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Metformin Effects on Clinical Features, Endocrine and Metabolic Profiles, and Insulin Sensitivity in Polycystic Ovary Syndrome: A Randomized, Double-Blind, Placebo-Controlled 6-Month Trial, followed by Open, Long-Term Clinical Evaluation¹

Division of Endocrinology and Metabolic Diseases (P.M., R.C., C.N., F.T., F.P., M.M.), and Division of Medical Statistics (E.Z.), University of Verona, Verona; Laboratory of Clinical Chemistry (M.C.), Ospedale Maggiore, Verona, Italy

Address correspondence and requests for reprints to: Dr. Paolo Moghetti, Divisione di Endocrinologia e Malattie del Metabolismo, Ospedale Maggiore, P.le Stefani, 1 I-37126 Verona, Italy. E-mail: moghetti{at}iol.it

	Abstract

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In the last few years some studies assessed the effects of attenuation of hyperinsulinemia and insulin resistance, obtained by insulin sensitizing agents, in women with polycystic ovary syndrome (PCOS), suggesting potential scope for these drugs in treating the whole spectrum of reproductive, endocrine, and metabolic abnormalities found in such subjects. However, the results of these studies, mostly uncontrolled and short-term, are still inconclusive, and there is no long-term follow-up. In the present study, 23 PCOS subjects [mean (± SE) body mass index 30.0 ± 1.1 kg/m²] were randomly assigned to double-blind treatment with metformin (500 mg tid) or placebo for 6 months, while maintaining their usual eating habits. Before and after treatment, menstrual history, endocrine and metabolic profiles, serum 17-hydroxyprogesterone response to GnRH-agonist testing, and insulin sensitivity measured by the glucose clamp technique were assessed. Eighteen of these women, as well as 14 additional PCOS patients, were subsequently given metformin in an open trial for 11.0 ± 1.3 months (range 4–26), to assess long-term effects of treatment and baseline predictors of metformin efficacy on reproductive abnormalities. After metformin treatment, mean frequency of menstruation improved (P = 0.002), due to striking amelioration of menstrual abnormalities in about 50% of subjects. Women given metformin showed reduced plasma insulin (at fasting: P = 0.057; during the clamp studies: P < 0.01) and increased insulin sensitivity (P < 0.05). Concurrently, ovarian hyperandrogenism was attenuated, as indicated by significant reductions in serum free testosterone (P < 0.05) and in the 17-hydroxyprogesterone response to GnRH-agonist testing (P < 0.05). No changes were found in the placebo group. Only comparable minor changes in body mass index were found both in the metformin group and in the placebo group. In the open, long-term trial 17 women (54.8%) showed striking improvements of their menstrual abnormalities and were considered as responders. Logistic regression analysis of baseline characteristics in responders and nonresponders showed that plasma insulin, serum androstenedione, and menstrual history were independent predictors of the treatment’s clinical efficacy. In 10 subjects whose menses proved regular after treatment, the great majority of cycles became ovulatory (32 out of 39 assessed, 79%). In conclusion, in women with PCOS metformin treatment reduced hyperinsulinemia and hyperandrogenemia, independently of changes in body weight. In a large number of subjects these changes were associated with striking, sustained improvements in menstrual abnormalities and resumption of ovulation. Higher plasma insulin, lower serum androstenedione, and less severe menstrual abnormalities are baseline predictors of clinical response to metformin.

	Introduction

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POLYCYSTIC ovary syndrome (PCOS) is a common and heterogeneous disorder of women of reproductive age, characterized by hyperandrogenism and chronic anovulation (1). The pathogenesis of PCOS is still largely unknown, and until now medical care of these subjects has been limited to symptomatic control of cosmetic concerns, menstrual dysfunction, and infertility. Women with the syndrome are frequently insulin resistant, independent of obesity (2). In this regard, several data support the hypothesis that insulin resistance and the associated hyperinsulinemia play a pathogenetic role in PCOS (2). Insulin has direct effects on ovarian steroidogenesis in vitro, stimulating androgen synthesis in thecal cells (3); it also decreases serum sex hormone-binding globulin synthesis in the liver (4), increasing free androgen levels. Furthermore, in vivo studies suggest a potentation by hyperinsulinemia of ACTH-stimulated adrenal androgen secretion (5). All these effects of insulin may contribute to the androgen excess of women with PCOS. Consistently, decreasing insulin secretion by diazoxide (6) or somatostatin (7) in these subjects has resulted in concurrent reductions of serum androgens.

