骨骼肌
肌肉肥大
生物
基因
转录因子
DNA甲基化
肌肉团
下调和上调
信使核糖核酸
基因表达
比目鱼肌
细胞生物学
内分泌学
内科学
遗传学
医学
作者
Sebastian Edman,Ronald G. Jones,Paulo R. Jannig,Rodrigo Fernandez‐Gonzalo,Jessica Norrbom,Nicholas T. Thomas,Sabin Khadgi,Pieter Koopmans,Francielly Morena da Silva,Toby L. Chambers,Calvin S. Peterson,Logan N. Scott,Nicholas P. Greene,Vandré C. Figueiredo,Christopher S. Fry,Zhengye Liu,Johanna T. Lanner,Yuan Wen,Björn Alkner,Kevin A. Murach,Ferdinand von Walden
标识
DOI:10.1038/s44319-024-00299-z
摘要
Abstract A detailed understanding of molecular responses to a hypertrophic stimulus in skeletal muscle leads to therapeutic advances aimed at promoting muscle mass. To decode the molecular factors regulating skeletal muscle mass, we utilized a 24-h time course of human muscle biopsies after a bout of resistance exercise. Our findings indicate: (1) the DNA methylome response at 30 min corresponds to upregulated genes at 3 h, (2) a burst of translation- and transcription-initiation factor-coding transcripts occurs between 3 and 8 h, (3) changes to global protein-coding gene expression peaks at 8 h, (4) ribosome-related genes dominate the mRNA landscape between 8 and 24 h, (5) methylation-regulated MYC is a highly influential transcription factor throughout recovery. To test whether MYC is sufficient for hypertrophy, we periodically pulse MYC in skeletal muscle over 4 weeks. Transient MYC increases muscle mass and fiber size in the soleus of adult mice. We present a temporally resolved resource for understanding molecular adaptations to resistance exercise in muscle ( http://data.myoanalytics.com ) and suggest that controlled MYC doses influence the exercise-related hypertrophic transcriptional landscape.
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