DNA Methylation Alters Transcriptional Rates of Differentially Expressed Genes and Contributes to Pathophysiology in Mice Fed a High Fat Diet

Overview

Journal Mol Metab

Specialty Cell Biology

Date 2017 Apr 6

PMID 28377872

Citations 21

Authors

Pili Zhang

Tianjiao Chu

N Dedousis

Benjamin S Mantell

Ian Sipula

Lucy Li

Kimberly D Bunce

Patricia A Shaw

Liora S Katz

Jun Zhu

Carmen Argmann

Robert M ODoherty

David G Peters

Donald K Scott

Affiliations

Soon will be listed here.

Abstract

Objective: Overnutrition can alter gene expression patterns through epigenetic mechanisms that may persist through generations. However, it is less clear if overnutrition, for example a high fat diet, modifies epigenetic control of gene expression in adults, or by what molecular mechanisms, or if such mechanisms contribute to the pathology of the metabolic syndrome. Here we test the hypothesis that a high fat diet alters hepatic DNA methylation, transcription and gene expression patterns, and explore the contribution of such changes to the pathophysiology of obesity.

Methods: RNA-seq and targeted high-throughput bisulfite DNA sequencing were used to undertake a systematic analysis of the hepatic response to a high fat diet. RT-PCR, chromatin immunoprecipitation and knockdown of an identified driver gene, , were used to validate the results.

Results: A high fat diet resulted in the hypermethylation and decreased transcription and expression of and several other genes. A subnetwork of genes associated with was identified from an existing Bayesian gene network that contained numerous hepatic regulatory genes involved in lipid and body weight homeostasis. Hepatic-specific depletion of in mice decreased expression of the genes in the subnetwork, and led to increased oil droplet size in standard chow-fed mice, an early indicator of steatosis, validating the contribution of this gene to the phenotype.

Conclusions: We conclude that a high fat diet alters the epigenetics and transcriptional activity of key hepatic genes controlling lipid homeostasis, contributing to the pathophysiology of obesity.

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