These observations suggested that insulin sensitizing agents, such as metformin or troglitazone, should be tested for the treatment of PCOS. These drugs improve insulin sensitivity by different mechanisms, thus determining a subsequent reduction in plasma insulin levels (8, 9). Recently, some short-term studies supported this hypothesis, reporting significant reductions of serum androgens in women with PCOS given either metformin (10, 11, 12, 13) or troglitazone (14, 15). Interestingly, improvements in reproductive abnormalities of these patients have also been reported in some of these studies (13, 16). On the other hand, other authors failed to observe any clinical or biochemical changes after metformin (17, 18). These discrepancies are not easily explained. In addition, controlled long-term studies assessing the clinical effects of these treatments are still lacking.

The present study was designed to assess, with a randomized, double-blind, placebo-controlled protocol, the effects on menstrual abnormalities of a 6-month course of metformin in a group of 23 subjects with PCOS with normal glucose tolerance. Subsequently, 18 of these subjects and 14 additional women with PCOS were included in an open trial to evaluate the long-term effects of metformin on clinical features of the syndrome and to determine any baseline predictors of the treatment’s efficacy.

	Materials and Methods

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Subjects and study protocols

Protocol A (double-blind study). Twenty-three caucasian women with PCOS, ages between 18–35 yr and with normal glucose tolerance by the criteria of the World Health Organization (19), were recruited for the double-blind, placebo-controlled study. All these subjects were referred to our division for menstrual abnormalities, with or without hirsutism.

Diagnosis of PCOS was based on the presence of hyperandrogenic chronic anovulation, after exclusion of Cushing’s syndrome, late-onset 21-hydroxylase deficiency, thyroid dysfunction, hyperprolactinemia, or androgen secreting tumors, according to recommendations of the NICHHD consensus conference on PCOS (2). No subject had other diseases or was taking medications.

All these women had an abnormal response of serum 17-hydroxyprogesterone to GnRH-agonist stimulation (20). Twenty of them had severe oligoamenorrhea (6 or fewer menses per year), whereas 3 women had less severe irregularities in menstrual cycles. In these 3 subjects, anovulation was confirmed by serum progesterone assessment in the luteal phase of the cycle.

The large majority of these subjects were overweight (mean body mass index 30.0 ± 1.1, range 19.0–38.7 kg/m²). Sixteen of them (70%) showed increased plasma insulin response to oral glucose, a rough parameter of insulin resistance.

Women were randomly assigned to double-blind oral metformin or placebo for 6 months. The dose of the study drug was increased stepwise, from 500 mg (1 capsule) once daily for the first week to 500 mg bid for the next week, and to 500 mg tid for a further 24 weeks. Patients were instructed not to modify their usual eating habits throughout the study.

Metformin effects on menstrual abnormalities of women with PCOS were evaluated by assessing post-treatment changes in frequency of cycles. Furthermore, changes in several endocrine and metabolic features of the syndrome were also assessed.

