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Repeated transient mRNA bursts precede increases in transcriptional and mitochondrial proteins during training in human skeletal muscle

机译:在人体骨骼肌训练过程中重复的瞬时mRNA爆发先于转录和线粒体蛋白的增加

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摘要

Exercise training induces mitochondrial biogenesis, but the time course of molecular sequelae that accompany repetitive training stimuli remains to be determined in human skeletal muscle. Therefore, throughout a seven-session, high-intensity interval training period that increased (12%), we examined the time course of responses of (a) mitochondrial biogenesis and fusion and fission proteins, and (b) selected transcriptional and mitochondrial mRNAs and proteins in human muscle. Muscle biopsies were obtained 4 and 24 h after the 1st, 3rd, 5th and 7th training session. PGC-1α mRNA was increased >10-fold 4 h after the 1st session and returned to control within 24 h. This ‘saw-tooth’ pattern continued until the 7th bout, with smaller increases after each bout. In contrast, PGC-1α protein was increased 24 h after the 1st bout (23%) and plateaued at +30–40% between the 3rd and 7th bout. Increases in PGC-1β mRNA and protein were more delayed and smaller, and did not persist. Distinct patterns of increases were observed in peroxisome proliferator-activated receptor (PPAR) α and γ protein (1 session), PPAR β/δ mRNA and protein (5 sessions) and nuclear respiratory factor-2 protein (3 sessions) while no changes occurred in mitochondrial transcription factor A protein. Citrate synthase (CS) and β-HAD mRNA were rapidly increased (1 session), followed 2 sessions later (session 3) by increases in CS and β-HAD activities, and mitochondrial DNA. Changes in COX-IV mRNA (session 3) and protein (session 5) were more delayed. Training also increased mitochondrial fission proteins (fission protein-1, >2-fold; dynamin-related protein-1, 47%) and the fusion protein mitofusin-1 (35%) but not mitofusin-2. This study has provided the following novel information: (a) the training-induced increases in transcriptional and mitochondrial proteins appear to result from the cumulative effects of transient bursts in their mRNAs, (b) training-induced mitochondrial biogenesis appears to involve re-modelling in addition to increased mitochondrial content, and (c) the ‘transcriptional capacity’ of human muscle is extremely sensitive, being activated by one training bout.
机译:运动训练诱导线粒体的生物发生,但是在人体骨骼肌中伴随重复训练刺激的分子后遗症的时程仍有待确定。因此,在增加的七个阶段的高强度间歇训练期间(12%),我们检查了以下时间响应过程:(a)线粒体的生物发生,融合和裂变蛋白,以及(b)选择的转录和线粒体mRNA和人体肌肉中的蛋白质。在第1、3、5和7次训练后的第4和24小时进行肌肉活检。在第一个疗程后4小时,PGC-1αmRNA增加> 10倍,并在24小时内恢复正常。这种“锯齿”模式一直持续到第七回合,每次回合后增加幅度较小。相反,PGC-1α蛋白在第一次发作后24小时增加(23%),在第三次和第七次发作之间稳定在+ 30–40%。 PGC-1βmRNA和蛋白的增加更多地延迟且更小,并且没有持续。过氧化物酶体增殖物激活受体(PPAR)α和γ蛋白(1个疗程),PPARβ/δmRNA和蛋白(5个疗程)和核呼吸因子-2蛋白(3个疗程)观察到明显的增加模式,而未发生变化在线粒体转录因子A蛋白中。柠檬酸合酶(CS)和β-HADmRNA迅速增加(1个疗程),随后2个疗程(3个疗程)之后,CS和β-HAD活性以及线粒体DNA的增加。 COX-IV mRNA(第3节)和蛋白质(第5节)的变化更为延迟。训练还增加了线粒体裂变蛋白(裂变蛋白1,> 2倍;与动力蛋白相关的蛋白-1,47%)和融合蛋白丝裂霉素1(35%),但丝裂霉素2却没有。这项研究提供了以下新信息:(a)训练诱导的转录和线粒体蛋白增加似乎是由于其mRNA瞬时爆发的累积效应所致;(b)训练诱导的线粒体生物发生似乎涉及重新建模除了增加线粒体含量外,(c)一次训练可以激活人的肌肉的“转录能力”。

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