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首页> 外文期刊>American Journal of Physiology >Aging differentially affects human skeletal muscle microRNA expression at rest and after an anabolic stimulus of resistance exercise and essential amino acids
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Aging differentially affects human skeletal muscle microRNA expression at rest and after an anabolic stimulus of resistance exercise and essential amino acids

机译:老化差异地影响休息和抗性运动和必需氨基酸的合成代谢刺激后的人骨骼肌microRNA表达

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Aging differentially affects human skeletal muscle microRNA expression at rest and after an anabolic stimulus of resistance exercise and essential amino acids. Am J Physiol Endo-crinol Metab .-Sarcopenia, skeletalmuscle loss during aging, is associated with increased falls, fractures, morbidity, and loss of independence. MicroRNAs (miRNAs) are novel posttranscriptional regulators. The role of miRNAs in cell size regulation after an anabolic stimulus in human skeletal muscle is unknown. We hypothesized that aging would be associated with a differential expression of skeletal muscle primary miRNA (pri-miRNA) and mature miRNA (miR). To test this hypothesis, we used real-time PCR and immunoblotting before and after an anabolic stimulus (resistance exercise + ingestion of a 20-g leucine-enriched essential amino acid solution) to measure the expression of muscle-specific miRNAs (miR-1, miR-133a, and miR-206), upstream regu-lators (MyoD and myogenin), and downstream targets [insulin-like growth factor-I, histone deacetylase-4, myocyte enhancing factor-2, and Ras homolog enriched in brain (Rheb)] in skeletal muscle of young and older men. Muscle biopsies were obtained at baseline and 3 and 6 h after exercise. At baseline, we found pri-miRNA-1-1, -1-2, -133a-l, and -133a-2 expression elevated in older compared with young men (P < 0.05). Pri-miRNA-1-2, -133a-l, and -133a-2 were reduced at 6 h after exercise only in the young men compared with baseline, whereas pri-miRNA-206 was elevated at different postexer-cise time points in older and young men (P < 0.05). Compared with baseline, miR-1 was reduced only in the young men, whereas Rheb protein was increased in both age groups after the anabolic stimulus (P < 0.05). We conclude that skeletal muscle primary and mature miRNA expression in young men is readily altered by an anabolic stimulus of resistance exercise + essential amino acid ingestion. However, aging is associated with higher basal skeletal muscle primary miRNA expression and a dysregulated miRNA response after the anabolic stimulus.
机译:老化差异地影响休息和经过合成的抗性运动和必需氨基酸的合成代谢刺激之后的人骨骼肌微瘤表达。 AM J Physiol Endo-Crinol Metab。 - 嗜睡期,老化期间的骨骼损失,与增加的跌落,骨折,发病率和独立丧失有关。 MicroRNAS(miRNA)是新的后术语监管机构。 miRNA在人骨骼肌中的合成代谢刺激后细胞尺寸调节中的作用是未知的。我们假设老化与骨骼肌原发性miRNA(PRI-miRNA)和成熟miRNA(miR)的差异表达相关。为了测试这一假设,我们在代谢刺激之前和之后使用实时PCR和免疫印迹(抗性运动+摄入20g亮氨酸浓缩的必需氨基酸溶液)以测量肌肉特异性miRNA的表达(miR-1 ,miR-133a和miR-206),上游调节蛋白(Myod和Myogenin)和下游靶标[胰岛素样生长因子-1,组蛋白脱乙酰酶-4,肌细胞增强因子-2和富含脑中的RAS同源物(RHEB)]在年轻人和老年人的骨骼肌中。在运动后在基线和3和6小时获得肌肉活组织检查。在基线时,我们发现PRI-miRNA-1-1,-1-2,-133a-L和-133A-2表达与年轻男性相比较大(P <0.05)。 PRI-miRNA-1-2,-133A-1和-133A-2在6小时后,只有在年轻人的运动后6小时,与基线相比,而PRI-miRNA-206在不同的发布时间点升高年龄和年轻人(P <0.05)。与基线相比,MIR-1只在年轻人中减少,而合成代谢刺激后,VHEB蛋白在两龄段组中增加(P <0.05)。我们得出结论,通过抗性运动+必需氨基酸摄入的合成代谢刺激,骨骼肌初级和成熟miRNA表达易于改变。然而,老化与较高的基础骨骼肌原发性miRNA表达和合成代谢刺激后的具有疑难的miRNA反应相关。

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