Suppression of Canonical TGF-β Signaling Enables GATA4 to Interact with H3K27me3 Demethylase JMJD3 to Promote Cardiomyogenesis

Overview

Journal J Mol Cell Cardiol

Specialty Cardiology & Vascular Diseases

Date 2020 Dec 28

PMID 33359755

Citations 16

Authors

Andrew S Riching

Etienne Danis

Yuanbiao Zhao

Yingqiong Cao

Congwu Chi

Rushita A Bagchi

Brianna J Klein

Hongyan Xu

Tatiana G Kutateladze

Timothy A McKinsey

Peter M Buttrick

Kunhua Song

Affiliations

Soon will be listed here.

Abstract

Direct reprogramming of fibroblasts into cardiomyocytes (CMs) represents a promising strategy to regenerate CMs lost after ischemic heart injury. Overexpression of GATA4, HAND2, MEF2C, TBX5, miR-1, and miR-133 (GHMT2m) along with transforming growth factor beta (TGF-β) inhibition efficiently promote reprogramming. However, the mechanisms by which TGF-β blockade promotes cardiac reprogramming remain unknown. Here, we identify interactions between the histone H3 lysine 27 trimethylation (H3K27me3) demethylase JMJD3, the SWI/SNF remodeling complex subunit BRG1, and cardiac transcription factors. Furthermore, canonical TGF-β signaling regulates the interaction between GATA4 and JMJD3. TGF-β activation impairs the ability of GATA4 to bind target genes and prevents demethylation of H3K27 at cardiac gene promoters during cardiac reprogramming. Finally, a mutation in GATA4 (V267M) that is associated with congenital heart disease exhibits reduced binding to JMJD3 and impairs cardiomyogenesis. Thus, we have identified an epigenetic mechanism wherein canonical TGF-β pathway activation impairs cardiac gene programming, in part by interfering with GATA4-JMJD3 interactions.

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