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The role of skeletal muscle mTOR in the regulation of mechanical load-induced growth

机译:骨骼肌mTOR在调节机械负荷诱导的生长中的作用

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摘要

Non-technical summaryChronic mechanical loading (CML) of skeletal muscle induces growth and this effect can be blocked by the drug rapamycin. Rapamycin is considered to be a highly specific inhibitor of the mammalian target of rapamycin (mTOR), and thus, many have concluded that mTOR plays a key role in CML-induced growth. However, direct evidence that mTOR confers the CML-induced activation of growth promoting events such as hypertrophy, hyperplasia and ribosome biogenesis is lacking. This study addressed that gap in knowledge by using a specialized line of transgenic mice. Surprisingly, the results indicate that only a few of the growth promoting events induced by CML are fully dependent on mTOR signalling (e.g. hypertrophy). These results advance our understanding of the molecular mechanisms that regulate skeletal muscle mass and should help future studies aimed at identifying targets for therapies that can prevent the loss of muscle mass during conditions such as bedrest, immobilization, and ageing.
机译:非技术摘要骨骼肌的慢性机械负荷(CML)诱导生长,这种作用可以被雷帕霉素药物所阻断。雷帕霉素被认为是雷帕霉素(mTOR)哺乳动物靶标的高度特异性抑制剂,因此,许多人得出结论,mTOR在CML诱导的生长中起关键作用。但是,缺乏直接证据证明mTOR赋予CML诱导的促进生长的事件(例如肥大,增生和核糖体生物发生)的激活。这项研究通过使用专门的转基因小鼠品系解决了这一知识鸿沟。令人惊讶地,结果表明,仅少数由CML诱导的促进生长的事件完全依赖于mTOR信号转导(例如肥大)。这些结果使我们对调节骨骼肌质量的分子机制有了更深入的了解,并应有助于未来的研究,旨在确定可预防诸如卧床休息,固定和老化等条件下肌肉质量损失的治疗目标。

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