Individuals Diagnosed with Binge-Eating Disorder Have DNA Hypomethylated Sites in Genes of the Metabolic System: A Pilot Study

Author:

Rodríguez-López Mariana Lizbeth,Martínez-Magaña José JaimeORCID,Ruiz-Ramos David,García Ana Rosa,Gonzalez Laura,Tovilla-Zarate Carlos AlfonsoORCID,Sarmiento Emmanuel,Juárez-Rojop Isela Esther,Nicolini HumbertoORCID,Gonzalez-Castro Thelma BeatrizORCID,Genis-Mendoza Alma Delia

Abstract

Binge-eating disorder, recently accepted as a diagnostic category, is differentiated from bulimia nervosa in that the former shows the presence of binge-eating episodes and the absence of compensatory behavior. Epigenetics is a conjunct of mechanisms (like DNA methylation) that regulate gene expression, which are dependent on environmental changes. Analysis of DNA methylation in eating disorders shows that it is reduced. The present study aimed to analyze the genome-wide DNA methylation differences between individuals diagnosed with BED and BN. A total of 46 individuals were analyzed using the Infinium Methylation EPIC array. We found 11 differentially methylated sites between BED- and BN-diagnosed individuals, with genome-wide significance. Most of the associations were found in genes related to metabolic processes (ST3GAL4, PRKAG2, and FRK), which are hypomethylated genes in BED. Cg04781532, located in the body of the PRKAG2 gene (protein kinase AMP-activated non-catalytic subunit gamma 2), was hypomethylated in individuals with BED. Agonists of PRKAG2, which is the subunit of AMPK (AMP-activated protein kinase), are proposed to treat obesity, BED, and BN. The present study contributes important insights into the effect that BED could have on PRKAG2 activation.

Funder

Fundación Gonzalo Río Arronte

Instituto Nacional de Medicina Genómica

Publisher

MDPI AG

Subject

Food Science,Nutrition and Dietetics

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