1. Prof. M.C.Bansal
MBBS., MS., FICOG., MICOG.
Founder Principal & Controller,
Jhalawar Medical College & Hospital Jjalawar.
MGMC & Hospital , sitapura ., Jaipur
2. Defining Sex and Gender
Gender identity (Psychological sex)
Inner sense of owns maleness / femaleness.
Sex of rearing
Gender role
Sexual identity (Organic sex)
The biologic sexual differentiation
Chromosomal sex
Gonadal sex
Internal genital sex
External genital sex
Hormonal sex
3. Human sexual differentiation
Chromosomal sex
Gonadal sex
Internal genital sex External genital sex
SEX ASSIGNMENT
Sex of rearing Gender identity
and role
4. Gonadal development
SRY-gene (TDF)
Short arm of Y chromosome
Present Absent
Bipotential
Gonad
Receptors 2 X chromosomes
For H -Y antigen
TESTES OVARY
5. Male
development
TESTIS
Leydig Sertoli
cells cells
Testosterone Mullerian inhibiting
factor
Wollfian duct 5a-reductase
DHT
Regrsession of
Muuleian ducts
Urogenital sinus
Male internal
Genital organs Male external genitalia
6. Female
development
Neutral
Development
OVARY
Urogenital sinus Mullerian
ducts
Female external genitalia Female internal genital
. Lower part of vagina Organs
. Most of upper vagina
Absence of androgen exposure
. Cervix and uterus
. Fallopian tubes
7. Summary of Normal Sex
Differentiation
genetic sex is determined at fertilization.
testes develop in XY fetus, ovaries develop in XX
fetus.
XY fetus produces MIS and androgens and XX fetus
does not.
XY fetus develops Wolffian ducts and XX fetus
develops Mullerian ducts.
XY fetus masculinizes the female genitalia to make it
male and the XX fetus retains female genitalia.
8. INTERSEX
An individual in whom there is discordance between
chromosomal, gonadal, internal genital, and
phenotypic sex or the sex of rearing
INTERSEXUALITY:
Discordance between any two of the organic sex
criteria
TRANSSEXUALITY:
Discordance between organic sex and psychological
sex components
11. How many children are born
with intersex conditions?
A conservative estimate is that 1 in 2000 children
born will be affected by an intersex condition
98 % of affected babies are due to congenital
adrenal hyperplasia
13. Congenital Adrenal Hyperplasia
It is a familial disorder of adrenal steroid
biosynthesis with autosomal recessive mode of
inheritance.
The defect is expressed as adrenal enzyme
deficiency.
5 major Enzymes deficiency are clinically
important
21-Hydroxylase
11-b-Hydroxylase
17-a-Hydroxylase
3-b-Hsteroid hydrogenese
20,22 Desmolase deficiency
14. CAH
The most frequent is steroid 21-
hydroxylase deficiency, accounting for
more than 90 percent of cases.
The enzyme deficiency causes reduction
in end-products, accumulation of
hormone precursors & increased ACTH
production.
The clinical picture reflects the effects of
inadequate production of cortisol &
aldosterone and the increased production
of androgens & steroid metabolites.
15. Biochemistry
Steroid
21-hydroxylase (CYP21, also termed
CYP21A2 and P450c21) is a cytochrome P-450
enzyme located in the endoplasmic reticulum.
Itcatalyzes the conversion of 17-
hydroxyprogesterone to 11-deoxycortisol, a
precursor of cortisol, and the conversion of
progesterone to deoxycorticosterone, a precursor
of aldosterone.
Owing to this loss of enzyme function, patients
with 21-hydroxylase deficiency cannot synthesize
cortisol efficiently, and as a result, the adrenal
cortex is stimulated by corticotropin and
overproduces cortisol precursors.
16.
17. Contd…
Cortisol is an adrenal steroid hormone that
is required for normal endocrine function.
Production begins in the second month of
fetal life. Poor cortisol production is a
hallmark of most forms of CAH. Inefficient
cortisol production results in rising levels of
ACTH, which in turn induces overgrowth
(hyperplasia) and overactivity of the steroid
-producing cells of the adrenal cortex. The
defects causing adrenal hyperplasia are
congenital (i.e., present at birth)
18. Contd…
Some of these precursors are diverted to the
biosynthesis of sex hormones, which may
cause signs of androgen excess, including
ambiguous genitalia in newborn girls and
rapid postnatal growth in both sexes.
Concomitant aldosterone deficiency may
lead to salt wasting with consequent failure
to thrive, hypovolemia, and shock.
20. 21-hydrxylase deficiency
congenital adrenal hyperplasia
Most common type, accounts for >80% of
cases.
Incidence is 1:5000 to 1:15000 live birth.
Gene is located on the short arm of
chromosome 6 near the C4 locus in close
association with HLA genes.
Heterozygous
carriers can be detected by
ACTH stimulation test.
21. Contd..
It is characterized by reduced production
of cortisol and aldosterone and increased
production of progesterone;
17-OH-progesterone, and sex
steroids.
The urinary steroid metabolites
(17-ketosteroids and pregnanetriol)
are elevated above normal levels.
22. Contd..
Decreased secretion of aldosterone results in
salt loss with hyponatremia and
hyperkalemia; plasma renin activity is
therefore elevated.
In partial enzyme deficiencies, the
aldosterone deficiency is not expressed, and
patients remain normonatremic and
normokalemic.
The excess androgens causes virilization of
girls & ambiguous genitalia & dark scrotum
in boys.
23. Contd…
There are 3 forms:
1. classic early virilization type with or
without salt-losing crisis(typically
identified at birth because of genital
ambiguity)
2.Salt wasting (in which there is
impairment of mineralocorticoid as well as
glucocorticoid secretion),
3. non-classic type with late-onset
virilization(in which heterosexual
development occurs at the expected age of
24. Contd…
Male babies with non salt-losing non-
classic type remains asymptomatic till
late childhood when they may show signs
of sexual precocity.
Because members of the same family
may have classic, non-classic &
asymptomatic forms, the disorder may
be due to allelic variations of the same
enzyme.
Massneonatal screening using filter
paper blood sample for 17-OH-
25. CLINICAL MANIFESTATIONS
1. In classic form(girls are born with ambiguous genitalia)
having
enlarged clitoris
fusion of the labioscrotal folds and the urogenital sinus.
