid treatment. This disorder is one of the few intersex conditions associated with
potentially normal fertility. Other sources of endogenous androgens include hormonally active
adrenocortical tumors or Leydig cell tumors of the testis.
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Male infertility
Male infertility contributes to approximately half of all cases of infertility and affects 7% of
the male population. For the majority of these men the cause remains unexplained. Despite a clear
role for genetic causes in male infertility, there is a distinct lack of diagnostically relevant
genes and at least 40% of all cases are classified as idiopathic
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Testicular causes
The Testis
Normal male reproduction requires that the testes have both endocrine (steroid production) and
exocrine (sperm maturation and excretion) function. Both of these functions are under the control
of the HPG axis. Steroidogenesis occurs in the interstitial compartment, where Leydig cells reside.
Spermatogenesis occurs in the seminiferous tubules with the support of Sertoli cells.
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Endocrine Testis
Testosterone is metabolized into two primary metabolites in target tissues: (1) dihydrotestosterone
(DHT) by the enzyme 5-alpha-reductase and (2) estradiol by the enzyme aromatase. DHT is a more
potent androgen than testosterone, and in many tissues, the conversion of testosterone to DHT is
required for androgen action. While aromatase is present in many tissues, adipocytes play a
significant role in the aromatization of testosterone to estradiol. While the mechanisms are still
being elucidated, estradiol appears to have a pivotal role in the regulation of the HPG axis.
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Exocrine Testis
FSH acts primarily on Sertoli cells within the seminiferous tubules to induce the production of a
number of proteins necessary for spermatogenesis, including androgen-binding protein, transferrin,
lactate, ceruloplasmin, clusterin, plasminogen activator, prostaglandins, and several growth
factors. Through these actions, seminiferous tubule growth is stimulated during development, and
sperm production is initiated during puberty and maintained in adulthood.
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Common Genetic Causes
Y Chromosome Microdeletions
Approximately 7% of men with low sperm counts and 13% of men with azoospermia have a structural
alteration in the long arm of the Y chromosome (Yq). The testis-determining region genes that
control testis differentiation are intact, but there may be gross deletions in other regions that
may lead to defective spermatogenesis. The recent explosion in molecular genetics has allowed for
sophisticated analysis of the Y chromosome. At present, three gene sites are being investigated as
putative AZF (azoospermia factor) candidates: AZFa, b, and c. The most promising site is AZFc,
which contains the DAZ gene region. The gene, of which there are at least six copies in this
region, appears to encode a ribonucleic acid (RNA)-binding protein that regulate the meiotic
pathway during germ cell production. Homologs of the DAZ gene are found in many other animals,
including mouse and Drosophila. A quantitative polymerase chain reaction–based assay is used to
test blood for these deletions. In the future, sperm DNA may also be tested as part of a semen
analysis. Since men with these microdeletions can have sperm in the ejaculate, they are likely to
pass them on to offspring if ART is used.
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Klinefelter Syndrome
Abnormalities in chromosomal constitution are well-recognized causes of male infertility. In a
study of 1263 infertile couples, a 6.2% overall prevalence of chromosomal abnormalities was
detected. Among men whose sperm count was <10 million/mL, the prevalence was 11%. In azoospermic
men, 21% had significant chromosomal abnormalities. For this reason, cytogenetic analysis
(karyotype) of autosomal and sex chromosomal anomalies should be considered in men with severe
oligospermia and azoospermia.
Klinefelter syndrome is the most common chromosomal aneuploidy and a common genetic cause of
azoospermia, accounting for up to 14% of cases in some series (overall incidence 1:500 males). The
classic triad of findings is small, firm testes; gynecomastia; and azoospermia. Some men may
present with delayed sexual maturation, increased height, decreased intelligence, varicosities,
obesity, diabetes, leukemia, increased likelihood of extragonadal germ cell tumors, and breast
cancer (20-fold higher than in normal men).
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Klinefelter syndrome
Among men with Klinefelter syndrome, 90% have an extra X chromosome (47,XXY) and 10% are mosaic,
with a combination of XXY/XY chromosomes. The testes are usually <2 cm in length and always <3.5
cm; biopsies show sclerosis and hyalinization of the seminiferous tubules with normal numbers of
Leydig cells. Hormones usually demonstrate decreased testosterone and frankly elevated LH and FSH
levels. Serum estradiol levels may also be elevated. With age, testosterone levels decline, and
most men will require androgen replacement therapy both for virilization and for normal sexual
function. Paternity with this syndrome is rare but more likely in the mosaic or milder form of the
disease. Some men will have limited spermatogenesis, whereby sperm may be retrieved from the
testicles and used with ICSI to cause pregnancy.
