PPARGC1A promoter DNA-methylation level and glucose metabolism in Ecuadorian women with Turner syndrome

Author:

Álvarez-Nava Francisco1ORCID,Salinas Marco2,Bastidas Daniela1,Vicuña Yosselin2,Racines-Orbe Marcia2

Affiliation:

1. Biological Sciences School, Faculty of Biological Sciences , Central University of Ecuador , Quito Ecuador

2. Institute of Biomedicine Research , Central University of Ecuador , Quito , Ecuador

Abstract

Abstract Objectives Reduced gene expression of PPARGC1A in subjects with insulin resistance (IR) has been reported. Insulin resistance occurs early on the course of Turner syndrome (TS). The main objective of this study was to evaluate the relationship between PPARGC1A promoter DNA methylation status in lymphocytes and insulin sensitivity and secretion in Ecuadorian females with TS. Methods We examined a cohort of 34 Ecuadorian patients with TS along with a sex-, age- and BMI-matched reference group. All subjects received a standard 75 g oral glucose tolerance test. Insulin resistance and secretion indices were calculated. The PPARGC1A methylated DNA/unmethylated DNA ratio and mitochondrial content (mtDNA/nDNA ratio) were further determined. Results Notably, the PPARGC1A DNA methylation level was significantly higher in TS subjects than the reference group and correlated with IR indices. Conversely, mitochondrial content was significantly lower in the study group than healthy controls and negatively correlated with the PPARGC1A methylated DNA/unmethylated DNA ratio in TS individuals. PPARGC1A promoter DNA methylation status contributed to 20% of the total variability in Homeostasis Model Assessment for Insulin Resistance (HOMA-IR) independently of BMI or age in TS subjects. Conclusions Our collective findings suggest that expression of PPARGC1A and lower mitochondrial number affect the metabolic phenotype in TS subjects.

Funder

Academie de Recherche et D’Enseignement Superieur of Belgique

Publisher

Walter de Gruyter GmbH

Subject

Endocrinology,Molecular Biology,General Medicine,Endocrinology, Diabetes and Metabolism

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