Thus, before and at the end of study, the following were carried out:

1. Assessment of menstrual history, with recording of menses in the 6-month periods before the study and during treatment;
   
2. Physical examination for body weight, waist/hip ratio, hirsutism score, measured by a modification of the Ferriman-Gallwey method (21), and blood pressure, measured by a mercury sphygmomanometer with the subject in the sitting position, after a rest of at least 5 min;
   
3. Venous blood withdrawal, after overnight fasting, for serum gonadotropins, androgens (total and free testosterone, dehydroepiandrosterone sulfate, androstenedione), 17-hydroxyprogesterone, estradiol, sex hormone-binding globulin and lipoproteins (total and HDL cholesterol, triglycerides);
   
4. GnRH-agonist challenge (20), with measurement of serum 17-hydroxyprogesterone, gonadotropins and estradiol, 24 h after 0.1 mg buserelin sc, as previously described (22);
   
5. Oral glucose tolerance test, with plasma glucose and insulin measurements on samples obtained every 30 min for 2 h;
   
6. Insulin sensitivity assessment by the glucose clamp technique (see below), in 16 out of 23 women participating in the protocol. The remaining subjects did not give their consent to this procedure.
   

All baseline evaluations were carried out in the early follicular phase of the menstrual cycle, or after at least 3 months of amenorrhea.

Each woman was asked to report any side-effect during the treatment. In addition, safety parameters (hematology, liver and renal function, serum electrolytes and uric acid) were assessed before and at 2-month intervals during the study.

All subjects gave their informed written consent before entering the study, which was conducted in accordance with the Declaration of Helsinki and approved by the institutional ethical committee.

Protocol B (open, long-term study). Eighteen out of the 23 women included in protocol A received metformin in an open design providing treatment for an unscheduled duration after the completion of the double-blind study, to assess long-term effects of treatment and to determine any predictors of the efficacy of metformin. Fourteen additional, previously untreated, severely oligoamenorrheic women with PCOS were also included in this protocol. Thus, the total number of subjects participating in the open study was 32, 21 overweight and 11 lean. These additional women with PCOS were evaluated at baseline by the procedures indicated in protocol A, except for the glucose clamp. Subjects participating in this protocol also gave their informed consent before entering the study. A placebo group was not included in this long-term protocol, as it was considered unethical after results of the double-blind study. Moreover, a control group is irrelevant to assessment of therapeutic efficacy predictors.

In all patients, metformin dosage was increased stepwise as indicated above, and the following were assessed at 4-month intervals: changes in menstrual history (main outcome), side effects, body weight, hirsutism score, blood pressure, fasting plasma insulin, serum testosterone, gonadotropins, sex hormone-binding globulin, and lipids. GnRH-agonist challenge was repeated after 4–6 months of metformin in 19 subjects.

To assess the effects of treatment on ovulatory function, serum progesterone levels were repeatedly measured in the luteal phases of subjects experiencing regular menses after metformin treatment. Ten women accepted these additional assessments, which were carried out in an overall total of 39 cycles. Ovulation was presumed to have occurred when serum progesterone exceeded 18 nmol/L.

Insulin sensitivity

Insulin sensitivity was measured by the euglycemic hyperinsulinemic glucose clamp, as previously described (5). Briefly, after overnight fasting, a primed, continuous insulin infusion (Humulin R, Eli Lilly & Co., Indianapolis, IN) was started; this was maintained for 120 min, at a constant rate of 80 mU/m² x min, which makes it possible to reach steady-state plasma insulin levels in the high in vivo range. Euglycemia was maintained throughout the test with a variable infusion of 20% dextrose, adjusted by monitoring plasma glucose levels in arterialized venous blood, approximately every 10 min. We previously found that in nondiabetic hyperandrogenic subjects endogenous glucose production was negligible at this insulin infusion rate (22). Therefore, the amount of glucose infused into each subject may be considered equivalent to the whole body insulin-induced glucose uptake.

Assays

Plasma insulin was measured by a specific immunoradiometric assay (cross-reactivity with proinsulin <5%), using a kit from Biosource Technologies, Inc. (Fleurus, Belgium). Serum gonadotropins, androgens, progesterone, 17-hydroxyprogesterone, estradiol, sex hormone-binding globulin and lipoproteins were measured by commercial kits, as previously described (22).

Statistical analysis

Differences in baseline characteristics between the two groups (metformin and placebo) were analyzed by Student’s t test (two-tailed). The Mann-Whitney U test and Wilcoxon matched pairs signed rank sum test were used for hirsutism score data.