The internal female organs (including the uterus,
fallopian tubes, and ovaries) develop normally because
they are not affected by the increased androgen levels.
early pubic hair and rapid growth in childhood
precocious puberty or failure of puberty to occur (
sexual infantilism: absent or delayed puberty)
excessive facial hair
Virilization
menstrual irregularity in adolescence
infertility due to anovulation
shallow vagina
27. 2. In salt wasting 21hydroxylase deficiency
hyponatremia
hyperkalemia
hypotension
CLASSICAL CAH
28. Contd…
During childhood, untreated girls with either the
classic or salt wasting form grow rapidly but have
advanced bone ages, enter puberty early, experience
early closure of their epiphyses, and ultimately are
short in stature as adults. CAH, with appropriate
therapy, is the only inherited disorder of sexual
differentiation in which normal pregnancy and
childbearing are possible.
Boys :
-no overt signs of the disease
except variable and subtle hyperpigmentation
and penile en-largement
29. BOYS WITH CAH
Are unrecognized at birth because their genitalia are
normal.
They are not diagnosed until later, often with a salt
wasting crisis resulting in dehydration, hypotension,
hyponatremia and hyperkalemia or later in childhood
with early pubic hair & phallic enlargement
accompanied by accelerated linear growth and
advancement of skeletal maturation.
High blood pressure & hypokalemia may occur in
those with 11-b-hydroxylase deficiency and 17-a-
hydroxylase deficiency due to the accumulation of the
mineralocorticoid desoxycorticosterone
31. 11-hydroxylase (P450c11) deficiency
Accounts for 5-10% of cases of CAH.
Gene is located on the long arm of chromosome 8.
caused by mutations in the CYP11B1 gene.
It is characterized by low plasma renin activity &
elevation of serum 11-Deoxycortisol and 11-
deoxycorticosterone.
Because of the strong mineralocorticoid activity of
deoxycorticosterone, the condition is characterized by
salt retention, hypertension & hypokalemic alkalosis.
The elevated plasma androgens may cause virilization
of the female fetus.
32. 3ß-hydroxysteroid dehydrogenase deficiency
This is a very rare disorder that results in accumulation of
DHEA, which is converted to testosterone in peripheral
tissues.
Enzyme defects in adrenal and ovary in autosomal –
recessive fashion
Caused by mutations in the HSD3B2 gene encoding the
3 ß- HSDII enzyme affects the synthesis of glucocorticoids,
mineralocorticoids, and sex steroids.
Cortisol ↓ & aldosterone ↓
Dehydroepiandrosterone ↑↑ the external genitalia
ambiguity
It can cause virilization of female fetus and leads to
ambiguous genitalia in the newborn.
A diagnosis based on baseline and ACTH-stimulated
changes in steroid levels is not accurate ; indeed, in adult
women, an apparent late-onset 3ß-hydroxysteroid
33. 17-hydroxylase deficiency
Genetic def ect is on chromosome 10.
Corticosterone, 11- deoxycorticosterone ↑
Presents with similar f eatures of those of 11-
Hydroxylase def iciency except that Androgens are low,
so no virilization in girls & genitalia is ambiguous in boys.
Hypertension (due to hypernatremia and hypervolemia),
hypokalemia
Inf antile f emale external genitalia & primary amenorrhea
34. ESSENTIALS OF DIAGNOSIS
Increased linear growth with advanced bone age and
eventual short stature
Pseudohermaphorditism in girls due to androgen
virilizing effect
Isosexual precocity in boys with small infantile testes.
Adrenal crisis with salt-loss & metabolic acidosis or
Hypertension & hypokalemic alkalosis.
Low cortisol with high androgens, ACTH and steroid
precursors e.g. 17-OH-Progest. or 11-Deoxycortisol.
Diagnosis is confirmed by measurement of ACTH,
Cortisol, Aldosterone, 17-OH-progesterone,
Testosterone & urinary 17-ketosteroids.
Needs alertness for the possibility in all babies with
Diarrhea & Vomiting, hypoglycemia or ↑ BP.
35. Diagnosis
Classic 21-hydroxylase deficiency is characterized by
markedly elevated serum levels of 17-
hydroxyprogesterone, the main substrate for the enzyme.
The gold standard for differentiating 21-hydroxylase
deficiency from other steroidogenic enzyme defects is the
corticotropin (cosyntropin) stimulation test,measuring
base-line and stimulated levels of 17-hydroxyprogesterone.
corticotropin (cosyntropin) stimulation test :
The most commonly used stimulatory test involves
measurement of 17-hydroxyprogesterone 30 minutes after
administration of a bolus of 250 mg of synthetic
cosyntropin (Cortrosyn).
36. Contd…
In normal women - this value seldom exceeds 400 ng/dL.
Patients with classic 21-hydroxylase deficiency - achieve peak levels of
3,000 ng/dL or higher.
Patients with nonclassic 21-hydroxylase deficiency-achieve levels of 1,500
ng/dL or more.
Heterozygous carriers - achieve peak levels up to
about 1,000 ng/dL.
In hirsute women with hypertension, 11-deoxycortisol levels can be
determined during the test. If both 11-deoxycortisol and 17-
hydroxyprogesterone levels are increased, the rare 11-hydroxylase
deficiency is present. Only measurements of several steroid precursors
after corticotropin stimulation can identify individuals with nonclassic
forms of 3-HSD deficiency.
The elevated levels of 17-hydroxyprogesterone present in all forms of 21-
hydroxylase deficiency are rapidly suppressed by administration of
exogenous corticoids. Even a single dose of a glucocorticoid such as
dexamethasone will suppress 17-hydroxyprogesterone in CAH but not
in virilizing ovarian and adrenal neoplasms.
37.
38. CONGENITAL ADRENAL HYPERPLASIA - Diagnosis
Normal iNfaNt :100Ng/dl (17
-hydroxyprogesteroNe)
affected iNfaNts : 3,000 - 40,000Ng/dl ↑
the severity of hormoNal abNormalities
: depeNds oN the type of 21-hydroxylase def
salt wastiNg : 17-hydroxyprogesteroNe:
100000Ng/dl
iN adult , raNdom 17-hydroxyprogesteroNe
(17-ohp)
: baseliNe - 200Ng/dl ↓
levels greater 200Ng/dl, but less thaN 800
Ng/dl
-> corticotropiN stimulatioN test
39. Lab Findings
Demonstration of inadequate production of cortisol and/or
aldosterone in the presence of accumulation of excess
concentrations of precursor hormones is diagnostic.
