Endothelial Brg1 fine-tunes Notch signaling during zebrafish heart regeneration

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作者
Chenglu Xiao
Junjie Hou
Fang Wang
Yabing Song
Jiyuan Zheng
Lingfei Luo
Jianbin Wang
Wanqiu Ding
Xiaojun Zhu
Jing-Wei Xiong
机构
[1] Peking University,Beijing Key Laboratory of Cardiometabolic Molecular Medicine, Institute of Molecular Medicine, College of Future Technology, and State Key Laboratory of Natural and Biomimetic Drugs
[2] China Agricultural University,National Key Laboratory of Veterinary Public Health Security, College of Veterinary Medicine
[3] Zhejiang University of Technology,College of Pharmaceutical Science
[4] Tsinghua University,School of Life Sciences
[5] Southwest University,Institute of Developmental Biology and Regenerative Medicine
[6] Beibei,undefined
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Myocardial Brg1 is essential for heart regeneration in zebrafish, but it remains unknown whether and how endothelial Brg1 plays a role in heart regeneration. Here, we found that both brg1 mRNA and protein were induced in cardiac endothelial cells after ventricular resection and endothelium-specific overexpression of dominant-negative Xenopus Brg1 (dn-xbrg1) inhibited myocardial proliferation and heart regeneration and increased cardiac fibrosis. RNA-seq and ChIP-seq analysis revealed that endothelium-specific overexpression of dn-xbrg1 changed the levels of H3K4me3 modifications in the promoter regions of the zebrafish genome and induced abnormal activation of Notch family genes upon injury. Mechanistically, Brg1 interacted with lysine demethylase 7aa (Kdm7aa) to fine-tune the level of H3K4me3 within the promoter regions of Notch family genes and thus regulated notch gene transcription. Together, this work demonstrates that the Brg1-Kdm7aa-Notch axis in cardiac endothelial cells, including the endocardium, regulates myocardial proliferation and regeneration via modulating the H3K4me3 of the notch promoters in zebrafish.
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