The difference in frequency of menstruation before and after the trial, a normally distributed variable, was studied by analysis of covariance, so that the effect of intergroup differences in basal body mass index and androgens could be accounted for.

Free testosterone levels and other relevant clinical, endocrine and metabolic features were analyzed by repeated measures analysis of variance. SPSS, Inc. Release 6.0 (SPSS, Inc., Chicago, IL) was used for these analyses.

For the open long-term study, Student’s t test was used to analyze differences in main baseline characteristics of responders and nonresponders. Predictors of response to metformin were identified by logistic regression, by the EGRET program (Statistics and Epidemiology Research Corp., EGRET, Seattle, WA).

	Results

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Double-blind, placebo-controlled study

Clinical and endocrine features. Table 1 shows the main characteristics of women given metformin or placebo, at baseline and after treatment. At baseline, the placebo group had significantly higher body mass index, whereas serum androgens tended to be higher in the metformin group.

Five subjects given metformin and two subjects given placebo reported the following mild to moderate side effects: nausea (n = 5), heartburn (n = 1), and mild abdominal pain (n = 1) in the metformin group; nausea (n = 2), vertigo (n = 1), and headache (n = 1) in the placebo group. These resolved within 4 weeks in all patients except one, receiving metformin, who required a stable reduction of the study drug dose to 1 capsule bid.

Menstrual abnormalities. Figure 1 shows the median and interquartile range of the changes after treatment in frequency of menstruation, in both groups. After treatment, the metformin group showed a significant improvement in frequency of menstruation, whereas no change was observed in subjects receiving placebo (P = 0.002 between groups, controlling for baseline body mass index and androstenedione). Five women in the metformin group vs. none in the placebo group had their menstrual pattern substantially improved during treatment. In subjects experiencing regular menses after metformin, improvement was observed within 3 months.

View larger version (34K): [in this window] [in a new window]   Figure 1. Boxplot of the differences in frequency of menstruation (cycles per month) before and after the trial, in the metformin and the placebo groups (P = 0.002 between groups). The heavy bars represent the median values; the lower and upper limits of the boxes represent the interquartile range (25th and 75th percentiles, respectively); the I bars indicate the extreme values.

GnRH-agonist challenge. Before treatment, serum 17-hydroxyprogesterone levels at basal evaluation and after GnRH-agonist stimulation were similar between the two groups, as were serum gonadotropins. After treatment, 17-hydroxyprogesterone response to buserelin was significantly lowered in women given metformin (10.4 ± 1.6 vs. 14.2 ± 3.4 nmol/l), but not in those receiving placebo (12.0 ± 2.0 vs. 9.9 ± 1.3 nmol/l) (P < 0.05 between groups). In both groups, GnRH-agonist-induced increases in serum gonadotropins did not change significantly (data not shown).

Metabolic parameters. Before treatment, plasma glucose and insulin at fasting and after oral glucose were not significantly different between the two groups, though there was a tendency to higher fasting insulin levels in the placebo group. The baseline serum lipid profile was also similar between groups (Table 2).

Insulin sensitivity. Before treatment, women in both the metformin and placebo groups had similar steady-state insulin levels during the clamp studies (273 ± 21 vs. 274 ± 23 µU/mL, respectively). After treatment, these values were reduced in women receiving metformin (226 ± 19 µU/mL, P < 0.01 vs. baseline), whereas they were unchanged in subjects receiving placebo (271 ± 22 µU/mL, P = NS vs. baseline) (by ANOVA, P < 0.05 between groups). As insulin infusion rates were similar before and after treatment, these findings suggest raised metabolic clearance of the hormone after metformin.

To allow comparison of insulin sensitivity changes in the two groups, measures of insulin-induced glucose metabolism were corrected for ambient plasma insulin (M/I ratio). Whole body insulin-stimulated glucose uptake was significantly increased after metformin, indicating improved insulin sensitivity (Table 2).