In 21-hydroxylase deficiency, very high serum 17-
hydroxyprogesterone is characteristic together with very high
urinary pregnanetriol (metabolite of 17-hydroxyprogesterone).
Both are accompanied by elevated 24-hour urinary 17-
ketosteroids, the urinary metabolites of adrenal androgens.
40. Other tests
Salt wasting forms of adrenal hyperplasia are
accompanied by low serum aldosterone,
hyponatremia, hyperkalemia and elevated plasma
renin activity indicating hypovolemia.
In contrast hypertensive forms of adrenal hyperplasia
(11-β-hydroxylase deficiency and 17- α-hydroxylase
deficiency) are associated with suppressed plasma
renin activity and hypokalemia
A karyotype
is essential in the evaluation of the infant with
ambiguous genitalia in order to establish the
chromosomal sex.
Prenatal diagnosis of adrenal hyperplasia is possible
through biochemical and genetic tests.
41. Imaging Studies
A pelvic ultrasound : in the infant with
ambiguous genitalia to demonstrate the
presence or absence of a uterus or
associated renal anomalies
A urogenitogram is often helpful to define
the anatomy of the internal genitalia.
A CT scan of the adrenal gland to R/O
bilateral adrenal hemorrhage in the patient
with signs of acute adrenal failure
A bone age study is useful in the evaluation
of the child who develops precocious pubic
hair, clitoromegaly, or accelerated linear
growth.
42. CONGENITAL ADRENAL HYPERPLASIA – Management
GOALS
According to the clinical course & hormonal level
Purpose
: Normal growth, B.Wt, pubertal development, optimal
adult height
Growth velocity, body Wt velocity, bone age maturation
Classic 21-OH def
-> glucocorticoid : adrenal androgen secretion ↓
-> mineralocorticoid : electrolytes & plasma renin activity
43. MODE OF TREATMENT
Steroid replacement
Supportive therapy when needed
Treatment is life-long
Plastic surgery for ambiguous genitalia at
early age
Genetic counseling
Psychological support
44. Treatment(1)-Glucocorticoids
Patients with classic 21-hydroxylase deficiency
require long-term glucocorticoid treatment to
inhibit excessive secretion of corticotropin-
releasing hormone and corticotropin by the
hypothalamus and pituitary, respectively, and to
reduce elevated levels of adrenal sex steroids.
In children, the preferred drug is hydrocortisone
(i.e., cortisol itself ) in maintenance doses of 10 to
20 mg per square meter of body-surface area per
day in three divided doses.
45. Treatment(2)-Glucocorticoids
Doses of up to 100 mg per square meter per day
are given during adrenal crises and life-threatening
situations.
Even these maintenance doses exceed physiologic
cortisol secretion (7 to 9 mg per square meter per
day in neonates and 6 to 8 mg per square meter
per day in children and adolescents).
The efficacy of treatment is best monitored by
measuring 17-hydroxyprogesterone and
androstenedione levels at a consistent time in
relation to the administration of medication.
46. Treatment(3)-Glucocorticoids
The therapeutic goal is to use the lowest dose of
glucocorticoid that adequately suppresses adrenal
androgens and maintains normal growth and
weight gain.
Children should also undergo radiography
annually to determine bone age, and their linear
growth should be carefully monitored.
Older adolescents and adults may be treated with
prednisone (e.g., 5 to 7.5 mg daily in two divided
doses) or dexamethasone (total, 0.25 to 0.5 mg
given in one or two doses per day).
47. Treatment(1)-Mineralocorticois
Infants with the salt-wasting form of 21-
hydroxylase deficiency require supplemental
mineralocorticoid (usually 0.1 to 0.2 mg of
fludrocortisone daily) and sodium chloride (1 to 2
g or 17 to 34 mmol of sodium chloride chloride
daily in addition to glucocorticoid treatment).
Older infants and children usually do not require
sodium chloride supplements, and they often have
reduced requirements for fludrocortisone.
48. Treatment(2)-Mineralocorticoids
Plasma renin activity levels or direct renin
immunoassays may be used to monitor the
adequacy of mineralocorticoid and sodium
replacement, taking into account the age-specific
reference ranges for each laboratory.
Hypotension, hyperkalemia, and elevated renin
levels suggest the need for an increase in the dose,
whereas hypertension, edema, tachycardia, and
suppressed plasma renin activity signify
overtreatment with mineralocorticoids.
49. NEW TRENDS OF T/T
A New approach therapy is the
combined use of 4 drugs:
glucocorticoid (to suppress ACTH and
adrenal androgen production),
mineralocorticoid (to reduce angiotensin II
concentrations),
aromatase inhibitor (to slow skeletal
maturation),
flutamide (an androgen blocker to reduce
virilization)
50. Management of Ambiguous
Genitalia
Improvements in the surgical correction of genital
anomalies over the past two decades have led to
earlier use of single-stage surgery — between two
and six months of life in girls with 21-hydroxylase
deficiency, a time when the tissues are maximally
pliable and psychological trauma to the child is
minimized.
The long-term outcomes of the newer surgical
procedures have yet to be evaluated.
51. SURGICAL T/T
Infants with CAH may require surgical
evaluation and, if needed, corrective
surgery.
Traditional approach is clitroplasty early in
life, followed by vaginoplasty after puberty.
Some female infants with adrenal
hyperplasia are only mildly virilized and may
not require corrective surgery if they receive
adequate medical therapy to prevent further
virilization.
52. Prenatal diagnosis and t/t
Done by chorionic villus sampling at 8-12 wk &
amniocentesis at 18-20 wk.
HLA typing in combination with measurement of 17-
OH-progesterone & androstenedion in amniotic fluid
is used for antenatal diagnosis.
Prenatal treatment of 21-hydroxylase deficiency
prevents intrauterine virilization of female fetuses.
According to the protocol proposed by Carlson et al,
the mother is treated with dexamethasone (20
µ/kg/d in 3 divided doses) as soon as the pregnancy
is recognized to suppress fetal ACTH secretion &
prevent the fetal adrenal gland from overproducing
adrenal androgens.