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Other Genetic Causes and Syndromes
XX Male Syndrome (De la Chapelle syndrome)
XX male syndrome is a structural and numerical chromosomal condition, a variant of Klinefelter
syndrome that presents as gynecomastia at puberty or as azoospermia in adults. Average height is
below normal, and hypospadias is common. Male external and internal genitalia are otherwise normal.
The prevalence of mental deficiency is not increased. Hormone evaluation shows elevated FSH and LH
and low or normal testosterone levels. Testis biopsy reveals absent spermatogenesis with fibrosis
and Leydig cell clumping. The most obvious explanation is that sex-determining ratio (SRY), or the
testis-determining region, is translocated from the Y to the X chromosome. Thus, testis
differentiation is present; however, the genes that control spermatogenesis on the Y chromosome are
not similarly translocated, resulting in azoospermia.
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Gonadotoxins
Radiation
The effects of radiotherapy on sperm production have been well described. Clifton and Bremner
(1983) examined the effects of ionizing irradiation on semen quality and spermatogenesis among a
population of healthy prisoners in the 1960s. Before a vasectomy, each of the volunteers was
exposed to various levels of radiation and found a distinct dose-dependent, inverse relationship
between irradiation and sperm count. Sperm count was significantly reduced at 15 cGy, and
azoospermia was temporarily induced at 50 cGy. Persistent azoospermia was induced at 400 cGy,
without evidence of recovery for a minimum of 40 weeks. In most subjects, sperm counts rebounded to
preirradiation levels with cessation of exposure.
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Drugs
Exposure to gonadotropic drugs can result in infertility by various mechanisms. Ketoconazole,
spironolactone, and alcohol inhibit testosterone synthesis, whereas cimetidine is an androgen
antagonist. Recreational drugs such as marijuana, heroin, and methadone are associated with lower
testosterone levels. Certain pesticides, like dibromochloropropane, are likely to have
estrogen-like activity. Importantly, the gonadotoxic potential of many pharmaceutical and
over-the-counter medications is unknown. Therefore, couples should consider discontinuing and
unnecessary medication or supplements prior to their attempt to conceive.
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Traumatic injury of testes
Torsion
Ischemic injury to the testis secondary to twisting of the testis on the spermatic cord pedicle is
common in prepubertal and early postpubertal boys. When diagnosed and corrected surgically within 6
hours of occurrence, the testis can usually be saved. Torsion may result in inoculation of the
immune system with testis antigens that may predispose to later immunological infertility. It
recognized that the “normal” contralateral mate of a torsed testis could also exhibit histologic
abnormalities. It has not been clearly demonstrated whether this is related to the actual torsion
or to an underlying abnormality in testes predisposed to torsion.
Trauma
Trauma to the testis can result in infertility. Because of the unique immunologic status of the
testis in the body (ie, it is an immunologically privileged site), trauma to the testis can invoke
an abnormal immune response in addition to atrophy resulting from injury. Both may contribute to
infertility. Trauma to the testis that results in fracture of the testis tunica albuginea should be
surgically explored and repaired to minimize exposure of testis tissue to the body.
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Varicocele
Varicocele is defined as dilated and incompetent veins within the pampiniform plexus of spermatic
cord. Varicocele has been described as the most common surgically correctable cause of male
subfertility. This is a disease that develops during puberty when both endocrine and exocrine
function of the testicle dramatically increases, along with testicular blood flow. Varicocele is
only rarely detected in boys <10 years of age. A left-sided varicocele is found in 15% of healthy
young men. In contrast, the incidence of a left varicocele in subfertile men approaches 40%.
Bilateral varicoceles are uncommon in healthy men (<10%) but are palpated in up to 20% of
subfertile men. In general, varicoceles do not spontaneously regress. An accurate physical
examination remains the cornerstone of varicocele diagnosis.
79

Posttesticular causes of male infertility
Congenital Blockages
Cystic Fibrosis
CF is the most common autosomal recessive genetic disorder in the United States with a carrier
frequency of 1:20 among Caucasians. The disease is caused by defective chloride ion transport
across cell membranes resulting in fluid and electrolyte abnormalities (abnormal chloride–sweat
test). CF typically presents with chronic lung obstruction and pulmonary infections, pancreatic
insufficiency, and infertility. More than 95% of men with CF also have congenital bilateral absence
of the vas deferens (CBAVD). In addition to the vas, parts of the epididymis, seminal vesicles, and
ejaculatory ducts may be atrophic or absent, causing obstruction. Although spermatogenesis is
quantitatively normal, recent data suggest that sperm from men with CF may lack the normal capacity
to fertilize an egg. Furthermore, some carriers of abnormal CF genes may also have functional sperm
defects. CBAVD accounts for 1–2% of infertility cases. On physical examination, no palpable vas
deferens is observed on one or both sides. As in CF, the rest of the reproductive tract ducts may
also be abnormal and unreconstructable. This disease is related to CF. Even though most of these
men demonstrate no symptoms of CF, up to 80% of patients will harbor a detectable CF mutation. In
addition, 15% of these men will have renal malformations, most commonly unilateral agenesis.