Open, long-term study

Long-term tolerability. The women already given metformin in the double-blind study did not report any additional side-effect during the open, long-term trial. Among the remaining PCOS patients (those from the placebo group and the newly treated subjects), one woman complained of persistent abdominal pain, diarrhea and nausea; she continued to receive 1 capsule per day of metformin for 3 weeks, after which the treatment was discontinued. This patient was considered in the evaluation of tolerability, but not of clinical efficacy. Seven subjects complained of transient nausea, diarrhea and/or heartburn, which disappeared within 1 month.

Considering the side-effects reported by women given metformin in both protocols as a whole, 13 subjects (40.6%) had some discomfort during treatment (mild and transient in 11 and severe or persistent in 2).

Reproductive abnormalities. In the overall population of oligoamenorrheic women with PCOS given metformin in the open, long-term study (mean duration of metformin therapy 11.0 ± 1.3 months, median 8, range 4–26; figures inclusive of the previous 6 months of treatment for those subjects previously given the active drug in the double-blind protocol), the frequency of menses improved from 0.22 ± 0.04 to 0.59 ± 0.07 cycles per month per patient (P < 0.001). Thirteen of these subjects experienced complete regularization (i.e. uterine bleeding every 25–33 days, with normal duration and amount of blood loss), and another 4 reported striking amelioration of menstrual cycle abnormalities. These 17 women (54.8%) were considered as "responders." Fifteen of them were overweight and 2 lean. In another 14 women (5 overweight and 9 lean), there was no appreciable clinical improvement, or there was a slight amelioration of their menstrual history (in 3 of these subjects), possibly attributable to spontaneous fluctuations of menstrual abnormalities, after metformin. These subjects were considered as "nonresponders" (Fig. 2).

View larger version (28K): [in this window] [in a new window]   Figure 2. Frequency of menstruation (cycles per month) in individual PCOS subjects, classed as responders (closed circles) or nonresponders (open circles) to metformin in the open, long-term study.

In women with excessive hair growth, hirsutism scores were not improved after metformin (10.3 ± 2.5 vs. 12.6 ± 1.7, before and after treatment respectively, P = NS), independently of any change in menstrual cycle abnormalities.

	Discussion

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Velazquez et al. (10) first reported, in an uncontrolled study, a reduction of serum free testosterone in 29 nondiabetic women with PCOS, mostly overweight, given metformin for 8 weeks. This protocol was designed to evaluate the effects of attenuation of insulin resistance and hyperinsulinemia on the metabolic and endocrine features of PCOS. Unexpectedly, 3 of these subjects became pregnant, and menstrual cycles were normalized in another 7, who continued the treatment indefinitely. These findings prompted the testing of insulin sensitizing agents, such as metformin or troglitazone, for the treatment of both the metabolic and the endocrine abnormalities of women with PCOS.

In the last few years, a number of mostly uncontrolled short-term studies assessed the effects of these drugs in nondiabetic hyperandrogenic women, with varying results (23). Nestler and Jakubowicz (11) reported a controlled study in 25 obese women with PCOS, many with acanthosis nigricans–a marker of severe insulin resistance. After 4–8 weeks of metformin, there were significant reductions in serum insulin, free testosterone, and LH, and an increase in serum sex hormone-binding globulin. The women also showed an attenuation in serum 17-hydroxyprogesterone hyperresponse to GnRH-agonist stimulation, a hallmark of ovarian hyperandrogenism (20). These effects were independent of changes in body weight. Subsequently, the authors fully replicated their results in nonobese women with PCOS (12), indirectly confirming that effects of metformin were not dependent on weight loss. Neither of these studies directly measured insulin sensitivity, but reductions in insulin levels suggest improved insulin resistance. More recently, a short-term single-blind study from the same group showed that clomifene-induced ovulatory capacity is strikingly improved in obese women with PCOS given metformin for 2 months (16). In this study, a significant increase in spontaneous ovulation rate in the first month of treatment suggested potential early reversal of reproductive abnormalities in PCOS treated with metformin alone.