55. Male pseudohermaphroditism
(XY- FEMALE)
Failure to utilize Failure to produce
testosterone testosterone
Defects in testicular
Androgen receptor deficiency steroidogenesis
* Complete androgen Gonadotropin-resistant
Insensitivity (TFS) testes (LH receptor mutation)
* Incomplete androgen Congenital lipoid adrenal
Insensitivity hyperplasia
5-alpha reductase deficiency Defective synthesis,
secretion, or response to
anti-mullerian hormone
56.
57. What is AIS?
A genetic condition where affected people have male chromosomes &
male gonads with complete or partial feminization of the ext. genitals
An inherited X-linked recessive disease with a mutation in the
Androgen Receptor (AR) gene resulting in:
– Functioning Y sex chromosome
– Abnormality on X sex chromosome
Types
1. CAIS (completely insensitive to AR gene)
-External female genitalia
-Lacking female internal organs
2. PAIS (partially sensitive-varying degrees)
-External genitalia appearance on a spectrum (male to female)
3. MAIS (mildly sensitive, rare)
-Impaired sperm development and/or impaired masculinization
Also called Testicular Feminization
58. Normal Sexual Development
MALE Sex Chromosome = XY
Gonads = Testes
External Genitalia = Male
FEMALE Sex Chromosome = XX
Gonads = Ovaries
External Genitalia = Female
Normally chromosome sex determines gonad sex which determines
phenotypic sex
?WHAT HAPPENS IN AIS
59. Androgen Receptor Gene
AIS results from mutations in the androgen receptor gene, located
on the long arm of the X chromosome (Xq11-q12)
The AR gene provides instructions to make the protein called
androgen receptor, which allows cells to respond to androgens,
such as testosterone, and directs male sexual development
Androgens also regulate hair growth and sex drive
Mutations include complete or partial gene deletions, point
mutations and small insertions or deletions
60. The Process of Sexual Development
In AIS the chromosome sex and gonad sex do not agree with the
phenotypic sex
Phenotypic sex results from secretions of hormones from the
testicles
The two main hormones secreted from the testicles are
testosterone & mullerian duct inhibitor
– Testosterone is converted into dyhydrotestosterone
– Mullerian duct inhibitor suppresses the mullerian ducts &
prevents the development of internal female sex organs in
males
Wolffian ducts help develop the rest of the internal male
reproductive system and suppress the Mullerian ducts
– Defective androgen receptors cause the wolffian ducts &
genitals to be unable to respond to the androgens
testosterone & DHT
61. AIS Fetus Development
• Each fetus has non-specific genitalia for the first 8 weeks
after conception
• When a Y-bearing sperm fertilizes an egg an XY embryo
is produced and the male reproductive system begins to
develop
• Normally the testes will develop first and the Mullerian
ducts will be suppressed and testosterone will be
produced
• Due to the inefficient AR gene cells do not respond to
testosterone and female genitalia begin to form
The amount of external feminization depends on the
severity of the androgen receptor defect
CAIS: complete female external genitalia
PAIS: partial female external genitalia
MAIS: Mild female external genitalia, essentially
male
63. Complete Androgen Insensitivity
Testicular Feminization SD (female phenotype)
– female-appearing external genitalia, and absence of müllerian derivatives
Blind ending vagina, reduced pubic hair
1 in 20-60,000 males, X-linked trait
In utero loss of androgen, & MIS secretion means loss of
internal genitalia
2% of males with an inguinal hernia have Complete androgen
sensitivity so vaginoscopy pruden
Usuallydiagnosed amenorrhea, absence of pubic hair or
hormonal profile
Gonadectomy and Oestrogen replacement therapy
64.
65. Incomplete Androgen Insensitivity
(Reifenstein’s Syndrome)
Incomplete male pseudohermaphroditism
Ambiguous genitalia to varying degrees
male with perineoscrotal hypospadias, cryptorchidism,
rudimentary Wolffian duct structures, gynecomastia, and
infertility
the phenotypic spectrum can range from hypospadias and a
pseudovagina to gynecomastia and azoospermia
etiology:
(1) a reduced number of normally functioning androgen
receptors
(2) a normal receptor number but decreased binding
affinity
Gender assignment is often dictated by phenotype and degree
of virilization
Normal testosterone, LH and testosterone/DHT ratio
All intermediate type of androgen insensitivity
66. Infertile male syndrome
– normal male phenotype but are azoospermic or
severely oligospermic
– normal to elevated serum testosterone
– normal to elevated LH
– decreased androgen receptor binding to DHT in
genital skin fibroblasts
67. Testing for AIS
Tests
– During Pregnancy
Chorionic Villus Sampling (9-12 weeks)
Ultrasound and Amniocentesis (after 16 weeks)
– After Birth
Presence of XY Chromosomes
– Buccal Mouth Smear
– Blood Test
Pelvic Ultrasound
Histological Examination of Testes
68. Biochemical Testing for
Carriers
Tests
– 1960-70s: Skin biopsies-evaluate androgen binding
capacity
Carries: 50% androgen binding
Problem: some cases skipped because mutation did
not always take place in the binding region of the
gene
– 1990s: DNA Testing
blood or mouth cavity smears
– Now:
Measure length of base pair repeat region in first
exon of gene and compare it to a female relative’s
repeat region to determine if they are a carrier
69. Non-Biochemical Testing
Maternal relatives affected by AIS
In an XX female
– Delayed puberty
– Reduced pubic-auxiliary hair
– Asymmetric pubic-auxiliary hair
– Reduced bone density
70. Treatments
Surgery
– Orchidectomy or gonadectomy
Removal of the testes
– Vaginal lengthening
– Genital plastic surgery
Reconstructive surgery on the female genitalia if
masculinization occurs
Phalloplasty
Vaginoplasty
– Pressure dilation
Clitorectomy
Debate
– What age?
– Who decides?
