Sexual Differentiation

Question 1

What is the difference between sexual determination and differentiation?

Answer 1

Sexual determination: genetically controlled process dependent on the Y chromosome ‘switch’. Once this male/fem determination has been made sexual differentiation starts.

Sexual differentiation: process by which internal and external genitalia develop as male or female.

Question 2

What is the SRY gene?

Answer 2

The SRY gene on the p arm of the Y chromosome codes for SRY protein, a transcription factor that upregulates its own gene

Sex determining region Y (SRY) switches on briefly during >week 7 of development to make the gonad into a testis. In its absence an ovary is formed.

Question 3

Describe the very first part of gonadal development, and explain the importance of genital ridges- what they are derived from, what do they develop into etc

Answer 3

After fertilisation, a pair of bipotential gonads develop
Image shows 3–4-week-old embryo, dotted line is a cross-section, which contains genital ridges.

Genital ridges: precursor is derived from mesenchymal tissue called genital ridge primordia. These develop on posterior lower thoracolumbar wall at ~3 ½ - 4 ½ weeks.
Rn embryo=bipotential; genital ridges can form testes or ovaries!

Question 4

Which ducts determine ovary/testi development? What do they eventually form?

Answer 4

Mullerian duct: will eventually form the uterus, uterine tubes and the upper 2/3rds of the vagina if the embryo becomes female

Wolffian duct: will eventually form the vas deferens, seminal vesicles and prostate gland if the Mullerian duct does not develop

Question 5

3 waves of cells invade the genital ridge…
What are these 3 cells?

Answer 5

Primordial germ cells: become spermatocytes (m) or oocytes (f)

Primitive sex cords: become Sertoli cells of the testis (m), or Granulosa cells of the ovary (f)

Mesonephric cells: become blood vessels and testosterone-producing Leydig cells in males, or Theca cells in females

Question 6

Three waves of cells which invade the genital ridge include
primordial germ cells
primitive sex chords
mesonephric cells.

Describe primoridial germ cells in detail- what and where are they, how do the cells divide, where do they migrate to?

Answer 6

Primordial germ cells become spermatocytes (m) or oocytes (f)
They r a small cluster of cells in the yolk sac epithelium that expand by mitosis at around 3 weeks
Atp cells are diploid (not haploid like gametes)

They then migrate to the connective tissue of the hind gut, to the region of the developing kidney and on to the genital ridge – completed by 6 weeks

Question 7

Three waves of cells which invade the genital ridge include
primordial germ cells
primitive sex chords
mesonephric cells.

Describe primitive sex cords in detail

Answer 7

Germinal epith cells overlying the genital ridge mesenchyme migrate inwards as columns called primitive sex cords

M: cells express SRY. They penetrate the medullary mesenchyme and surround primordial germ cells to form testis cords. Primitive sex cords then differentiate–> Sertoli cells, which express AMH

F: primitive sex cord cells don’t express SRY, ill-defined cords
They do not penetrate deeply, but condense in the cortex as clusters around primordial germ cells, like mature ovary follicles. Cells differentiate–> Granulosa cells

Question 8

Three waves of cells which invade the genital ridge include
primordial germ cells
primitive sex chords
mesonephric cells.

Describe mesonephric cells in detail- where do they originate, what do they form in males vs females etc

Answer 8

Mesonephric cells originate in the mesonephric primordium, just lateral to the genital ridges

In males, under pre-Sertoli cells (which express SRY), they form:
vascular tissue
Leydig cells (make testosterone, don’t express SRY)
Basement membrane (forms seminiferous tubules + rete testis)

In females, w/o SRY the mesonephric cells form vascular tissue and Theca cells (make androstenedione only after puberty)

Question 9

What are mullerian and wolfian ducts stimulated and inhibited by?

Answer 9

Wolffian (mesonephric) ducts: Stimulated by testosterone. Females dont have testosterone so Wolffian duct degenerates

Mullerian (paramesonephric) ducts: inhibited by AMH produced by Sertoli cells in the developing male

Question 10

Describe external genitalia formation in males

Answer 10

Testosterone is converted to androgen DHT by 5a-reductase
DHT binds to testosterone receptor, but is 10x more potent than testosterone
DHT causes differentiation of male external genitalia:
Clitoral area (genital tubercle + urethral fold) enlarges –>penis
Labia (genital swellings) fuse and rugate to form scrotum
Prostate forms

note- 5a-reductase also in females but no testosterone–>DHT is not formed, foetus follows fem external genitalia pathway

Question 11

What are some disorders of sexual differentiation?