Two groups have examined the effects of troglitazone, given for 3 months, in massively obese women with PCOS (14, 15). These studies reported improvements in insulin sensitivity and reductions in serum testosterone (14, 15) and LH levels (14). After treatment, these women also showed an attenuation of abnormalities in glucose tolerance and insulin secretion and an increase in fibrinolytic capacity (15).

These short-term studies suggest that insulin sensitizers may affect the entire spectrum of endocrine, metabolic and reproductive abnormalities found in women with PCOS. On the other hand, other studies that assessed metformin effects in hyperandrogenic subjects did not confirm these findings (17, 18). The reasons for the striking discrepancies among these studies are not readily explained. Interestingly, where insulin levels were reduced by treatment, serum androgens were lowered as well.

A similar relationship was found in studies in which attenuation of hyperinsulinemia was obtained in obese subjects by weight loss (24, 25, 26). In this regard, Crave et al. (27) did not observe any additional benefit of metformin over the effects of diet alone, in a double-blind study comparing the effects of a 4-month low calorie diet vs. diet plus metformin in obese hirsute women. Unfortunately, this study was not specifically designed to recruit women with PCOS and actually the large majority of patients had regular menses. This weakens any conclusion, as hyperinsulinemia likely plays a major role in the pathogenesis of hyperandrogenism only in PCOS subjects (2).

The present controlled study was conducted in women with PCOS with normal glucose tolerance, mostly overweight. In these subjects metformin treatment for 6 months determined significant reductions in baseline serum free testosterone, as well as in the serum 17-hydroxyprogesterone response to GnRH-agonist testing. These data are consistent with the results obtained in short-term studies by the Nestler and Jakubovicz group (11, 12) and indicate that in PCOS subjects attenuation of ovarian hyperandrogenism after metformin treatment is sustained. In these women, insulin sensitivity, measured by the glucose clamp–the gold standard method to assess in vivo insulin action (28)–was improved, and consistent with this finding, plasma insulin levels were lowered. Furthermore, serum HDL cholesterol was increased, consistent with attenuation of both hyperinsulinemia and hyperandrogenemia (29, 30).

Interestingly, although improvements of insulin sensitivity in these women were not dramatic, effects of metformin on menstrual abnormalities were striking. About 50% of these subjects, most with severe oligoamenorrhea at baseline, had their cycles normalized. These effects of treatment were independent of changes in body weight and were shown to be sustained up to 2 years in the open, long-term protocol. In addition, consistent with the short-term findings of Nestler et al. (16), serum progesterone assessment in women who experienced regular menses after metformin showed that most cycles became ovulatory.

At baseline, women randomized to metformin and those randomized to placebo were not entirely similar. In particular, body mass index was significantly lower and androgens tended to be higher in subjects given the active drug. These counfounding factors were taken into account in the analysis. Noticeably, the open long-term study shows that responders had higher body mass index and lower serum androstenedione than nonresponders. Thus, baseline differences between groups in the double-blind study could actually have reduced evidence of benefits of metformin vs placebo.

Low calorie diet should be the first choice of treatment for obese PCOS subjects (24, 25, 26). Nevertheless, insulin sensitizing agents may offer greater scope for practical application in these women, whose compliance with diet is often poor. Hyperinsulinemia and insulin resistance are also characteristic features of many lean PCOS patients (2), in whom weight loss would be undesirable. In these subjects as well insulin sensitizers may be a feasible choice (12), although our data indicate that the expected response rate is lower in lean patients.

In the present study, almost half of the women given the active drug had no improvement in their menstrual history. The reasons for the striking differences in clinical response to metformin among the individual PCOS subjects are not easily explained. We hypothesize that this phenomenon might reflect the heterogeneity in the pathogenesis of the syndrome. While insulin resistance is a common but not universal feature in women with PCOS, it likely plays a pathogenetic role only in a subset of women (2). Only these subjects would benefit substantially from improved insulin sensitivity. This hypothesis could also account for the discordant results among previous studies that considered metformin for the treatment of women with PCOS.

