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Circulating follistatin concentrations in adolescent PCOS: Divergent effects of randomized treatments

Purpose: Follistatin is a glycoprotein that represses members of the transforming growth factor-β superfamily including activin. Higher follistatin levels have been associated with an increased risk for type 2 diabetes and with polycystic ovary syndrome (PCOS). In non-obese adolescent girls with PCOS, insulin sensitization results in a healthier endocrine-metabolic outcome than oral contraception (OC); we assessed whether those differences are underscored by changes in serum follistatin concentrations.

Methods: Circulating follistatin, endocrine-metabolic markers and hepato-visceral fat were measured longitudinally in 72 girls with PCOS [age, 16 years; body mass index (BMI), 23 Kg/m2] randomized to receive PioFluMet [pioglitazone (7.5 mg/d), metformin (850 mg/d) and flutamide (62.5 mg/d), n=17]; EE-CA [an OC containing 35 µg ethinylestradiol (EE) and 2 mg cyproterone acetate (CA), n=17]; SPIOMET [Spironolactone (50 mg/d), pioglitazone (7.5 mg/d) and metformin (850 mg/d), n=18], or EE-LNG [an OC containing 20 µg EE and 100 mg levonorgestrel (LNG), n=20]. Twenty-eight age- and BMI-matched healthy girls served as controls.

Results: Pre-treatment follistatin levels were similar in PCOS and controls. OCs raised serum follistatin after 6 months (6.8-fold vs 2.5-fold for EE-CA and EE-LNG, respectively). Neither SPIOMET nor PioFluMet changed follistatin levels. Follistatin correlated negatively with high-molecular weight adiponectin and positively with mean serum insulin concentrations during an oral glucose tolerance test at baseline, and with liver fat after 6 months.

Conclusion: In girls with PCOS, follistatin levels rise significantly after 6 months on OCs and this increase associates to a worsening of markers of insulin resistance and to changes in liver fat.

Comments:

The study aimed to investigate whether changes in serum follistatin concentrations are associated with differences in endocrine-metabolic outcomes in non-obese adolescent girls with polycystic ovary syndrome (PCOS) undergoing different treatments. The study included 72 girls with PCOS and 28 age- and BMI-matched healthy controls. The PCOS group was randomized to receive different treatments: PioFluMet (pioglitazone, metformin, and flutamide), EE-CA (an oral contraceptive containing ethinylestradiol and cyproterone acetate), SPIOMET (spironolactone, pioglitazone, and metformin), or EE-LNG (an oral contraceptive containing ethinylestradiol and levonorgestrel).

The researchers found that pretreatment follistatin levels were similar in the PCOS group and the healthy controls. After 6 months, the use of oral contraceptives (EE-CA and EE-LNG) resulted in a significant increase in follistatin levels (6.8-fold and 2.5-fold, respectively), while neither SPIOMET nor PioFluMet changed follistatin levels. Follistatin levels were negatively correlated with high-molecular-weight adiponectin and positively correlated with mean serum insulin concentrations during an oral glucose tolerance test at baseline, as well as with liver fat after 6 months.

The study suggests that higher follistatin levels are associated with an increased risk for insulin resistance and changes in liver fat in non-obese adolescent girls with PCOS, particularly when using oral contraceptives. These findings highlight the importance of monitoring follistatin levels when treating PCOS and considering alternative treatments to oral contraceptives.

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PPAR