Contraction-induced endocardial id2b plays a dual role in regulating myocardial contractility and valve formation-Reference-Cited by-同舟云学术

Contraction-induced endocardial id2b plays a dual role in regulating myocardial contractility and valve formation

Published:2024-09-11 Issue: Volume: Page:
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Author:

Chen Shuo¹²³^ORCID,Yin Jie¹²³,Liang Jinxiu¹²³,Zhang Weijia¹²³,Jiang Peijun¹²³,Wang Wenyuan⁴⁵,Chen Xiaoying⁶⁷^ORCID,Zhou Yuanhong⁸,Xia Peng⁸,Yang Fan⁶⁷^ORCID,Gu Ying¹²³,Zhang Ruilin⁴⁵^ORCID,Han Peidong¹²³^ORCID

Affiliation:

1. Center for Genetic Medicine, The Fourth Affiliated Hospital, Zhejiang University School of Medicine

2. Institute of Genetics, Zhejiang University International School of Medicine

3. Division of Medical Genetics and Genomics, The Children’s Hospital, Zhejiang University School of Medicine, National Clinical Research Center for Child Health

4. TaiKang Medical School (School of Basic Medical Sciences), Wuhan University

5. Hubei Provincial Key Laboratory of Developmentally Originated Disease

6. Department of Biophysics, and Kidney Disease Center of the First Affiliated Hospital, Zhejiang University School of Medicine

7. Liangzhu Laboratory, Zhejiang University Medical Center

8. Zhejiang Provincial Key Laboratory for Cancer Molecular Cell Biology, Life Sciences Institute, Zhejiang University

Abstract

Biomechanical cues play an essential role in sculpting organ formation. Comprehending how cardiac cells perceive and respond to biomechanical forces is a biological process with significant medical implications that remains poorly understood. Here we show that biomechanical forces activate endocardial id2b (inhibitor of DNA binding 2b) expression, thereby promoting cardiac contractility and valve formation. Taking advantage of the unique strengths of zebrafish, particularly the viability of embryos lacking heartbeats, we systematically compared the transcriptomes of hearts with impaired contractility to those of control hearts. This comparison identified id2b as a gene sensitive to blood flow. By generating a knockin reporter line, our results unveiled the presence of id2b in the endocardium, and its expression is sensitive to both pharmacological and genetic perturbations of contraction. Furthermore, id2b loss-of-function resulted in progressive heart malformation and early lethality. Combining RNA-seq analysis, electrophysiology, calcium imaging, and echocardiography, we discovered profound impairment in atrioventricular (AV) valve formation and defective excitation-contraction coupling in id2b mutants. Mechanistically, deletion of id2b reduced AV endocardial cell proliferation and led to a progressive increase in retrograde blood flow. In the myocardium, id2b directly interacted with the bHLH component tcf3b (transcription factor 3b) to restrict its activity. Inactivating id2b unleashed its inhibition on tcf3b , resulted in enhanced repressor activity of tcf3b , which subsequently suppressed the expression of nrg1 (neuregulin 1), an essential mitogen for heart development. Overall, our findings identify id2b as an endocardial cell-specific, biomechanical signaling-sensitive gene, which mediates intercellular communications between endocardium and myocardium to sculpt heart morphogenesis and function.

Publisher

eLife Sciences Publications, Ltd

Link

https://elifesciences.org/reviewed-preprints/101151v1/pdf

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