Moreover, all the women with PCOS reported oligomenorrhea from the time of menarche, whereas type 2 diabetes developed during their late 20s and early 30s. Therefore, it seems likely that PCOS preceded the development of type 2 diabetes by many years.
CONCLUSIONS
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ABSTRACT
INTRODUCTION
RESEARCH DESIGN AND METHODS
RESULTS
CONCLUSIONS
References
It has been established that women with PCOS have a markedly increased risk of developing type 2 diabetes (6,7). However, the prevalence of PCOS in premenopausal women with type 2 diabetes is unknown. In our study, we screened the charts of 618 women with type 2 diabetes and identified 47 premenopausal women who met our eligibility requirements. The low percentage of premenopausal women (7.6%) in this clinic population is not surprising because the onset of type 2 diabetes typically occurs after the age of 50 years.
After further evaluation, eight premenopausal women with type 2 diabetes were diagnosed with PCOS. If only the 30 women who participated in the study are included, this is a prevalence rate of 26.7%. If all 47 eligible women are included, including those who could not be contacted or refused to participate, the 17% prevalence rate is still fourfold higher than the reported prevalence of 4.6% for nondiabetic women (1). The women with PCOS did not differ from the unaffected women with respect to diabetic history, weight, or ethnic background.
To date, only one other study has addressed this question, albeit using a different approach. To determine the prevalence of PCOS among premenopausal women in the diabetes clinic at Middlesex Hospital in England, Conn et al. (8) performed transvaginal ultrasonography in 38 women with type 2 diabetes, and 31 (82%) had anatomically polycystic ovaries. This ultrasonographic finding alone does not establish the diagnosis of PCOS because it has been reported that up to 24% of normal eumenorrheic women have polycystic ovaries on ultrasonography (11). Further evaluation revealed that 8 of the 38 women (21%) had either oligomenorrhea or amenorrhea, whereas 11 women (29%) had hirsutism. If we assume that all of the women with menstrual abnormalities also suffered from hirsutism, then the resulting 21% prevalence of PCOS in this population compares well with the 26.7% prevalence found in our present study.
We recognize that because this study was conducted at an academic medical center known for its interest in PCOS, the potential of ascertainment bias exists. Patients with both type 2 diabetes and PCOS may be preferentially referred to our institution by community physicians. To explore this possibility, we examined the initial referral visit of each patient with oligomenorrhea. Of the eight oligomenorrheic women, only two were referred with a dual diagnosis of PCOS and type 2 diabetes. Two women were referred for evaluation of oligomenorrhea and were subsequently found to also have type 2 diabetes. The remaining four women were referred for diabetes treatment only, and neither oligomenorrhea nor hirsutism was noted on the initial visit.
Perhaps most surprising, two of the eight women were not diagnosed with PCOS until their enrollment into this study, despite being actively followed in our diabetes clinic by physicians with special expertise in the syndrome. Hence, 25% (two of eight) women with PCOS remained unrecognized, and therefore not treated, for the disease in this subspecialty clinic.
In summary, PCOS was observed in approximately one of every four premenopausal women with type 2 diabetes, and had been undiagnosed in 25% of the case subjects. This is clinically significant because of the known reproductive morbidity associated with untreated disease. Physicians can quickly assess women with type 2 diabetes for PCOS by taking a menstrual history and noting clinical signs of hyperandrogenism. Finally, limited anecdotal experience in our clinic suggests that women with type 2 diabetes and PCOS who are treated with insulin may benefit from discontinuation of insulin therapy and use of an insulin-sensitizing drug. We have noted that after this therapeutic change, some women demonstrate a decrease in serum androgens and improved menstrual cyclicity. This result was not unexpected given recent reports of the salutary effects of insulin-sensitizing drugs in this syndrome (121314). A formal study assessing the efficacy of this practice in this population is warranted.
ACKNOWLEDGMENTS
This work was supported by National Institutes of Health Grant M01-RR00065 and an A.D. Williams/Aesculapian Student Summer Research Fellowship from Virginia Commonwealth University.
FOOTNOTES
Address correspondence and reprint requests to John E. Nestler, MD, Medical College of Virginia, P.O. Box 980111, Richmond, VA 23298-0111. E-mail:
nestler@hsc.vcu.edu.
Received for publication 10 November 2000 and accepted in revised form 22 February 2001.
A table elsewhere in this issue shows conventional and Système International (SI) units and conversion factors for many substances.
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RESEARCH DESIGN AND METHODS
RESULTS
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