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题名

Translational control by DHX36 binding to 5′UTR G-quadruplex is essential for muscle stem-cell regenerative functions

作者
通讯作者Sun,Hao; Muñoz-Cánoves,Pura; Wang,Huating
共同第一作者Yuan,Jie
发表日期
2021-12-01
DOI
发表期刊
ISSN
2041-1723
EISSN
2041-1723
卷号12期号:1
摘要

Skeletal muscle has a remarkable ability to regenerate owing to its resident stem cells (also called satellite cells, SCs). SCs are normally quiescent; when stimulated by damage, they activate and expand to form new fibers. The mechanisms underlying SC proliferative progression remain poorly understood. Here we show that DHX36, a helicase that unwinds RNA G-quadruplex (rG4) structures, is essential for muscle regeneration by regulating SC expansion. DHX36 (initially named RHAU) is barely expressed at quiescence but is highly induced during SC activation and proliferation. Inducible deletion of Dhx36 in adult SCs causes defective proliferation and muscle regeneration after damage. System-wide mapping in proliferating SCs reveals DHX36 binding predominantly to rG4 structures at various regions of mRNAs, while integrated polysome profiling shows that DHX36 promotes mRNA translation via 5′-untranslated region (UTR) rG4 binding. Furthermore, we demonstrate that DHX36 specifically regulates the translation of Gnai2 mRNA by unwinding its 5′ UTR rG4 structures and identify GNAI2 as a downstream effector of DHX36 for SC expansion. Altogether, our findings uncover DHX36 as an indispensable post-transcriptional regulator of SC function and muscle regeneration acting through binding and unwinding rG4 structures at 5′ UTR of target mRNAs.

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英语
重要成果
NI期刊
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其他
资助项目
General Research Funds (GRF) from the Research Grants Council (RGC) of the Hong Kong Special Administrative Region[14115319,14100018,14100620,14106117,14106521,14120420,14116918,14120619] ; Guangdong Natural Science Foundation from Guangdong Basic and Applied Basic Research Foundation[2019A1515010670] ; National Natural Science Foundation of China (NSFC)[31871304] ; Area of Excellence Scheme (AoE) from RGC[AoE/M-402/20] ; CUHK Direct Grant for Research[4054482] ; NSFC/RGC Joint Research Scheme[N_CUHK 413/18] ; Spanish Ministry of Science, Innovation and Universities, Spain[
WOS研究方向
Science & Technology - Other Topics
WOS类目
Multidisciplinary Sciences
WOS记录号
WOS:000686770100012
出版者
Scopus记录号
2-s2.0-85113209842
来源库
Scopus
引用统计
被引频次[WOS]:33
成果类型期刊论文
条目标识符http://sustech.caswiz.com/handle/2SGJ60CL/244977
专题生命科学学院_生物系
生命科学学院
作者单位
1.Department of Orthopaedics and Traumatology,Li Ka Shing Institute of Health Sciences,Chinese University of Hong Kong,Hong Kong
2.Department of Chemical Pathology,Li Ka Shing Institute of Health Sciences,Chinese University of Hong Kong,Hong Kong
3.Department of Experimental & Health Sciences,Universitat Pompeu Fabra (UPF),CIBERNED,ICREA,Barcelona,Spain
4.Centro Nacional de Investigaciones Cardiovasculares (CNIC),Madrid,Spain
5.Key Laboratory of RNA Biology,Institute of Biophysics,Chinese Academy of Sciences,Beijing,China
6.University of Chinese Academy of Sciences,Beijing,China
7.Department of Biology,Southern University of Science and Technology,Shenzhen,China
8.Department of Chemistry and State Key Laboratory of Marine Pollution,City University of Hong Kong,Kowloon Tong,Hong Kong
9.College of Life Sciences,Xinyang Normal University,Xinyang,China
10.Friedrich Miescher Institute for Biomedical Research,Novartis Research Foundation,Basel,Switzerland
11.Shenzhen Research Institute of City University of Hong Kong,Shenzhen,China
推荐引用方式
GB/T 7714
Chen,Xiaona,Yuan,Jie,Xue,Guang,等. Translational control by DHX36 binding to 5′UTR G-quadruplex is essential for muscle stem-cell regenerative functions[J]. Nature Communications,2021,12(1).
APA
Chen,Xiaona.,Yuan,Jie.,Xue,Guang.,Campanario,Silvia.,Wang,Di.,...&Wang,Huating.(2021).Translational control by DHX36 binding to 5′UTR G-quadruplex is essential for muscle stem-cell regenerative functions.Nature Communications,12(1).
MLA
Chen,Xiaona,et al."Translational control by DHX36 binding to 5′UTR G-quadruplex is essential for muscle stem-cell regenerative functions".Nature Communications 12.1(2021).
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