Polycystic Ovary Syndrome Clinical Trial
Official title:
Effect of Increased Circulating Androgens on Granulosa Cell Responses to FSH
The purpose of this study is to evaluate the effect of increased circulating androgens on estradiol production by the granulosa cells in response to FSH stimulus.
Various previous studies have demonstrated that androgens enhance granulosa cell function in
a variety of animal species including rodents and non-human primates. In vitro studies have
shown that granulosa cells exposed to either testosterone or dihydrotestosterone exhibit
increased production of estrogen, progesterone and inhibin in response to FSH. Studies done
in non-human primates have also shown that androgen increases the numbers of preantral and
antral follicles as well as increases FSH receptor mRNA expression in granulosa cells. This
suggests that granulosa cell hyperresponsiveness to FSH in polycystic ovary syndrome (PCOS)
may be related to androgen excess. The investigators plan to address this possibility by
performing a series of in vivo studies. In one of the investigator's prior studies androgen
blockade was done by administration of flutamide and E2 responses to FSH assessed. This
study has been completed and the manuscript is being prepared for publication. In the
present protocol, the investigators propose to further study the role of androgens with a 2
phase study. In the first phase the investigators plan to suppress endogenous steroid
hormone production by the ovaries via treatment with the GnRH analog Lupron for 4 weeks
beyond which a gradual resumption of ovarian activity will occur. Granulosa cell (inhibin B)
responses to FSH will be examined before and after ovarian suppression as well as during
early and moderate recovery of ovarian steroidogenesis. These results will provide control
data to which comparisons can be made from results of the next phase.
In the second phase, after a 2 month washout interval, the same subjects will again receive
Lupron to suppress endogenous steroid production. After 4 weeks, at the beginning of ovarian
activity resumption, the investigators will administer Letrozole 5mg for 14 days and again
examine granulosa cell responses to FSH during recovery. Letrozole is a 3rd generation
aromatase inhibitor which results in suppression of E2 production and increase in
circulating serum androgen levels to about 40% greater than pre-treatment values. It is now
also being used for ovulation induction. It has minimal side effects and is in general very
well tolerated. By using Letrozole for 2 weeks after GnRH suppression of the ovaries, the
investigators will more effectively increase the amount of circulating androgen while
keeping estrogen at low levels, thereby allowing the investigators to more completely study
the effects of isolated and elevated androgen levels on granulosa cell responses to FSH. By
comparing results obtained in phase 1, the investigators will be able to determine if there
is an androgen mediated response by granulosa cells to FSH stimulation in the absence of
other ovarian steroids. Also, the addition of a control group will allow investigators to
determine if the granulosa cell response is different between PCOS and normals.
It is hypothesized that there will be a significant rise in inhibin B production by the
granulosa cells in PCOS women in response to FSH after treatment with Letrozole as compared
to both the control group and to responses observed in the control phase of study. This
would confirm that androgens are indeed responsible at least in part for the
hyperresponsiveness to FSH seen in women with PCOS.
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Allocation: Non-Randomized, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Health Services Research
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