MEF2C repressor variant deregulation leads to cell cycle re-entry and development of heart failure

Ana Helena M Pereira; Alisson C Cardoso; Silvio R Consonni; Renata R Oliveira; Angela Saito; Maria Luisa B Vaggione; Jose R Matos-Souza; Marcelo F Carazzolle; Anderson Gonçalves; Juliano L Fernandes; Gustavo C A Ribeiro; Mauricio M Lopes; Jeffery D Molkentin; Kleber G Franchini

doi:10.1016/j.ebiom.2019.11.032

MEF2C repressor variant deregulation leads to cell cycle re-entry and development of heart failure

EBioMedicine. 2020 Jan:51:102571. doi: 10.1016/j.ebiom.2019.11.032. Epub 2020 Jan 3.

Authors

Affiliations

¹ Brazilian Biosciences National Laboratory (LNBio), Brazilian Center for Research in Energy and Materials (CNPEM), 13083-970 Campinas, Sao Paulo, Brazil.
² Department of Biochemistry and Tissue Biology, University of Campinas, Campinas, Brazil.
³ Department of Internal Medicine, University of Campinas, Campinas, Brazil.
⁴ Genomics and Expression Laboratory, University of Campinas, Campinas, Brazil.
⁵ Jose Michel Kalaf Research Institute, Campinas, Brazil.
⁶ Cardiovascular Surgery, Pontifical Catholic University, Campinas, Brazil.
⁷ Cardiology, Pontifical Catholic University, Campinas, Brazil.
⁸ Cincinnati Children's Hospital Medical Center, University of Cincinnati, Cincinnati, USA.
⁹ Brazilian Biosciences National Laboratory (LNBio), Brazilian Center for Research in Energy and Materials (CNPEM), 13083-970 Campinas, Sao Paulo, Brazil; Department of Internal Medicine, University of Campinas, Campinas, Brazil. Electronic address: kleber.franchini@lnbio.cnpem.br.

Abstract

Background: A pathophysiological link exists between dysregulation of MEF2C transcription factors and heart failure (HF), but the underlying mechanisms remain elusive. Alternative splicing of MEF2C exons α, β and γ provides transcript diversity with gene activation or repression functionalities.

Methods: Neonatal and adult rat ventricular myocytes were used to overexpress MEF2C splicing variants γ+ (repressor) or γ-, or the inactive MEF2Cγ+23/24 (K23T/R24L). Phenotypic alterations in cardiomyocytes were determined by confocal and electron microscopy, flow cytometry and DNA microarray. We used transgenic mice with cardiac-specific overexpression of MEF2Cγ+ or MEF2Cγ- to explore the impact of MEF2C variants in cardiac phenotype. Samples of non-infarcted areas of the left ventricle from patients and mouse model of myocardial infarction were used to detect the expression of MEF2Cγ+ in failing hearts.

Findings: We demonstrate a previously unrealized upregulation of the transrepressor MEF2Cγ+ isoform in human and mouse failing hearts. We show that adenovirus-mediated overexpression of MEF2Cγ+ downregulates multiple MEF2-target genes, and drives incomplete cell-cycle reentry, partial dedifferentiation and apoptosis in the neonatal and adult rat. None of these changes was observed in cardiomyocytes overexpressing MEF2Cγ-. Transgenic mice overexpressing MEF2Cγ+, but not the MEF2Cγ-, developed dilated cardiomyopathy, correlated to cell-cycle reentry and apoptosis of cardiomyocytes.

Interpretation: Our results provide a mechanistic link between MEF2Cγ+ and deleterious abnormalities in cardiomyocytes, supporting the notion that splicing dysregulation in MEF2C towards the selection of the MEF2Cγ+ variant contributes to the pathogenesis of HF by promoting cardiomyocyte dropout.

Funding: São Paulo Research Foundation (FAPESP); Brazilian National Research Council (CNPq).

Keywords: Cardiomyocyte; Cell cycle re-entry; Dedifferentiation; Heart failure; MEF2; Sarcomere disassembly; Splicing.

MeSH terms

Alternative Splicing
Animals
Apoptosis / genetics
Cell Cycle / genetics*
Disease Models, Animal
Gene Expression Regulation*
Genetic Association Studies
Genetic Predisposition to Disease*
Genetic Variation*
Heart Failure / diagnosis
Heart Failure / etiology*
Heart Failure / metabolism*
Heart Failure / therapy
Humans
MEF2 Transcription Factors / genetics
Mice
Mice, Transgenic
Myocytes, Cardiac / metabolism
Myocytes, Cardiac / ultrastructure
Rats

Substances

MEF2 Transcription Factors
MEF2C protein, human