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The Normal Menstrual Cycle

The normal menstrual cycle depends on changes in hormone levels controlled by the hypothalamic-pituitary-ovarian axis. The hypothalamus secretes GnRH to stimulate the pituitary to release FSH and LH. FSH and LH act on the ovaries to regulate follicle development and ovulation. During the follicular phase, FSH causes follicle growth and estrogen production. Rising estrogen triggers an LH surge near ovulation. Following ovulation, the corpus luteum produces progesterone during the luteal phase.

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0% found this document useful (0 votes)
58 views

The Normal Menstrual Cycle

The normal menstrual cycle depends on changes in hormone levels controlled by the hypothalamic-pituitary-ovarian axis. The hypothalamus secretes GnRH to stimulate the pituitary to release FSH and LH. FSH and LH act on the ovaries to regulate follicle development and ovulation. During the follicular phase, FSH causes follicle growth and estrogen production. Rising estrogen triggers an LH surge near ovulation. Following ovulation, the corpus luteum produces progesterone during the luteal phase.

Uploaded by

Dheyaa A. Sabah
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© © All Rights Reserved
We take content rights seriously. If you suspect this is your content, claim it here.
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The Normal Menstrual cycle L1&2

Introduction :
The external manifestation of a normal menstrual cycle is the
presence of regular vaginal bleeding . This occurs as a result of
the shedding of the endometrial lining following failure of
fertilization of the oocyte or failure of implantation . The cycle
depends on changes occurring within the ovaries and fluctuation
in ovarian hormone levels , that are themselves controlled by the
pituitary and hypothalamus , the hypothalamo-pituitary-ovarian
axis ( HPO ) .

Hypothalamus :
The hypothalamus in the forebrain secretes the peptide hormone
gonadotrophn-releasing hormone ( GnRH ) , which in turn controls
pituitary hormone secretion . GnRH must be released in a pulsatile
fashion to stimulate pituitary secretion of luteinizing hormone ( LH )
and follicle stimulating hormone ( FSH ) . If GnRH is giving in a
constant high dose , it desensitizes the GnRH receptor and
reduces LH and FSH release .

Clinical view :
Drugs that are GnRH agonists ( e.g. buserelin and goserelin ) .
Although they mimic the GnRH hormone , when administered
continuously , they will downregulate the pituitary and
consequently decrease LH and FSH secretion . This has effects on
ovarian function such that oestrogen and progesterone levels
also fall . These preparations are used as treatments for
endometriosis and to shrink fibroids prior surgery .

Pituitary gland
GnRH stimulation of the basophil cells in the anterior pituitary
gland causes synthesis and release of the gonadotrophic
hormones , FSH and LH . This process is modulated by the ovarian
sex steroid hormones oestrogen and progesterone ( see Figure

1
1 ) . Low levels of oestrogen have an inhibitory effect on LH
production ( negative feedback ) , whereas high levels of
oestrogen will increase LH production ( positive feedback ) . The
mechanism of action for the positive feedback effect of
oestrogen involves an increase in GnRH receptor concentrations ,
while the mechanism of the negative feedback effect is
uncertain .
The high levels of circulating oestrogen in the late follicular
phase of the ovary act via the positive feedback mechanism to
generate a periovulatory LH surge from the pituitary .
The clinical relevance of these mechanisms is seen in the use of
the combined oral contraceptive pill , which artificially creates a
constant serum oestrogen level in the negative feedback range ,
inducing a correspondingly low level of gonadotriphin hormone
release .

Figure (1) Hyothalamo-pituitary-ovarian axis .

Unlike oestrogen , low levels of progresterone have a positive


feedback effect on pituitary LH and FSH secretion ( as seen
immediately prior to ovulation ) and contribute to the FSH surge .
High levels of progesterone , as seen in the luteal phase , inhibit

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pituitary LH and FSH production . Positive feedback effects of
preogesterone occur via increasing sensitivity to GnRH in the
pituitary . Negative feedback effects are generated through
both decreased GnRH production from the hypothalamus and
decreased sensitivity to GnRH in the pituitary . It is known that
progesterone can only have these effects on gonadotropic
hormone release after priming by oestrogen ( Figure 2 ) .
There are other hormones which are involved in pituitary
gonadotrophin secretion . Inhibin inhibits pituitary FSH secretion ,
whereas activin stimulates it .