71. Treatments
Hormone Replacement Therapy (HRT)
– Types
Female: Estrogen
– Progesterone (sometimes take to reduce risk of
breast or uterine cancer)
– postorchidectomy
Male: Testosterone and DHT
– Form
Oral, transdermal, implant, injection, vaginally
– Prevents osteoporosis (age 10 or 11)
Body responds as if it is post-menopausal, thus body
density decreases and osteoporosis occurs
72. The Androgen Insensitivity Syndromes
5α-redutase Complete Incomplete Reifenstein Infertile
Inheritance Autosomal X-linked X-linked X-linked X-linked
recessive recessive recessive recessive recessive
Spermatogenesis Decreased Absent Absent Absent Decreased
Mullerian Absent Absent Absent Absent Absent
Wolffian Male Absent Male Male Male
External Female Female Female Male Male
Clitomegaly Hypospadia
Breasts Male Female Female Gynecomastia Gynecomastia
73. 5-alpha reductase deficiency
Secondary to mutations in the type II gene
Phenotype may vary from penoscrotal hypospadias to, more commonly,
markedly ambiguous genitalia
Normal internal genitalia
: testes secrete T, MIH causes Mullerian ducts to degenerate
Lack of DHT leads to inadequate masculinization of external genitalia at
birth
– Testes in labia or inguinal canal
– Urogenital sinus: urethra & blind vagina
– Prostate gland: small or absent
At puberty, lots of T
testes descend, scrotum darkens, phallus enlarges, muscular &
deep voice
74. 5-alpha-reductase
46-XY/SRY
Testis MIF deficiency
Testosterone
5-∝-rductase
DHT
Female or Male Internal
Ambiguous Genitalia
external Genitalia
75. Male Pseudohermaphroditism
Disorders of Testosterone Biosynthesis
– Defect in any of the five enzymes incomplete (or absent) virilization
of the male fetus during embryogenesis
– Inheritance is autosomal recessive
Cholesterol Side Chain Cleavage Deficiency (StAR Deficiency)
– a defect in cholesterol transport prevents conversion of cholesterol to
pregnenolone
– 46,XY individuals have female or ambiguous external genitalia
a blind-ending vaginal pouch
intra-abdominal, inguinal, or labial testes
absence of müllerian structures & Wolffian ducts are present but
rudimentary
severe adrenal insufficiency and salt wasting
– suspect this if nonvirilized female external genitalia with:
cortisol and aldosterone deficiency
hyponatremia, hyperkalemia, and metabolic acidosis.
– Abdominal CT scanning demonstrates large, lipid-laden adrenal
glands
76. Testosterone Biosynthesis
5 enzymes involved in the conversion of cholesterol to
testosterone
–3 in the adrenal & testis Cholesterol side change cleavage
3β O steroid Dehydrogenase
H
17α Hydroxylase
–2 in the testis only 17,20 Lyase Deficiency
17β O steroid Dehydrogenase
H
78. Leydig Cell hypoplasia /LH receptor mutation
-46,XY male karyotype, normal-appearing female phenotype
– Palpable testes but ↑LH and ↓Testosterone
– No stimulation of testosterone with HCG
–spectrum absent Leydig cells to Leydig cells with abnormal LH receptor
–autosomal recessive trait
– No Mullerian structures / short vagina
–DDx = androgen insensitivity syndrome or a terminal defect in androgen
synthesis.
–Testis histology = absent of Leydig cells in intratubular spaces, normal
Sertoli cells
79. Leydig-cell agenesis
46-XY/SRY
TESTIS MIF
( partial/ complete absence
Of leydig-cells)
No or testosterone
No or DHT
Female or ± Male
ambiguous Internal
external Genitalia
Genitalia
80. Hernia Uterine Inguinale
(persistant mullerian structures)
Normal phallus, uterus and tubes in the inguinal hernia sac
Poor sperm and hormone production
Gonad cancer risk
Can be familial
Presumed failure of AMH function
Fertility – rarely preserved
81. Diagnosis of XY Female
Testosterone concentration
Low Normal
Male level
Concentration of
Testosterone precurcers DHT
High Low Low Normal
Testicular Absent testes or 5 ∝-reductase Testicular
enzyme Absent leydig- Deficiency Feminization
Failure cell Syndrome
Surgical
exploration
82. Seminiferous Tubule Dysgenesis
(Klinefelter's syndrome)
Syndrome characterized by eunuchoidism, gynecomastia, azoospermia,
increased gonadotropin levels, and small, firm testes, 47,XXY karyotype
– nondisjunction during meiosis
– 1 of 1000 liveborn males
– associated with 48,XXYY; 49,XXXYY; 48,XXXY; 49,XXXXY;
46,XY/47XXY
Gynecomastia can be quite marked at pubertal development
– 8 X risk for breast carcinoma compared with normal males
Seminiferous tubules degenerate and are replaced with hyaline
– Fertility, with the benefit of ICSI, has been reported in one patient
– decreased androgens prevents normal secondary sexual development
poor muscle development, the fat distribution is more female than
male.
Normal amounts of pubic and axillary hair, but facial hair is
sparse.
Patients tend to be taller than average, due to disproportionately
long legs
Predisposed to malignant neoplasms of extragonadal germ cell origin.
Androgen supplementation to improve libido & reduction mammoplasty
– surveillance for breast carcinoma
84. 46,XX maleness
Occurs in 1 of every 20,000 males
Testicular development in subjects who have two X
chromosomes and lack a normal Y chromosome.
Most of these subjects have normal male external genitalia, but
10% have hypospadias and all are infertile
– 80% are Sry positive and rest are Sry negative
– Sry -positive group rarely have genital abnormalities, but they have
phenotypic features of Klinefelter's syndrome
Shorter (mean height, 168 cm) and have more normal skeletal
proportions than Klinefelter’s patients
Due to translocation of Y chromosomal material, including
SRY, to the X chromosome
Infertile lack of germ cell elements
86. Gonadal Dysgenesis Features:
Turners Syndrome (45 X0) 1. Female Phenotype
2. Short Stature
3. No Secondary Sexual
Characteristics
4. Somatic Abnormalities
Occult Y Ch. Material: - Webbed Neck
Predisposed to Virilisation - Broad Chest
and Gonadoblastoma (30%) - Short Ring finger
and other GCT (50%).
