Linc-YY1 promotes myogenic differentiation and muscle regeneration through an interaction with the transcription factor YY1

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作者
Liang Zhou
Kun Sun
Yu Zhao
Suyang Zhang
Xuecong Wang
Yuying Li
Leina Lu
Xiaona Chen
Fengyuan Chen
Xichen Bao
Xihua Zhu
Lijun Wang
Ling-Yin Tang
Miguel A. Esteban
Chi-Chiu Wang
Ralf Jauch
Hao Sun
Huating Wang
机构
[1] Li Ka Shing Institute of Health Sciences,Department of Chemical Pathology
[2] The Chinese University of Hong Kong,Department of Obstetrics and Gynaecology
[3] Prince of Wales Hospital,Department of Orthopedics and Traumatology
[4] Li Ka Shing Institute of Health Sciences,undefined
[5] Chinese University of Hong Kong,undefined
[6] Prince of Wales Hospital,undefined
[7] The Chinese University of Hong Kong,undefined
[8] Genome Regulation Laboratory,undefined
[9] Drug Discovery Pipeline,undefined
[10] Key Laboratory of Regenerative Biology,undefined
[11] Guangdong Provincial Key Laboratory of Stem Cell and Regenerative Medicine,undefined
[12] South China Institute for Stem Cell Biology and Regenerative Medicine,undefined
[13] Guangzhou Institutes of Biomedicine and Health,undefined
[14] Chinese Academy of Sciences,undefined
[15] Laboratory of Chromatin and Human Disease,undefined
[16] Key Laboratory of Regenerative Biology,undefined
[17] South China Institute for Stem Cell Biology and Regenerative Medicine,undefined
[18] Guangzhou Institutes of Biomedicine and Health,undefined
[19] Chinese Academy of Sciences,undefined
[20] Prince of Wales Hospital,undefined
[21] Li Ka Shing Institute of Health Sciences,undefined
[22] The Chinese University of Hong Kong,undefined
[23] Present address: Department of Radiation Medicine,undefined
[24] Guangdong Provincial Key Laboratory of Tropical Disease Research,undefined
[25] School of Public Health and Tropical Medicine,undefined
[26] Southern Medical University,undefined
[27] Guangzhou,undefined
[28] Guangdong 510515,undefined
[29] PR China.,undefined
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摘要
Little is known how lincRNAs are involved in skeletal myogenesis. Here we describe the discovery of Linc-YY1 from the promoter of the transcription factor (TF) Yin Yang 1 (YY1) gene. We demonstrate that Linc-YY1 is dynamically regulated during myogenesis in vitro and in vivo. Gain or loss of function of Linc-YY1 in C2C12 myoblasts or muscle satellite cells alters myogenic differentiation and in injured muscles has an impact on the course of regeneration. Linc-YY1 interacts with YY1 through its middle domain, to evict YY1/Polycomb repressive complex (PRC2) from target promoters, thus activating the gene expression in trans. In addition, Linc-YY1 also regulates PRC2-independent function of YY1. Finally, we identify a human Linc-YY1 orthologue with conserved function and show that many human and mouse TF genes are associated with lincRNAs that may modulate their activity. Altogether, we show that Linc-YY1 regulates skeletal myogenesis and uncover a previously unappreciated mechanism of gene regulation by lincRNA.
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