Hierarchical and stage-specific regulation of murine cardiomyocyte maturation by serum response factor

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作者
Yuxuan Guo
Blake D. Jardin
Pingzhu Zhou
Isha Sethi
Brynn N. Akerberg
Christopher N Toepfer
Yulan Ai
Yifei Li
Qing Ma
Silvia Guatimosim
Yongwu Hu
Grigor Varuzhanyan
Nathan J. VanDusen
Donghui Zhang
David C. Chan
Guo-Cheng Yuan
Christine E. Seidman
Jonathan G. Seidman
William T. Pu
机构
[1] Boston Children’s Hospital,Department of Cardiology
[2] Boston University,Department of Biology
[3] Dana-Farber Cancer Institute,Department of Biostatistics and Computational Biology
[4] Harvard Medical School,Department of Genetics
[5] University of Oxford,Radcliffe Department of Medicine and Wellcome Trust Centre for Human Genetics
[6] Sichuan University,Key Laboratory of Birth Defects and Related Diseases of Women and Children of MOE, Department of Pediatrics, West China Second University Hospital
[7] Universidade Federal de Minas Gerais,Department of Physiology and Biophysics, Institute of Biological Sciences
[8] California Institute of Technology,Division of Biology and Biological Engineering
[9] Brigham and Women’s Hospital,Division of Cardiovascular Medicine
[10] Howard Hughes Medical Institute,Hubei Collaborative Innovation Center for Green Transformation of Bio
[11] Harvard Stem Cell Institute,resources, Hubei Key Laboratory of Industrial Biotechnology, College of Life Sciences
[12] Wenzhou Medical University,undefined
[13] School of Life Sciences,undefined
[14] Hubei University,undefined
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摘要
After birth, cardiomyocytes (CM) acquire numerous adaptations in order to efficiently pump blood throughout an animal’s lifespan. How this maturation process is regulated and coordinated is poorly understood. Here, we perform a CRISPR/Cas9 screen in mice and identify serum response factor (SRF) as a key regulator of CM maturation. Mosaic SRF depletion in neonatal CMs disrupts many aspects of their maturation, including sarcomere expansion, mitochondrial biogenesis, transverse-tubule formation, and cellular hypertrophy. Maintenance of maturity in adult CMs is less dependent on SRF. This stage-specific activity is associated with developmentally regulated SRF chromatin occupancy and transcriptional regulation. SRF directly activates genes that regulate sarcomere assembly and mitochondrial dynamics. Perturbation of sarcomere assembly but not mitochondrial dynamics recapitulates SRF knockout phenotypes. SRF overexpression also perturbs CM maturation. Together, these data indicate that carefully balanced SRF activity is essential to promote CM maturation through a hierarchy of cellular processes orchestrated by sarcomere assembly.
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