–Presence of one functioning X Chromosome
–1 in 2500 females. Mosaicism 45 X/46 XX (10%) or 45 X/46 XY (3%)
–Oocytes degenerate leaving streak gonads (in broad lig.) at birth
–Reduced Oestrogen, Raised FSH/LH. No pubertal development
Renal Anomalies:
–Management includes: 90% Multiple Renal Arteries
20% Renal agenesis/Duplication
Growth Hormone to Children & estrogens at puberty 15% Malrotation
10% Horseshoe kidney
Up to one third may have functioning ovaries
- so pregnancy is possible
Remove Streak gonads in Mosaic patients
Alternative Names:Bonnevie-Ullrich syndrome; Gonadal
dysgenesis; Monosomy X
89. Turner syndrome
Karyotype 45,X (60%)
(45,X/46,XX, structural abnormalities of X chromosome)
Short stature (final height 142-147 cm)
Gonadal dysgenesis - streak gonad & sexual infantilism
Skletal abnormalities & dysmorphic face
Cardiac and kidney malformation
Autoimmune ds : Hashimoto’s thyroditis, Addison’s ds
Mild insulin resistance & hearing loss
Lymphedema
Essential hypertension
No mental defect
Impairment of cognitive function : mathematical ability↓
Visual–motor coordination, spatial-temporal processing↓
H. Tuner, 1938
90. Turner syndrome – work up
IVP or renal USG
Echocardiography
Audiometry
Lipid profile & glucose metabolism (annually)
Annual pelvic examination & appropriate screening for
gonadal neoplasm as an adnexal mass
Expert consultation to pursue further analysis with X-
and Y- specific DNA probes
91. Pure Gonadal Dysgenesis
All subjects with female genitalia, normal mullerian structure &
streak gonads ( with either 46,XX or 46,XY karyotypes)
None of Turner phenotype anomalies
93. 46,XX pure gonadal dysgenesis
Features:
– normal female external genitalia
– normal müllerian ducts with absence of wolffian duct
structures
– a normal height
– bilateral streak gonads
– sexual infantilism
– normal 46,XX karyotype
streak
gonads elevated serum gonadotropins
Management of 46,XX "pure" gonadal dysgenesis:
– cyclic hormone replacement with estrogen and progesterone.
– growth is basically normal so GH is not needed
possibly autosomal recessive trait
94.
95. 46,XY Complete Gonadal
Dysgenesis
Characterized by :
– normal female genitalia
– well-developed müllerian structures
– bilateral streak gonads
– nonmosaic karyotype
Ambiguity of genitalia is not an issue
Sexual infantilism is the primary clinical problem
– present in their teens with delayed puberty
An abnormality of the Sry gene function, or loss of another gene
downstream from Sry that is necessary for SRY protein action
LH elevated clitoromegaly
30% risk of germ cell tumor development by age 30 years
– gonadoblastoma is most common
– embryonal carcinoma, endodermal sinus tumor, choriocarcinoma, and immature
teratoma have also been reported
Management removal of both streak gonads and proper cyclic
hormone replacement with estrogen and progesterone
96. Gonadal Dysgenesis
Multiple X female (47,XXX)
– Normal development & reproductive
function
– Mental retardation- frequent
– Secondary amenorrhea & eunuchoidism
97. Mixed Gonadal Dysgenesis
Features:
Unilateral testis (undescended)
Contralateral Streak Gonad
Persistent Mullerian Structures
Some masculinisation
–Mosaicism: 45 XO/ 46 XY Mostly females with;
Enlarged phallus
–Second most common cause for Ambiguous Labioscrotal folds
genitalia Uterus /vagina & tubes
–Mostly phenotypic females, but entire spectrum
covered Increased risk of:
–Due to lack of MIS production in unilateral Gonadoblastoma (20%)
- testis > streak gonad
dysgenetic Wilm’s tumor
Denys-Drash Syndrome
testis with ipsilateral fallopian tube - Nephropathy /CRF
- Genital Abnormalities
–Management includes Gender assignment (2/3 - Wilms tumour
female), - XX/XY mosaicism
May need prophylactic
Appropriate gonadectomy & screen for Wilm’s bilateral nephrectomy
tumor
98. Mixed Gonadal Dysgenesis
Karyotype 46XY / 45X0
Combined features of Turner’s SD
& male pseudohermaphroditism
Short stature
Streak gonad on one side with a
testis on the other side
Unicornuate uterus & fallopian tube-
side of streak gonad
Considrable variation in the sexual
phenotype
99. Gonadal Dysgenesis
Surgical Removal of Gonadal Tissue
The gonadal tissue having any Y chromosome
component in phenotypic females removal as soon
as the diagnosis is made to avoid the risk of
malignant gonadal tumor
(except complete androgen insensitivity)
: Laparoscopy or laparotomy
The uterus and tubes should be preserved for the
possibility of pregnancy with donor oocytes
100. Gonadal Dysgenesis
Hormone Treatment of Patients
Without Ovaries
Starting when the bone age is 12 with unopposed
estrogen ( 0.3mg conjugated estrogens or 0.5mg
estradiol daily)
After 2 years , a sequential program is initiated with
0.625mg conjugated estrogens or 1.0mg conjugated
estrogens
+ 5mg medroxyprogesterone acetate for 14days
(if a uterus is present)
In patients with genetic shortness in stature (e.g.