Ovary
Ovaries with developing oocytes are present in the female
fetus from an early stage of development . By the end of the
second trimester in utero , the number of occytes has reached a
maximum and they arrest at the first prophase step in meiotic
division . No new occytes are formed during the female lifetime .
With the onset of menarche , the primordial follicles containing
oocytes will activate and grow in a cyclical fashion , causing
ovulation and subsequent menstruation in the event of non-
fertilization .
In the course of a normal menstrual cycle , the ovary will go
through three phases :
1. Follicular phase .
2. Ovulation .
3. Luteal phase .

Follicular phase :
The initial stages of follicular development are independent of
hormone stimulation . However , follicular development will fail at
the preantral stage and follicular atresia will ensue if pituitary
hormones LH and FSH are absent .
FSH levels rise in the first days of the menstrual cycle , when
oestrogen , progesterone and inhibin levels are low . This
stimulates a cohort of small antral follicles on the ovaries to grow .

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Within the follicles , there are two cell types which are involved
in the processing of steroids , These are the theca and the
granulosa cells , which respond to LH and FSH stimulation ,
respectively . LH stimulation production of androgens from
cholesterol within theca cells . These androgens are converted
into oestrogens by the process of aromatization in granulose cells ,
under the influence of FSH . The roles of FSH and LH in follicular
development are demonstrated by studies on women
undergoing ovulation induction in whom endogenous
gonadotrophin production has been suppressed . If pure FSH
alone is used for ovulation induction , as ovulatory follicle can be
produced , but oestrogen production is markedly reduced . Both
FSH and LH are required to generate a normal cycle with
adequate amounts of oestrogen .
As the follicles grow and oestrogen secretion increases , there is
negative feedback on the pituitary to decrease FSH secretion .
This assists in the selection of one follicle to continue in its
development towards ovulation – the dominant follicle . In the
ovary , the follicle which has the most efficient aromatase activity
and highest concentration of FSH – induced LH receptors will be
the most likely to survive as FSH levels drop , while smaller follicles
will undergo atresia . The dominant follicle will go on producing
oestrogen and also inhibin , which enhances androgen synthesis
under LH control .

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Figure (2) Changes in hormone levels , endometrium and follicle
development during the menstrual cycle .

Clinical view :
Administration of exogenous gonadotrophins is likely to
stimulate growth of multiple follicles which continue to develop
and are released at ovulation ( and can lead to multiple
gestations at a rate of around 30 per cent ) .
This situation is used to advantage in patients requiring in vitro
fertilization ( IVF ) , as many occytes can be harvested from
ovaries which have been stimulated as described above .
There are other autocrine and paracrine mediators playing a
role in the follicular phase of the menstrual cycle .
These include : Inhibin and activin . Inhibin participates in
feedback to the pituitary to downregulate FSH release , and also
appears to enhance ongoing androgen synthesis . Activin is
structurally similar to inhibin , but has an opposite action is
structurally similar to inhibin , but has an opposite action . It is
produced in granulosa cells and in the pituitary , and acts to
increase FSH binding on the follicles .
Insulin-like growth factors ( IGF – I , IGT – II ) act as paracrine
regulators .
1. In the follicular phase , IGF-I is produced by theca cells under
the action of LH. IGF-I receptors are present on both theca
granulosa cells . Within theca , IGF-I augments LH-induced
steroidogenesis . In granulosa cells , IGF-I augments the
stimulatory effects of FSH on mitosis , aromatase activity and
inhibin production .
2. In the preovulatory follicle , IGF-I enhances LH-induced
progesterone production from granulosa cells .

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3. Following ovulation , IGF-II is produced from luteinized
granulosa cells , and acts in an autocrine manner to
augment LH-induced proliferation of granulosa cells .
Kisspeptins are proteins which have more recently been found to
play a role in regulation of the HPO axis , via the mediation of the
metabolic hormone leptin's effect on the hypothalamus , Leptin is
thought to be key in the relationship between energy production ,
weight and reproductive health . Mutations in the kisspeptin
receptor , gpr-54 , are associated with delayed or absent
puberty , probably due to a reduction in leptin-liked triggers for
gonadotrophin release .

