运动通过调节肌肉卫星细胞中Mettl3介导的MyoD的m6A甲基化来促进青少年骨骼肌生长。
Exercise promotes skeletal muscle growth in adolescents via modulating Mettl3-mediated m6A methylation of MyoD in muscle satellite cells.
作者信息
Feng Shujing, Zhou Hao, Lin Xingzuan, Zhu Siyuan, Chen Huifang, Zhou Han, Wang Ru, Wang Peng, Shao Xiexiang, Wang Jianhua
机构信息
Xinhua Hospital affiliated to Shanghai Jiao Tong University School of Medicine, Shanghai, China.
School of Exercise and Health, Shanghai University of Sport, Shanghai, China.
出版信息
Cell Mol Biol Lett. 2024 Dec 4;29(1):150. doi: 10.1186/s11658-024-00670-x.
BACKGROUND
Exercise exerts positive impacts on skeletal muscle health and homeostasis. Emerging evidence suggests that m6A methylation is involved in various physiological processes. However, the impact of exercise on adolescent skeletal muscle growth and the underlying epigenetic mechanisms remain poorly understood.
METHODS
The lower-limb skeletal muscles were harvested from exercise and control groups to compare the skeletal muscle growth in adolescents. mRNA sequencing was conducted to explore the mechanisms underlying enhanced skeletal muscle growth following exercise. The effects and mechanisms of Mettl3-mediated m6A methylation on adolescent skeletal muscle growth were investigated using muscle satellite cell (MuSC)-specific Mettl3 knockout (KO) mice. The potential function of MyoD for skeletal muscle growth in adolescents was explored by phenotypes after overexpression and evaluation of in vivo myogenesis. Additionally, the effects of the methyl donor betaine on adolescent skeletal muscle growth were investigated in vitro and in vivo.
RESULTS
Exercise could promote skeletal muscle growth in adolescents. Sequencing data analysis and confirmation assays uncovered that exercise significantly increased Mettl3-mediated m6A methylation and elevated the expression levels of activation marker MyoD in MuSCs. Establishment of MuSC-specific Mettl3 KO mice further demonstrated that Mettl3-mediated m6A methylation in MyoD contributed to skeletal muscle growth during adolescence. Mettl3-mediated m6A methylation regulated MyoD mRNA stability at the posttranscriptional level in MuSCs, with a functional site at 234 bp A. Increased expression of MyoD could contribute to myogenesis of adolescent MuSCs. Furthermore, the methyl donor betaine could enhance MyoD expression, contributing to MuSCs activation and skeletal muscle growth in adolescents by boosting m6A methylation levels.
CONCLUSIONS
Exercise promoted skeletal muscle growth in adolescents through facilitating MyoD mRNA stability of MuSCs in a Mettl3-mediated m6A-dependent manner. The methyl donor betaine could be a potential alternative to exercise for promoting adolescent skeletal muscle growth by directly augmenting the global levels of m6A methylation. These findings may provide a theoretical foundation for encouraging daily fitness exercise and ensuring healthy growth in adolescents.
背景
运动对骨骼肌健康和体内平衡具有积极影响。新出现的证据表明,m6A甲基化参与多种生理过程。然而,运动对青少年骨骼肌生长的影响及其潜在的表观遗传机制仍知之甚少。
方法
从运动组和对照组采集下肢骨骼肌,以比较青少年的骨骼肌生长情况。进行mRNA测序以探索运动后骨骼肌生长增强的潜在机制。使用肌肉卫星细胞(MuSC)特异性Mettl3基因敲除(KO)小鼠研究Mettl3介导的m6A甲基化对青少年骨骼肌生长的影响及其机制。通过过表达后的表型和体内成肌评估,探索MyoD对青少年骨骼肌生长的潜在作用。此外,在体外和体内研究了甲基供体甜菜碱对青少年骨骼肌生长的影响。
结果
运动可促进青少年骨骼肌生长。测序数据分析和验证试验发现,运动显著增加了Mettl3介导的m6A甲基化,并提高了MuSC中激活标记物MyoD的表达水平。建立MuSC特异性Mettl3 KO小鼠进一步证明,Mettl3介导的MyoD中的m6A甲基化有助于青春期骨骼肌生长。Mettl3介导的m6A甲基化在转录后水平调节MuSC中MyoD mRNA的稳定性,其功能位点位于234 bp A处。MyoD表达的增加可能有助于青少年MuSC的成肌作用。此外,甲基供体甜菜碱可通过提高m6A甲基化水平增强MyoD表达,从而促进青少年MuSC的激活和骨骼肌生长。
结论
运动通过Mettl3介导的m6A依赖方式促进MuSC的MyoD mRNA稳定性,从而促进青少年骨骼肌生长。甲基供体甜菜碱可能是一种潜在的运动替代物,通过直接提高m6A甲基化的整体水平来促进青少年骨骼肌生长。这些发现可能为鼓励青少年日常健身运动和确保健康成长提供理论基础。
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