Turner SD) Estrogens treatment is not
started until bone age is 12
(to avoid epiphysial closure)
101. Gonadal Dysgenesis
Stimulation of Growth
Growth hormone treatment for short stature in turner
syndrome
: Optimal response an early onset of Tx around age
6~7
Now that the success of GH treatment in recognized &
accepted, an argument can be made for chromosomal
screening by molecular analysis of all growth-retarded
girls
102. Gonadal Dysgenesis
The Possibility of Pregnancy
In women who have variants of gonadal dysgenesis and
who menstruate, pregnancy can occur
30% incidence of congenital anomalies in the offspring
amniocentesis or chorionic villus biopsy
Donated oocytes yields excellent results
Fatal aortic events (aneurysm, dissection, or rupture)
can occure during pregnancy in patients with gonadal
genesis. A cardiology consultation with a
echocardiogram is strongly advised
103. Swyer’s syndrome
(Bilateral dysgenesis of the testes)
46, XY
No SRY OR its receptors
STREAK GONADS
- NO MIF
(Uterus +)
- NO SEX
STEROIDS
Female Female
external Internal
Genitalia Genitalia
104. Embryonic Testicular Regression and
Bilateral Vanishing Testes Syndromes
46,XY karyotype and absent testes but clear evidence of testicular
function during embryogenesis
"embryonic testicular regression" = loss of testicular tissue within the
first trimester and is associated with ambiguity of external genitalia
"bilateral vanishing testes syndrome" refers to individuals in whom
male sexual differentiation of ducts and genitalia took place but loss of
testicular tissue occurred subsequently in utero
Diagnosis can be made on the basis of a 46,XY karyotype and castrate
levels of testosterone despite persistently elevated serum LH and FSH
– bilateral vanishing testes syndrome, agonadal XY phenotypic males with fully
developed wolffian structures, but an empty scrotum, absent prostate, and
microphallus
Spectrum of presentation
– intermediate point presentation is the 46,XY patient with absent gonads and internal
ductal structures but with ambiguous genitalia incomplete elaboration of
androgen
– most severe form, agonadism is discovered in a 46,XY phenotypic female with no
internal genital structures; the testis has elaborated MIS but vanishes at 60-70
days before elaboration of androgen
106. TRUE HERMAPHRODITISM
• Gonads :
- ovary one side and testis on the other side of the abdomen
- bilateral ovotestis
• Karyotype :
46,XX most common(70%); XY and XX/XY
• Internal genitalia :
Both mullerian and wolffian derivates
• Phenotype is variable
• Gonadal biopsy is required for confirming diagnosis
107. True Hermaphroditism
Individuals who have
both testicular tissue
with well-developed
seminiferous tubules and
ovarian tissue with
primordial follicles,
which may take the form
of one ovary and one
testis or, more
commonly, one or two
ovotestes.
External genitalia and
internal duct structures of
true hermaphrodites (Williams Textbook of Endocrinology, 10th ed, 2003)
display gradations
between male and female
108. True Hermaphroditism
In most patients, the external genitalia are ambiguous but
masculinized to variable degrees, and 75% are raised as male
Internal ductal development are influenced by ipsilateral
gonad
– Fallopian tubes are consistently present on the side of the
ovary
– a vas deferens is always present adjacent to a testis
– Fallopian tube is present with 66% of ovotestes, vas or both in
33%
– Most have urogenital sinus and and uterus
80% of those raised as male have hypospadias and chordee
Ovaries usually on left in normal position, testis usually on right
and located anywhere along path of descent
60% of gonads palpable in canal or labia are ovotestes
109. True Hermaphroditism
Ovarian portion of the ovotestis is frequently normal, whereas the
testicular portion is typically dysgenetic
66% of patients are 46 XX
Gonadal tumors is approximately 10% in 46,XY true hermaphroditism
and 4% in 46,XX true hermaphroditism
Most important aspect of management in true hermaphroditism is
gender assignment
Sex assignment should be based on the functional potential of external
genitalia, internal ducts, and gonads, according to the findings at
laparoscopy or laparotomy.
Unlike patients with most other forms of gonadal dysgenesis, true
hermaphrodites have the potential for fertility if raised as female
with the appropriate ductal structures
Males, remove ovaries and/or ovotestis and mullerian duct structures
consider gonadectomy
Females remove all testicular and wolffian structures
110. Noonan syndrome
Both affected males and females have apparently normal
chromosome complements and normal gonadal function
The phenotype appearance of Turner syndrome
: short stature, webbed neck, shield chest & cardiac malformations
(esp, pulmonic stenosis)
The trait as autosomal-dominant with variable expression
111. MANAGEMENT OF NEWBORN
WITH AMBIGUOUS GENITALIA
GENERAL GIUDELINES
Medical and social emergency
Avoid immediate declaration of sex
Proper counselling of the parents
Team management; obstetrician,
neonatologist, pediatric endocrinolgist,
genetist and paediatric surgeon.
112. EVALUATION AND MANAGEMENT OF THE
NEWBORN WITH AMBIGUOUS GENITALIA
Medical and psychosocial emergency to be handled with great sensitivity
toward the family
Goals:
– precise diagnosis of the intersex disorder
– assign a proper sex of rearing based on the diagnosis
– determine the status of the child's anatomy
– delineate the functionality of genitalia and reproductive tract
Valuable history points:
– infant death
– infertility
– amenorrhea
– hirsutism
– maternal medications (i.e. steroids , OCP), during pregnancy
Physical examination: the presence of one or two gonads
Distinctly palpable gonad along the pathway of descent is highly suggestive
of a testis
113. MANAGEMENT OF NEWBORN
WITH AMBIGUOUS GENITALIA
DIAGNOSIS
History : pregnancy; family
Detailed examination
; Abdomen; pelvis; external genitalia; urethral and anal openings
– Are gonads palpable?
– What is the phallus length?
– What is the position of the urethral meatus?
– To what degree are the labioscrotal folds fused?
– Is there s vagina, vaginal pouch, or urogenital sinus?
– Dehydration, hypotension, hyperpigmentation in adrenal hyperplasia
115. EVALUATION AND MANAGEMENT OF THE
NEWBORN WITH AMBIGUOUS GENITALIA
Posterior urethral meatal position is a strong
predictor of intersex 65%, versus 5% to 8% with a
midshaft to anteriorly located hypospadiac meatus
Penile size should be assessed and an accurate
measure of stretched penile length recorded.
Precise means of assessing müllerian anatomy is by
pelvic ultrasound
Karyotype should be obtained
Serum studies should be immediately sent to rule out
a salt-wasting form of CAH.
Serum electrolytes, testosterone and DHT should be
measured early
116. MANAGEMENT OF NEWBORN
WITH AMBIGUOUS GENITALIA
Investigations
• Pelvic US and sometimes MRI or Genitogram
• Karyotype
• Rule out Cong. Adrenal hyperplasia
Serum electrolytes; 17-OHP level,11-DOC & urinary levels of 17-ketosteroids
• Serum androgen (androstenedione, testosterone, DEA, DEAS)
• Laparoscopy
• Gonadal biopsy (Laparotomy)
117.
