首页> 外文期刊>Pfluegers Archiv: European Journal of Physiology >High force development augments skeletal muscle signalling in resistance exercise modes equalized for time under tension
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High force development augments skeletal muscle signalling in resistance exercise modes equalized for time under tension

机译:高强度发展增强了抵抗运动模式中骨骼肌的信号传导,使之在紧张状态下保持时间平衡

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摘要

How force development and time under tension (TUT) during resistance exercise (RE) influence anabolic signalling of skeletal muscle is incompletely understood. We hypothesized that high force development during RE is more important for post-exercise-induced signalling than submaximal and fatiguing RE with lower force development but similar TUT. Twenty-two male subjects (24 +/- 6 years, 181 +/- 9 cm, 79 +/- 2 kg) performed three distinct RE modes in the fed state with equal TUT but distinct force output: (i) maximal eccentric RE (ECC, n = 7) three sets, eight reps, 100 % eccentric dynamic force; (ii) standard RE (STD, n = 7), three sets, 10 reps, 75 % dynamic force; and (iii) high fatiguing single-set RE (HIT, n = 8), 20 reps, 100 % eccentric-concentric force; vastus lateralis biopsies were collected at baseline, 15, 30, 60, 240 min and 24 h after RE, and the signalling of mechanosensitive and mammalian target of rapamycin (mTOR)-related proteins was determined. The phosphorylation levels of pFAK(Tyr397), pJNK(Thr183/Tyr185), pAKT(Thr308/Ser473), pmTOR(Ser2448), p4E-BP1(Thr37/46), p70s6k(Thr389)/(Ser421/Thr424) and pS6(Ser235/236) were significantly higher in ECC than those in STD and HIT at several time points (P < 0.01). pJNK(Thr183/Tyr185) and pS6(Ser235/236) levels were significantly higher in type II myofibres in ECC compared with STD and HIT. HIT exerted throughout the weakest signalling response. We conclude that high force development during acute RE is superior for anabolic skeletal muscle signalling than fatiguing RE with lower force output but similar TUT. Our results suggest that this response is substantially driven by the higher activation of type II myofibres during RE.
机译:抵抗运动(RE)期间的力量发展和拉伸时间(TUT)如何影响骨骼肌的合成代谢信号。我们假设,RE期间的高力量发展对于运动后诱发的信号传递比次最大和疲劳性RE(具有较低的力量发展但TUT类似)更为重要。 22名男性受试者(24 +/- 6岁,181 +/- 9厘米,79 +/- 2公斤)在进食状态下以相同的TUT但有不同的力输出执行三种不同的RE模式:(i)最大偏心RE (ECC,n = 7)三组,八次重复,100%偏心动力; (ii)标准RE(STD,n = 7),三套,每组10次,动态力为75%; (iii)高疲劳单组RE(HIT,n = 8),20次重复,100%偏心同心力;在RE后的第15、30、60、240、24小时,在基线时收集股外侧肌活检,并确定雷帕霉素(mTOR)相关蛋白的机械敏感性和哺乳动物靶标的信号传导。 pFAK(Tyr397),pJNK(Thr183 / Tyr185),pAKT(Thr308 / Ser473),pmTOR(Ser2448),p4E-BP1(Thr37 / 46),p70s6k(Thr389)/(Ser421 / Thr424)和pS6(磷酸化水平)在几个时间点,ECC中的Ser235 / 236)显着高于STD和HIT(P <0.01)。与STD和HIT相比,ECC II型肌纤维中的pJNK(Thr183 / Tyr185)和pS6(Ser235 / 236)水平显着更高。 HIT贯穿了最弱的信号响应。我们得出结论,在合成代谢的骨骼肌信号传导方面,急性RE期间的高力量发展要比具有较低力量输出但TUT相似的疲劳RE更具优势。我们的结果表明,这种反应基本上是由RE期间II型肌纤维的更高激活所驱动的。

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