It should be borne in mind that the mechanisms of insulin resistance in PCOS and the ways by which both metformin and troglitazone may improve insulin action in these women are still largely unknown. These drugs seem to act at different levels, at least as far as glucose metabolism is concerned (31). Thus, intersubject differences in efficacy might be observed according to the specific defect responsible for the impairment in insulin action and the specific effects of each drug. On the other hand, the universal clinical efficacy of reductions in insulin levels (whether obtained by metformin, troglitazone, diet, diazoxide, somatostatin, or the putative mediator of insulin action D-chiro-inositol) (6, 7, 10, 11, 12, 14, 15, 16, 24, 25, 26, 32) in PCOS suggests that reproductive abnormalities in these patients may be directly related to hyperinsulinemia and not to any specific mechanism of insulin resistance.

An original aspect of our study was analysis of baseline predictors of clinical response to metformin. Actually, responders differed from nonresponders in several characteristics. Logistic regression analysis showed that higher plasma insulin, lower serum androstenedione, and less severe menstrual abnormalities were independent predictors of clinical efficacy of metformin. These data further strengthen the hypothesis that insulin sensitizers may be effective only in the insulin-resistant subset of this heterogeneous syndrome. On the other hand, the unfavorable predictive effect of higher baseline serum androstenedione levels may indicate poor efficacy of metformin in women with either a different pathogenesis of the syndrome or more advanced disease.

An intriguing finding of this study was the significant post-treatment reduction of serum LH, in responders only. Reductions in serum LH after treatment with metformin were previously found in the other studies, which likewise reported improvements in biochemical and/or clinical features of PCOS (10, 11, 12, 13). Furthermore, Dunaif et al. (14), but not Ehrmann et al. (15), reported similar concurrent changes after troglitazone. Interestingly, insulin stimulates gonadotropin release in vitro, at least in the rat (33). As a whole, these data suggest that changes in insulin levels might also contribute to changes in ovarian androgen secretion through effects at the pituitary level. However, current knowledge of these aspects is too limited to encourage the formulation of precise hypotheses.

In our study, while reproductive abnormalities strikingly improved after treatment, hirsutism was unaffected both in the 6-month controlled trial and in the long-term follow-up, despite substantial reductions in serum testosterone. These findings resemble those of other authors in hirsute subjects with congenital adrenal hyperplasia, in whom adrenal androgen suppression by glucocorticoid therapy has limited efficacy on established hair excess (34). In these women, a course of antiandrogen drugs is needed to improve their hirsutism, whereas corticosteroid therapy is sufficient for clinical maintenance. Whether this would also be true for hirsute PCOS subjects given metformin should be investigated by further research. Further studies should also establish whether metformin and troglitazone might have synergic effects in improving reproductive and endocrine abnormalities of women with PCOS, as recently shown for glucose metabolism abnormalities in type 2 diabetic subjects (31).

In conclusion, treatment with the insulin sensitizing agent metformin is effective in many women with PCOS, independently of changes in body weight, in attenuating insulin resistance and hyperandrogenemia and in reversing menstrual abnormalities and chronic anovulation. Insulin sensitizing agents may prove an efficacious therapeutic tool in a large subset of subjects with this common disease.

	Acknowledgments

 
We wish to thank Ms. Marilena Longo and Mr. Luciano Meneghelli for their excellent secretarial support and Ms. Paola Branzi, Ms. Alessandra Rossi, Ms. M. Grazia Zanotti, Ms. Federica Moschetta, and Ms. Monica Zardini for their helpful technical assistance.

	Footnotes

 
¹ This work was presented in part at the 79th Annual Meeting of The Endocrine Society, Minneapolis, Minnesota, June 11–14, 1997. This work was supported by grants from the Italian Ministry of Higher Education and Scientific Research, and the Regione del Veneto (DGRV 964, n.652 and n.693).

Received July 29, 1999.

Revised September 27, 1999.

Accepted October 4, 1999.

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