Original Articles: Hormones and Reproductive Health
Aromatization Mediates Testosterones Short-Term Feedback Restraint of 24-Hour Endogenously Driven and Acute Exogenous Gonadotropin-Releasing Hormone-Stimulated Luteinizing Hormone and Follicle-Stimulating Hormone Secretion in Young Men1
J. A. Schnorr2,
M. J. Bray and
J. D. Veldhuis
Division of Endocrinology, Departments of Internal Medicine and
Obstetrics and Gynecology, General Clinical Research Center,
Center for Biomathematical Technology, University of Virginia School of
Medicine, Charlottesville, Virginia 22908
Address all correspondence and requests for reprints to: J. D. Veldhuis, M.D., Division of Endocrinology, Department of Internal Medicine, Box 202, University of Virginia Health System, Charlottesville, Virginia 22908. E-mail: JDV{at}Virginia.Edu
Abstract
The present clinical study examines the neuroregulatory hypothesisthat
feedback restraint of LH and FSH secretion by testosteronerequires
in vivo aromatization. To test this postulate, we
prospectivelyand randomly assigned 47 healthy young men to 1 of 5
parallelshort-term (5-day) double-blind interventions with: 1)
placebo;2) high-dose ketoconazole (KTCZ, 400 mg orally 4 times daily)
toblock both Leydig-cell and adrenal steroidogenesis; 3) KTCZand
transdermal testosterone delivery (7.5 mg daily); 4) KTCZand
transdermal estradiol (0.05 mg daily); or 5) KTCZ, testosterone,
andthe selective and potent aromatase inhibitor, anastrazole (5mg
orally twice daily). Blood was sampled every 10 min for 27h on
the last day of intervention to quantitate 24-h mean spontaneousand
3-h post-GnRH-stimulated (100 ng/kg iv bolus) LH and FSHrelease. KTCZ
administration lowered the serum total testosteroneconcentration
markedly from (mean ± SEM) 423 ±57 ng/dL
(15 ± 2.0 nmo/L) during placebo ingestion to58 ± 8.6 ng/dL
(2.0 ± 0.3 nmol/L) (P <
10-3).Transdermal androgen addback along with
KTCZ blockade increasedtestosterone levels to 607 ± 57 ng/dL
(21 ± 2.0nmol/L). KTCZ exposure alone drove a 3-fold increase in
serumLH concentrations (P <
10-3) and a 2.5-fold rise in FSH secretion
(P= 0.015), as assessed by high-specificity
immunoradiometricassays. Concomitant transdermal testosterone (or
estradiol)delivery repressed the elevated secretion of both LH and FSH
tomid-normal baseline values. A 3-fold administration of anastrazole,
KTCZ,and testosterone completely opposed exogenous testosterones
suppressionof 24-h LH and FSH secretion. Anastrazole coadministration
likewiseabolished testosterone-dependent inhibition of 3-h
GnRH-stimulatedLH and FSH release. In summary, assuming the
specificity ofanastrazoles inhibition of aromatase activity, we
concludethat circulating testosterone in healthy men curtails
endogenouslydriven as well as exogenous GnRH-stimulated LH and FSH
secretionconditional on its in vivo aromatization.
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