Answer 11

Gonadal dysgenesis: incomplete sexual differentiation/abnormal gonadal development
Usually due to male missing SRY, or deletion of the 2nd X chromosome in females.

Intersex: Pts have components of both repro tracts, or ambiguous genitalia. Makes sex of an infant hard to determine

Sex reversal: phenotype doesn’t match genotype

note: pts prefer ‘disorder of sexual differentiation’ or DSD

Question 12

Explain androgen insenstivity syndrome in gonadal dysgenesis

Answer 12

Androgen insensitivity syndrome (AIS): XY makes testosterone, but it has no effect
XY individual still makes SRY, so will develop testes
The testes contain Sertoli cells which produce AMH, leading to normal Mullerian duct regression

Leydig cells produce testosterone, though it has no effect.
So Wolffian ducts won’t grow–> lack of internal male genitalia (except testes)
Lack of testosterone limits 5Alpha-reductase activity–> limits DHT production, affecting external genitalia as well

Question 13

What is the difference between complete and partial AIS? How do these patients present?
What is the incidence of complete AIS?

Answer 13

Complete AIS= aprox 1 in 20,000.
Appear completely female at birth despite being XY, undescended testes.
First present w primary amenorrhoea and no body hair (lack of testosterone). USS reveals undescended testes, bloods reveal male androgen levels, karyotypes reveal XY genotype. Since the pt has never responded to androgens, they appear and feel fem

Partial AIS: range from ambiguous genitalia to large clit/micropenis. Surgery was universal treatment but is now optional.

Question 14

What happens if in an XY individual has 5-α-reductase deficiency?

Answer 14

In XY individual, SRY forms testes, which produce AMH from Sertoli cells, Mullerian ducts regress
The Leydig cells of the testes produce testosterone, causing Wolffian duct differentiation, so internal genitalia unaffected

BUT 5a-reductase deficiency stops DHT production–> external genitalia + prostate wont form, so fem/ambiguous external genitalia seen

Question 15

How does presentation of 5-α-reductase deficiency differ?

Answer 15

The degree of enzyme block varies, so so does presentation
Incidence varies enormously as it’s an autosomal recessive condition, which can depend on inter-related marriage

At puberty, potential must be assessed bc high testosterone levels that occur at adrenarche (as less is converted to DHT) may induce virilisation

Question 16

What is the clincial presentation of turner syndrome?

Answer 16

Turner’s syndrome is a 45XO genotype, w internal and external fem genitalia due to no SRY
Despite having ovaries, Turner’s pts lack ovarian function.
Streak ovaries, due to ovarian dysgenesis, show that 2 XChr are needed for proper ovarian development (tho only 1 is active in each cell at any one time)
The uterus and uterine tubes may be present but small
Most pts are infertile- some maybe fertile due to mosaicism

Dysfunctional ovaries mean that oestrogen and progestogen supplementation given to support bones and the uterus

Question 17

Describe the formation of steroid hormones in the gonads
What are they derived from?
What are the different compositons?
what are the 3 types of oestrogens?

Answer 17

Steroid hormones= derived from cholesterol (27C structure)
Cleaving carbons 22-27 to leave a 21C structure forms progestogens.
21-hydroxylase forms aldosterone and gccs (cortisol) from progestogens

Cleaving C 20-27 will leave the androgens (19C) E.g. testosterone, androstenedione

Cleaving carbons 19-27 will leave the oestrogens (18C):
Oestrone has 1 OH group, oestradiol has 2, oestriol 3
Oestradiol=most common/potent, and is measured clinically

Question 18

The normal process of the HPA axis is…

Answer 18

ACTH stimulates cholesterol uptake into adrenal cortex and also upregulates cholesterol side chain cleavage enzyme (P450scc), producing more progestogens

Question 19

What happens in congenital adrenal hyperplasia?

Answer 19

In congenital adrenal hyperplasia, 21-hydroxylase is not functioning in females
Progestogens thus not converted into mineralocorticoids or gccs, so progesterone conc increases.
Progestogens are converted into more androgens (testosterone)
No cortisol is made due to the enzyme block, so no neg feedback loop to stop ACTH production
ACTH stimulates adrenals to make more progestogens–> more testosterone made in adrenals

Question 20

What is the clinical presentation and treatment of congenital adrenal hyperplasia?

Answer 20

XX female has no SRY, so no testes and AMH
DHT formed from high testosterone levels (m & f both have 5a-reductase)–> male external genitalia
Masculinised external genitalia, but androgen levels not usually high enough to fully rescue Wolffian ducts

As there is lack of aldosterone, pt will also be salt wasting and may need to be treated for that
The patient will also need treatment with gccs to correct the neg feedback issues