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首页> 外文期刊>The FASEB Journal >Diminished skeletal muscle microRNA expression with aging is associated with attenuated muscle plasticity and inhibition of IGF-1 signaling
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Diminished skeletal muscle microRNA expression with aging is associated with attenuated muscle plasticity and inhibition of IGF-1 signaling

机译:随着年龄的增长,骨骼肌 microRNA 表达减少与肌肉可塑性减弱和 IGF-1 信号传导抑制有关

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摘要

Older individuals have a reduced capacity to induce muscle hypertrophy with resistance exercise (RE), which may contribute to the age-induced loss of muscle mass and function, sarcopenia. We tested the novel hypothesis that dysregulation of microRNAs (miRNAs) may contribute to reduced muscle plasticity with aging. Skeletal muscle expression profiling of protein-coding genes and miRNA was performed in younger (YNG) and older (OLD) men after an acute bout of RE. 21 miRNAs were altered by RE in YNG men, while no RE-induced changes in miRNA expression were observed in OLD men. This striking absence in miRNA regulation in OLD men was associated with blunted transcription of mRNAs, with only 42 genes altered in OLD men vs. 175 in YNG men following RE, demonstrating a reduced adaptability of aging muscle to exercise. Integrated bioinformatics analysis identified miR-126 as an important regulator of the transcriptional response to exercise and reduced lean mass in OLD men. Manipulation of miR-126 levels in myocytes, in vitro, revealed its direct effects on the expression of regulators of skeletal muscle growth and activation of insulin growth factor 1 (IGF-1) signaling. This work identifies a mechanistic role of miRNA in the adaptation of muscle to anabolic stimulation and reveals a significant impairment in exercise-induced miRNA/mRNA regulation with aging.
机译:老年人通过阻力运动 (RE) 诱发肌肉肥大的能力降低,这可能导致年龄引起的肌肉质量和功能丧失,即肌肉减少症。我们测试了新的假设,即 microRNA (miRNA) 的失调可能导致肌肉可塑性随着年龄的增长而降低。在急性 RE 发作后,在年轻 (YNG) 和老年 (OLD) 男性中进行蛋白质编码基因和 miRNA 的骨骼肌表达谱分析。在 YNG 男性中,RE 改变了 21 个 miRNA,而在 OLD 男性中未观察到 RE 诱导的 miRNA 表达变化。老年男性miRNA调控的这种显着缺失与mRNA的迟钝转录有关,在RE之后,老年男性中只有42个基因发生了改变,而YNG男性中则有175个基因发生了改变,这表明衰老肌肉对运动的适应性降低。综合生物信息学分析确定 miR-126 是 OLD 男性运动和瘦体重减少的转录反应的重要调节因子。在体外操纵肌细胞中的 miR-126 水平揭示了其对骨骼肌生长调节因子表达和胰岛素生长因子 1 (IGF-1) 信号激活的直接影响。这项工作确定了 miRNA 在肌肉适应合成代谢刺激中的机制作用,并揭示了运动诱导的 miRNA/mRNA 调节随年龄增长的显着损害。

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