Ebf Factors and MyoD Cooperate to Regulate Muscle Relaxation Via Atp2a1

Overview

Journal Nat Commun

Specialty Biology

Date 2014 May 3

PMID 24786561

Citations 28

Authors

Saihong Jin

Jeehee Kim

Torsten Willert

Tanja Klein-Rodewald

Mario Garcia-Dominguez

Matias Mosqueira

Rainer Fink

Irene Esposito

Lorenz C Hofbauer

Patrick Charnay

Matthias Kieslinger

Affiliations

Soon will be listed here.

Abstract

Myogenic regulatory factors such as MyoD and Myf5 lie at the core of vertebrate muscle differentiation. However, E-boxes, the cognate binding sites for these transcription factors, are not restricted to the promoters/enhancers of muscle cell-specific genes. Thus, the specificity in myogenic transcription is poorly defined. Here we describe the transcription factor Ebf3 as a new determinant of muscle cell-specific transcription. In the absence of Ebf3 the lung does not unfold at birth, resulting in respiratory failure and perinatal death. This is due to a hypercontractile diaphragm with impaired Ca(2+) efflux-related muscle functions. Expression of the Ca(2+) pump Serca1 (Atp2a1) is downregulated in the absence of Ebf3, and its transgenic expression rescues this phenotype. Ebf3 binds directly to the promoter of Atp2a1 and synergises with MyoD in the induction of Atp2a1. In skeletal muscle, the homologous family member Ebf1 is strongly expressed and together with MyoD induces Atp2a1. Thus, Ebf3 is a new regulator of terminal muscle differentiation in the diaphragm, and Ebf factors cooperate with MyoD in the induction of muscle-specific genes.

Citing Articles

Unveiling the prenatal features of HADDS: A case report and literature review.

Hu L, Li D, Zhen L, Wang Y Heliyon. 2025; 11(2):e41591.

PMID: 39911434 PMC: 11795036. DOI: 10.1016/j.heliyon.2024.e41591.

STAIG: Spatial transcriptomics analysis via image-aided graph contrastive learning for domain exploration and alignment-free integration.

Yang Y, Cui Y, Zeng X, Zhang Y, Loza M, Park S Nat Commun. 2025; 16(1):1067.

PMID: 39870633 PMC: 11772580. DOI: 10.1038/s41467-025-56276-0.

Gene expression patterns of the developing human face at single cell resolution reveal cell type contributions to normal facial variation and disease risk.

Khouri-Farah N, Winchester E, Schilder B, Robinson K, Curtis S, Skene N bioRxiv. 2025; .

PMID: 39868299 PMC: 11761091. DOI: 10.1101/2025.01.18.633396.

Multi-trait Genome-Wide Analysis Identified 20 Novel Loci for Sarcopenia-Related Traits in UK Biobank.

Ran S, Lin X, Wang S, Li Z, Liu B Calcif Tissue Int. 2025; 116(1):10.

PMID: 39751833 DOI: 10.1007/s00223-024-01312-2.

Investigating the Causal Effects of Exercise-Induced Genes on Sarcopenia.

Wang L, Zhang S Int J Mol Sci. 2024; 25(19).

PMID: 39409102 PMC: 11476887. DOI: 10.3390/ijms251910773.