Ovulation
By the end of the follicular phase , which lasts an average of 14 days , the
dominant follicle has grown to approximately 20 mm in diameter . As the
follicle matures :
1. FSH induces LH receptors on the granulosa cells to compensate for
lower FSH levels and prepare for the signal ovulation .
2. Production of oestrogen increases until they reach the necessary
threshold to exert a positive feedback effort on the hypothalamus and
pituitary to cause the LH surge .
3. This occurs over 24 – 36 hours , during which time the LH-induced
luteinization of granulosa cells in the dominant follicle causes
progesterone to be produced , adding further to the positive
feedback for LH secretion and causing a small periovulatory rise in
FSH .
4. Androgens , synthesized in the theca cells , also rise around the time
of ovulation and this is thought to have an important role in stimulating
libido , ensuring that sexual activity is likely to occur at the time of
greatest fertility .

Clinical view :
1. The LH surge is one of the best predictors of imminent ovulation , and
this is the hormone detected in urine by most over-the-counter
'ovulation predictor' tests .
2. The LH surge has another function in stimulating the resumption of
meiosis in the occyte just prior to its release . The physical ovulation of
the oocyte occurs after breakdown of the follicular was occurs under

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the influence of LH , FSH and progesterone-controlled proteolytic
enzymes , such as plasminogen activators and protaglandins . There
appears to be an inflammatory-type response within the follicle wall
which may assist in extrusion of the oocyte by stimulating smooth
muscle activity .
Thus , women wishing to become pregnant should be advised to
avoid taking prostaglandin synthetase inhibitors .

Luteal phase :
After the release of the oocyte , the remaining granulosa and
theca cells on the ovary form the corpus luteum . The granulosa
cells have a vacuolated appearance with accumulated yellow
pigment , hence the name corpus luteum ( ' yellow body ' )
Ongoing pituitary LH secretion and granulosa cell activity
ensures a supply of progesterone which stabilizes the
endometrium in preparation for pregnancy . Progesterone levels
are at their highest in the cycle during the luteal phase . This also
has the effect of suppressing FSH and LH secretion to a level that
will not produce further follicular growth in the ovary during that
cycle .
The luteal phase lasts 14 days in most women , without great
variation . In the absence of beta human chorionic
ganadotrophin ( BHCG ) being produced from an implanting
embryo , the corpus luteum will regress in a process known as
luteolysis .
The withdrawal of progesterone has the effect on the uterus of
causing shedding of the endometrium and thus menstruation .
Reduction in levels of progesterone , oestrogen and inhibin
feeding back to the pituitary cause increased secretion of
gonadotrophic hormone , particularly FSH . New preantral follicles
begin to be stimulated and the cycle begins anew .

Endometrium :
The specific secondary changes in the uterine endometrium
give the most obvious external sign of regular cycles .

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Menstruation :
The endometrium is under the influence of sex steroids that
circulate in females of reproductive age .
During the ovarian follicular phase , the endometrium
undergoes profileration ( the ' proliferative phase ' ) ; during the
ovarian luteal phase , it has its ' secretory phase ' ,
Decidualization , the formation of a specialized glandular
endometrim , is an irreversible process and apoptosis occurs if
there is no embryo implantation . Menstruation (day 1) is the
shedding of the 'dead' endometrium and ceases as the
endometrium regenerates ( which normally happens by day 5 – 6
of the cycle ) .
The endometrium is composed of two layers , the uppermost of
which is shed during menstruation . A fall in circulating levels of
oestrogen and progesterone approximately 14 days after
ovulation leads to loss of tissue fluid , vasoconstriction of spiral
arterioles and distal ischaemia . This results in tissue breakdown ,
and loss of the upper layer along with bleeding from fragments of
the remaining arterioles is seen as menstrual bleeding . Enhanced
fibrinolysis reduces clotting .

