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Metabolic inflexibility in women with PCOS is similar to women with type 2 diabetes
Authors:Nicholas T. Broskey  Charmaine S. Tam  Elizabeth F. Sutton  Abby D. Altazan  Jeffrey H. Burton  Eric Ravussin  Leanne M Redman
Affiliation:1.Pennington Biomedical Research Center,Baton Rouge,USA;2.School of Life and Environmental Sciences and Centre of Translational Data Science,University of Sydney,Sydney,Australia
Abstract:

Background

An ability to switch between primarily oxidizing fat in the fasted state to carbohydrate in the fed state, termed metabolic flexibility, is associated with insulin sensitivity. Metabolic flexibility has been explored previously in women with polycystic ovary syndrome (PCOS), yet the independent or synergistic contributions of androgen excess and/or insulin resistance is not yet known. Therefore, the purpose of this article was to characterize metabolic flexibility in women with PCOS compared to women of normal BMI, obesity, or type 2 diabetes (T2DM).

Methods

Eighty-six weight-stable women; thirty with either PCOS (n?=?30), or fifty-six with obesity (n?=?12), T2DM (n?=?27), or normal BMI (n?=?17) underwent a hyperinsulinemic euglycemic clamp and indirect calorimetry to measure insulin sensitivity and substrate oxidation via indirect calorimetry, respectively.

Results

All analyses were adjusted for differences in age, ethnicity, and BMI between groups. Women with PCOS were less metabolically flexible compared to healthy women with obesity (p?p?p?=?0.99). When dividing women with PCOS above and below the mean cutoff for insulin resistance, the insulin resistant women with PCOS had lower rates of non-oxidative glucose metabolism (p?=?0.0001), higher levels of percent free testosterone (p?=?0.04), a higher free androgen index (p?=?0.006), more visceral adipose tissue (p?=?0.02), and were less metabolically flexible (p?=?0.007).

Conclusions

Women with T2DM were as metabolically inflexible as women with PCOS. When stratifying women with PCOS into those who are metabolically flexible and inflexible, the women who are inflexible display greater amounts of visceral fat and androgen excess. The inability to alter substrate use given the physiological stimulus may lead to subsequent increases in adiposity in women with PCOS thereby further worsening the insulin resistance.

Trial registration number

Clinical Trials.gov, NCT01482286. Registered 30 November 2011.
Keywords:
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