118. Gender Assignment
Issues related to the diagnosis-specific potential for normal sexual
functioning and fertility and the risk of gonadal malignancy should be
addressed
In the setting of a 46,XX karyotype, gender assignment is usually
appropriately female
If the karyotype is 46,XY, the issue is a more complex one and includes
factors such as penile length and evidence of androgen insensitivity
The degree of masculinization of the external genitalia appears to vary with the
amount of testicular tissue present
– gender assignment depends on the functional potential of the gonadal
tissue, reproductive tracts, and genitalia
Parameters of Optimal Gender Policy (Meyer-Bahlberg, 1998)
– Reproductive potential (if attainable at all)
– Good sexual function
– Minimal medical procedures
– An overall gender-appropriate appearance
– A stable gender identity
– Psychosocial well being
Notas del editor
A and B , An untreated girl with the non–salt-losing form of congenital adrenal hyperplasia. Androgens caused disproportionate acceleration of bone maturation compared with stature. C , Virilized adult female with non–salt-losing adrenal hyperplasia. The patient had a deep voice, shaved daily, and wore a toupee for baldness. After treatment with cortisone, her 17-ketosteroid levels fell to normal values, her breasts enlarged, she underwent a normal menarche, and hair regrew on her head. Note short stature and short extremities. D , Female pseudohermaphroditism caused by maternal ingestion of an oral progestational compound from the 8th to 12th week of pregnancy. Labioscrotal fusion is sufficient to obscure the vaginal orifice and create a urogenital sinus. Clitoris is enlarged. There is no progressive virilizing tendency. (C, from Wilkins L. The Diagnosis and Treatment of Endocrine Disorders in Childhood and Adolescence, 3rd ed. Springfield, IL, Charles C Thomas, 1965.)
Because testosterone production never significant, brain imprinting not a factor in gender assignment.
At least one Y and two X to be Klinefelter’s. ICIS intracytoplasmic sperm injection
A 19-year-old phenotypic male with chromatin-positive seminiferous tubule dysgenesis (Klinefelter's syndrome). The karyotype was 47,XXY, gonadotropin levels were elevated, and testosterone levels were low normal. Note normal virilization with long legs and gynecomastia (B, C) . The testes were small and firm and measured 1.8 × 0.9 cm. Testicular biopsy revealed a severe degree of hyalinization of the seminiferous tubules and clumping of Leydig cells. D , A 48-year-old male with 47,XXY Klinefelter's syndrome with severe leg varicosities.
Characterized by … Patients typically present for evaluation of gynecomastia. Androgen replacement and reduction mamoplasty in selected pts. Lack of germ cell elements obviates testicular biopsy & ICSI (intracytoplasmic sperm injection)
Three patients with 45,X/46,XY sex chromosome mosaicism who illustrate the highly variable phenotype in this variant of the syndrome of gonadal dysgenesis. (Numbers of the patients refer to designation in Table 22-13 .) A , Patient 1, a phenotypic female, was age 15 years, 4 months. She had short stature (-3.1 SD), an increased number of pigmented nevi, puffiness over the dorsa of fingers, and broad and short hands, and she was sexually infantile (breast development seen in photograph followed estrogen therapy) except for sparse pubic and axillary hair. The urinary gonadotropins were markedly elevated. B , Patient 3, aged 3 years, 1 month, had ambiguous external genitalia, perineal hypospadias, and undescended gonads. He was of average height and had a broad chest and a duplication of the left kidney. C , Patient 9, aged 8 years, 1 month, was a phenotypic male with a penile urethra and unilateral undescended gonad, average height, cubitus valgus, short fourth metacarpals, and puffiness of dorsa of fingers. By age 15, male secondary sexual characteristics were well advanced and a left scrotal testis, which was normal in histologic appearance, measured 4.0 × 2.4 cm.
Closely related to Turner’s syndrome In contrast to Turner’s growth hormone here is normal.
Elevated LH likely responsible for androgen production clitoromegaly
The syndrome entails the presence of testes that "vanish" during embryogenesis and is distinguished from pure gonadal dysgenesis, in which there is no evidence of testicular function in utero. Possible etiology genetic mutation, teratogen, bilateral torsion. At puberty males get androgens and females get estrogen supplementation.
75% raised male; hypospadius and chordee in about 80%. Virtually all have UG sinus present and most have uterus present. 2/3 are 46,XX karyotype but 46,XY and mosaics occur less commonly. Fallopian tubes present on the side of ovary and vas deferens present adjacent to testis. A 17-year-old true hermaphrodite with bilateral scrotal ovotestes and a 46,XX sex chromosome constitution in cultures of peripheral blood and skin, perineal hypospadias (partially repaired in photograph), moderate bilateral gynecomastia and pubic hair (recently shaved in picture), sparse axillary hair, a high-pitched voice, and absent facial hair. Height was 168 cm. Urinary 17-ketosteroid level was 1.3 mg/day; urinary gonadotropin levels were elevated. A male type of urethra, bilateral scrotal fallopian tubes and ovotestes, and rudimentary bicornuate uterus and vagina attached to the posterior urethra were seen at operation. The photomicrographs show histopathology of the ovarian and testicular portion of one ovotestis. B , Immature seminiferous tubules lined with Sertoli cells and spermatogonia and Leydig cells. C , Ova and follicles. (From Grumbach MM, Barr ML. Cytologic tests of chromosomal sex in relation to sexual anomalies in man. Recent Prog Horm Res 1958; 14:255–334.)
Partial gonadectomy possible in female but stimulate the bHCG post op to ensure all testicular tissue removed.
Presence of one or two gonads on exam rules out female pseudohermaphroditism Because ovaries do not descend…
Diagnostic algorhythm for newborn with ambiguous genitalia based on gonadal palpability, presence or absence of mullerian structures, 17, hydroxyprogesterone concentration, and karyotype If no testes check for elevated LH or stimulate with hCG to demonstrate testicular tissue.
Study by Kaefer and associates 1999, studied incidence of intersex in pts with chriptorchidism and hypospadius without ambiguous genitalia. Karyotype usually takes 2-3 days, but can get rapid analysis with FISH (fouorescent in situ hybridizaiton) few hrs.
High quality data regarding long-term psychosocial outcomes of gender assignment are lacking at this point but longitudinal studies are being persued. 46, XX Normal ovaries, mullerian ducts, and reproductive potential. 46, XY if complete androgen insensitivity then female appropriate gender, whereas 5a-reductase deficiency more appropriately male. Most frequent abnormal karyotype is 45X/46XY mosaicism variable phenotypic pattern. Ultimately this is a challenging and humbling process to say the least