Clinical view :
1. The effects of oestrogen and progesterone on the
endometrium can be reproduced artificially , for example in
patients taking the combined oral contraceptive pill or
hormone replacement therapy who experience a
withdrawal bleed during their pill-free week each month .
Vaginal bleeding will cease after 5 – 10 days as arterioles
vasconstrict and the endometrium begins to regenerate .
2. In rare cases , the tissue breakdown and vasoconstriction does not
occur correctly and the endometrium may develop scarring which
goes on to inhibit its function . This is known as ' Asherman's syndrome
' . The endocrine influences in menstruation are clear . However there
is also paracrine mediators influence in menstruation ,include :

8
prostaglandin F2 a , endothelin-1 and platelet activating factor ( PAF )
are vasoconstrictors which are produced within the endometrium .
They may be balanced by the effect of vasodilator agents , such as
prostaglandin E2 , prostacyclin ( PGI ) and nitric oxide (NO) , which are
also produced by the endometrium .
3. Recent research has shown that progesterone withdrawal increases
endometrial prostaglandin ( PG ) synthesis and decreases PG
metabolism . The COX-2 enzyme and chemokines are involved in PG
synthesis and this is likely to be the target of non-steroidal anti-
inflammatory agents used for the treatment of heavy and painful
periods .

The proliferative phase :


Once endometrial repair is complete . After this time , the endometrium
enters the proliferative phase , when glandular and stromal growth occur .
The epithelium lining the endometrial glands changes from a single layer of
columnar cells to a pseudostratified epithelium with frequent mitoses .
Endometrial thickness increases rapidly , from 0.5 mm at menstruation to
3.5 – 5 mm at the end of the proliferative phase .

Figure (3) Tissue sections of normal endometrium during proilferative and


secretory phases of the menstrual cycle .

The secretory phase


After ovulation ( generally around day 14 ) , there is a period
of endometrial glandular secretory activity . following the
progesterone surge , the oestrogen-induced cellular proliferation
is inhibited and the endometrial thickness does not increase any

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further . However , the endometrial glands will become more
tortuous , spiral arteries will grow , and fluid is secreted into
glandular cells and into the uterine lumen . Later in the secretory
phase , progesterone induces the formation of a temporary
layer , known as the decidua . Stromal cells show increased
mitotic activity , nuclear enlargement and generation of a
basement membrane .
Recent research into infertility has identified apical membrane
projections of the endometrial epithelial cells known as
pinopodes , which appear after day 21-22 and appear to be a
progesterone-dependent stage in making the endmetrium
receptive for embryo implantation ( Figure 4 ) .

Figure (4) photomicrograph of endometrial pinopodes from the


implantation window .

Immediately prior to menstruation , three distinct layers of


endometrium can be seen .
1. The basalis is the lower 25 per cent of the endomtrium ,
which will remain throughout menstruation and shows few
changes during the menstrual cycle .
2. The mid-portion is the stratum spongiosum with oedematous
stroma and exhausted glands .
3. The superficial portion ( upper 25 per cent ) is the stratum
compactum with prominent decidualized stromal cells . On
the withdrawal of both oestrogen and progesterone , the

10
decidua will collapse , with vasoconstriction and relaxation
of spiral arteries and shedding of the outer layers of the
endometrium .

New developments :
Measurement of ovarian reserve :
Female reproductive potential is directly proportionate to the
remaining number of oocytes in the ovaries . This number
decreases from birth onwards .
It is desirable to be able to quantify the residual ovarian
capacity of women of older age or after undergoing treatment
in order to give prognostic information and management advice
to patients , and also to compare different forms of treatment .
Research using :
1. Ultrasound markers has looked at measurements of ovarian
volume , mean ovarian diameter and antral follicle count to
calculate ovarian reserve .
2. Biochemical markers include FSH . oestrodiol , inhibin B , anti-
Mullerian hormone ( AMH ) . AMH is produced in the
granulosa cells of ovarian follicles and does not change in
response to gonadotrophins during the menstrual cycle . As
a result , it can be measured and compared from any point
in the cycle .

Harvesting ovarian tissue :


Harvesting and cryopreservation of ovarian tissue is an emerging
technique in reproductive biology . At present , its use is experimental and

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offered to nulliparious women or young females undergoing gonadotrophic
therapy , for example to treat cancer . The theory is that strips of ovarian
cortex can be removed at laparoscopy or laparotomy and preserved by
freezing , in the hope that future technology will allow them to be thawed
and used to generate occytes for IVF treatment .

Objective
It is important to have an understanding of the physiology of
the normal menstrual cycle to understand the causes of any
abnormalities , and also to tackle problems , such as infertility and
the prevention of unwanted pregnancy . This lecture aims to
describe the mechanisms involved in the normal menstrual cycle ,
with emphasis on the clinical relevance of each phase .

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