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Idiopathic Epididymal Obstruction
Idiopathic epididymal obstruction is a relatively uncommon condition found in otherwise healthy
men. There is recent evidence linking this condition to CF in that one-third of men so obstructed
may harbor CF gene mutations.
Adult Polycystic Kidney Disease
Adult polycystic kidney disease is an autosomal dominant disorder associated with numerous cysts of
the kidney, liver, spleen, pancreas, epididymis, seminal vesicle, and testis. Disease onset usually
occurs in the twenties or thirties with symptoms of abdominal pain, hypertension, and renal
failure. Infertility with this disease is usually secondary to obstructing cysts in the epididymis
or seminal vesicle.
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Acquired blockages
Groin and Hernia Surgery
Groin and hernia surgery can result in inguinal vas deferens obstruction in 1% of cases. There has
been concern that Marlex mesh used for hernia repairs may add to perivasal inflammation and
increase the likelihood of vassal obstruction.
Bacterial Infections
Bacterial infections (E. coli in men age >35 or Chlamydia trachomatis in young men) may involve the
epididymis, with scarring and obstruction.
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Disorders of Sperm Function or Motility
Immotile Cilia Syndromes
Immotile cilia syndromes are a heterogeneous group of disorders (1:20,000 males) in which sperm
motility is reduced or absent. The sperm defects are due to abnormalities in the motor apparatus or
axoneme of sperm and other ciliated cells. Normally, nine pairs of microtubules are organized
around a central microtubule pair within the sperm tail and are connected by dynein arms (ATPase)
that regulate microtubule and therefore sperm tail motion. Various defects in the dynein arms cause
deficits in ciliary and sperm activity. Kartagener syndrome is a subset of this disorder (1:40,000
males) that presents with the triad of chronic sinusitis, bronchiectasis, and situs inversus. Most
immotile cilia cases are diagnosed in childhood with respiratory and sinus difficulties. Cilia
present in the retina and ear may also be defective and lead to retinitis pigmentosa and deafness
in Usher's syndrome. Men with immotile cilia characteristically have nonmotile but viable sperm in
normal numbers. The diagnosis can only be confirmed with electron microscopy of sperm.
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Disorders of Sperm Function or Motility
Immunologic Infertility
Autoimmune infertility has been implicated as a cause of infertility in 10% of infertile couples.
The testis is an immunologically privileged site, probably owing to the blood–testis barrier, which
consists of Sertoli cell tight junctions and locally downregulated cellular immunity. Autoimmune
infertility may result from an abnormal exposure to sperm antigens as the result of vasectomy,
testis torsion, or biopsy, which then incites a pathologic immune response. Antibodies may disturb
sperm transport or disrupt sperm–egg interaction. Many assays are available to detect ASAs, but
assays that detect sperm-bound, and not serum, antibodies are the most clinically relevant.
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Infections
Various products of activated leukocytes can exist in infected semen. A correlation exists between
leukocytes in semen and the generation of superoxide anions, hydrogen peroxide, and hydroxyl
radicals (reactive oxygen species), all of which can damage sperm membranes. Sperm are highly
susceptible to the effects of oxidative stress because they possess little cytoplasm and therefore
little antioxidant activity. Damage to sperm from oxidative stress has been correlated to loss of
function and damaged DNA. Although genital tract infection has been linked to infertility in
epidemiologic studies, the correlation between individual organisms and infertility is unclear.
Uncontrolled studies suggest that pregnancy rates may improve after treatment, but controlled
studies do not confirm these findings.
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Disorders of Coitus
Impotence
Sexual dysfunction stemming from low libido or impotence is a frequent cause of infertility. The
male hormonal evaluation can detect organic reasons for such problems. Most cases of situational
impotence, in which the stress of attempting to conceive results in poor erections, are treated
with sexual counseling and oral phosphodiesterase inhibitors.
Hypospadias
Anatomic problems like hypospadias can cause inappropriate placement of the seminal coagulum too
distant from the cervix and result in infertility.
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The next week plan
Pathophysiology of pregnancy
Pathophysiology of birth
Pathophysiology of early post-partum adaptation
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