Journal of Adolescent Health Care
Volume 11, Issue 6 , Pages 480-484, November 1990

Preliminary results suggesting exaggerated ovarian androgen production early in the course of polycystic ovary syndrome

  • Gary L. Francis, M.D., Ph.D.

      Affiliations

    • Corresponding Author InformationAddress reprint requests to: Gary L. Francis, LTC, Department of Pediatrics, Walter Reed Army Medical Center, Washington, DC 20307-5001.
    • From the Department of Pediatrics, Eisenhower Army Medical Center, Fort Gordon, Georgia, USA
  • ,
  • Alan Getts, M.D.

      Affiliations

    • From the Department of Pediatrics, Eisenhower Army Medical Center, Fort Gordon, Georgia, USA
  • , Ph.D.
  • J.C. Mcpherson III

      Affiliations

    • From the Department of Clinical Investigation, Eisenhower Army Medical Center, Fort Gordon, Georgia, USA

Accepted 6 March 1990.

Abstract 

Excess ovarian androgen production might be a cause of the polycystic ovary syndrome (PCO). Previous studies have evaluated adult women with long-standing abnormality of the hypothalamic-pituitary gonadal axis. Abnormal ovarian function in such patients could be a primary or even a secondary finding. For that reason, this study was designed to evaluate ovarian androgen production in symptomatic adolescent females. Simultaneous adrenal suppression, by using dexamethasone, and ovarian stimulation, by using gonadotropin-releasing hormone (GnRH), were achieved in 12 patients. Following stimulation, blood was serially obtained over 8 hr to measure gonadotropin, estrogen, and androgen responses. Based on the androgen response, patients could be divided into two groups. Group A (five) had a significant increase (p < 0.01) in free testosterone, whereas group B (seven) had no increase in any androgen, including free testosterone (significantly different from group A, p = 0.01). All patients in group A had enlarged or cystic ovaries, whereas only one-quarter patients in group B had enlarged ovaries (significantly different from group A, p < 0.03). The pituitary and estrogenic response was similar in both groups. These preliminary data suggest that some patients with PCO (group A) have a primary abnormality in ovarian androgen production early in the course of their disease.

Keywords: Polycystic ovary Androgen GnRH

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 The opinions or assertions contained herein are the private views of the authors and are not to be construed as official or as reflecting the views of the Department of the Army or the Department of Defense.

PII: 0197-0070(90)90106-C

Journal of Adolescent Health Care
Volume 11, Issue 6 , Pages 480-484, November 1990