Abstract
The etiology of hyperandrogenic chronic anovulation is heterogeneous and relatively
unknown in the majority of cases. Affected individuals in this latter segment are
considered to have polycystic ovary syndrome (PCOS) of which 50 to 60% exhibit androgen
excess of adrenal origin. An understanding of normal adrenal function provides insight
into the factors that contribute to adrenal androgen excess in PCOS. Since pituitary
ACTH secretion promotes developmental growth and overall steroidogenic efficiency
within the adrenal cortex, it is probable that these actions of ACTH along with the
adrenal's unique centripetal circulation play a major role in the induction of adrenarche.
This latter phenomenon is characterized by alterations in adrenocortical morphology
and steroidogenic enzyme activities culminating in increases in adrenal androgens
to normal circulating adult levels. Thus, it is not surprising that adrenal dynamic
testing has revealed increased 17,20 lyase activity or adrenal androgen hyper-responsiveness
to ACTH as the two abnormalities leading to adrenal androgen excess in PCOS. Whereas
17,20 lyase hyperactivity diagnosed by defined criteria in response to pharmacological
ACTH may be an intrinsic genetic defect, increases in 17,20 lyase activity and adrenal
androgen hyper-responsiveness to ACTH in response to physiological ACTH may be promoted
by the functional elevation of estrogen of ovarian origin in PCOS. The latest in vitro
data suggest the estrogen may elicit its effect on the adrenal cortex through a receptor
mediated mechanism. Therefore, the currently available data indicate that adrenal
androgen excess in PCOS is also heterogeneous etiology.
Keywords:
Adrenal morphology - adrenal dynamic testing - 17,20 lyase hyperactivity - adrenal
androgen hyper-responsiveness to ACTH - ovarian induced adrenal hyperandrogenism
