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骨骼肌肥大适应性变化在抗阻运动训练的早期阶段占主导地位,与源自氧化氘的肌肉蛋白质合成测量值以及雷帕霉素复合物1信号传导的机制靶点相匹配。

Skeletal muscle hypertrophy adaptations predominate in the early stages of resistance exercise training, matching deuterium oxide-derived measures of muscle protein synthesis and mechanistic target of rapamycin complex 1 signaling.

作者信息

Brook Matthew S, Wilkinson Daniel J, Mitchell William K, Lund Jonathan N, Szewczyk Nathaniel J, Greenhaff Paul L, Smith Ken, Atherton Philip J

机构信息

*Medical Research Council-Arthritis Research UK Centre of Excellence for Musculoskeletal Ageing Research, Division of Clinical, Metabolic, and Molecular Physiology, University of Nottingham, Derby, United Kingdom; and Department of Surgery, Royal Derby Hospital, Derby, United Kingdom.

*Medical Research Council-Arthritis Research UK Centre of Excellence for Musculoskeletal Ageing Research, Division of Clinical, Metabolic, and Molecular Physiology, University of Nottingham, Derby, United Kingdom; and Department of Surgery, Royal Derby Hospital, Derby, United Kingdom

出版信息

FASEB J. 2015 Nov;29(11):4485-96. doi: 10.1096/fj.15-273755. Epub 2015 Jul 13.

Abstract

Resistance exercise training (RET) is widely used to increase muscle mass in athletes and also aged/cachectic populations. However, the time course and metabolic and molecular control of hypertrophy remain poorly defined. Using newly developed deuterium oxide (D2O)-tracer techniques, we investigated the relationship between long-term muscle protein synthesis (MPS) and hypertrophic responses to RET. A total of 10 men (23 ± 1 yr) undertook 6 wk of unilateral (1-legged) RET [6 × 8 repetitions, 75% 1 repetition maximum (1-RM) 3/wk], rendering 1 leg untrained (UT) and the contralateral, trained (T). After baseline bilateral vastus lateralis (VL) muscle biopsies, subjects consumed 150 ml D2O (70 atom percentage; thereafter 50 ml/wk) with regular body water monitoring in saliva via high-temperature conversion elemental analyzer:isotope ratio mass spectrometer. Further bilateral VL muscle biopsies were taken at 3 and 6 wk to temporally quantify MPS via gas chromatography:pyrolysis:isotope ratio mass spectrometer. Expectedly, only the T leg exhibited marked increases in function [i.e., 1-RM/maximal voluntary contraction (60°)] and VL thickness (peaking at 3 wk). Critically, whereas MPS remained unchanged in the UT leg (e.g., ∼1.35 ± 0.08%/d), the T leg exhibited increased MPS at 0-3 wk (1.6 ± 0.01%/d), but not at 3-6 wk (1.29 ± 0.11%/d); this was reflected by dampened acute mechanistic target of rapamycin complex 1 signaling responses to RET, beyond 3 wk. Therefore, hypertrophic remodeling is most active during the early stages of RET, reflecting longer-term MPS. Moreover, D2O heralds promise for coupling MPS and muscle mass and providing insight into the control of hypertrophy and efficacy of anabolic interventions.

摘要

抗阻运动训练(RET)被广泛用于增加运动员以及老年/恶病质人群的肌肉量。然而,肥大的时间进程以及代谢和分子调控仍未明确。我们使用新开发的氧化氘(D2O)示踪技术,研究了长期肌肉蛋白合成(MPS)与RET肥大反应之间的关系。共有10名男性(23±1岁)进行了6周的单侧(单腿)RET训练[6组,每组8次重复,每周3次,75%的1次重复最大值(1-RM)],使一条腿不训练(UT),对侧腿训练(T)。在进行双侧股外侧肌(VL)肌肉活检作为基线后,受试者饮用150毫升D2O(70原子百分比;此后每周50毫升),并通过高温转换元素分析仪:同位素比质谱仪对唾液中的身体水分进行定期监测。在第3周和第6周再次进行双侧VL肌肉活检,通过气相色谱:热解:同位素比质谱仪对MPS进行时间量化。不出所料,只有训练腿的功能[即1-RM/最大自主收缩(60°)]和VL厚度显著增加(在第3周达到峰值)。关键的是,虽然未训练腿的MPS保持不变(例如,约1.35±0.08%/天),但训练腿在0至3周时MPS增加(1.6±0.01%/天),而在3至6周时未增加(1.29±0.11%/天);这在第3周后对RET的雷帕霉素复合物1信号急性机制反应减弱中得到体现。因此,肥大重塑在RET的早期阶段最为活跃,反映了长期的MPS。此外,D2O有望将MPS与肌肉量联系起来,并为肥大的控制和合成代谢干预的效果提供见解。

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