运动处方原则，以及它们如何影响运动诱导的转录因子和其他线粒体生物发生调节剂的变化。

Principles of Exercise Prescription, and How They Influence Exercise-Induced Changes of Transcription Factors and Other Regulators of Mitochondrial Biogenesis.

机构信息

Institute of Sport, Exercise and Active Living (ISEAL), College of Sport and Exercise Science, Victoria University, Melbourne, Australia.

Department of Diabetes, Central Clinical School, Faculty of Medicine, Nursing and Health Sciences, Monash University, Alfred Centre, 99 Commercial Rd, Melbourne, VIC, 3004, Australia.

出版信息

Sports Med. 2018 Jul;48(7):1541-1559. doi: 10.1007/s40279-018-0894-4.

DOI:10.1007/s40279-018-0894-4

PMID:29675670

Abstract

Physical inactivity represents the fourth leading risk factor for mortality, and it has been linked with a series of chronic disorders, the treatment of which absorbs ~ 85% of healthcare costs in developed countries. Conversely, physical activity promotes many health benefits; endurance exercise in particular represents a powerful stimulus to induce mitochondrial biogenesis, and it is routinely used to prevent and treat chronic metabolic disorders linked with sub-optimal mitochondrial characteristics. Given the importance of maintaining a healthy mitochondrial pool, it is vital to better characterize how manipulating the endurance exercise dose affects cellular mechanisms of exercise-induced mitochondrial biogenesis. Herein, we propose a definition of mitochondrial biogenesis and the techniques available to assess it, and we emphasize the importance of standardizing biopsy timing and the determination of relative exercise intensity when comparing different studies. We report an intensity-dependent regulation of exercise-induced increases in nuclear peroxisome proliferator-activated receptor γ coactivator-1α (PGC-1α) protein content, nuclear phosphorylation of p53 (serine 15), and PGC-1α messenger RNA (mRNA), as well as training-induced increases in PGC-1α and p53 protein content. Despite evidence that PGC-1α protein content plateaus within a few exercise sessions, we demonstrate that greater training volumes induce further increases in PGC-1α (and p53) protein content, and that short-term reductions in training volume decrease the content of both proteins, suggesting training volume is still a factor affecting training-induced mitochondrial biogenesis. Finally, training-induced changes in mitochondrial transcription factor A (TFAM) protein content are regulated in a training volume-dependent manner and have been linked with training-induced changes in mitochondrial content.

摘要

身体活动不足是导致死亡的第四大主要风险因素，它与一系列慢性疾病有关，这些疾病的治疗费用占发达国家医疗保健费用的 85%左右。相反，身体活动促进了许多健康益处；耐力运动尤其能强有力地刺激线粒体生物发生，它被常规用于预防和治疗与线粒体功能不佳相关的慢性代谢疾病。鉴于维持健康的线粒体池的重要性，更好地描述操纵耐力运动剂量如何影响细胞内运动诱导的线粒体生物发生的机制至关重要。在此，我们提出了线粒体生物发生的定义和评估它的可用技术，并强调在比较不同研究时标准化活检时机和确定相对运动强度的重要性。我们报告了运动诱导的核过氧化物酶体增殖物激活受体 γ 共激活因子 1α（PGC-1α）蛋白含量、核 p53（丝氨酸 15）磷酸化和 PGC-1α 信使 RNA（mRNA）的强度依赖性调节，以及训练诱导的 PGC-1α 和 p53 蛋白含量增加。尽管有证据表明 PGC-1α 蛋白含量在几次运动后达到稳定，但我们证明更大的训练量会进一步增加 PGC-1α（和 p53）蛋白含量，而短期减少训练量会降低这两种蛋白质的含量，这表明训练量仍然是影响训练诱导的线粒体生物发生的一个因素。最后，线粒体转录因子 A（TFAM）蛋白含量的训练诱导变化受训练量的调节，并与训练诱导的线粒体含量变化有关。

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运动处方原则，以及它们如何影响运动诱导的转录因子和其他线粒体生物发生调节剂的变化。

Principles of Exercise Prescription, and How They Influence Exercise-Induced Changes of Transcription Factors and Other Regulators of Mitochondrial Biogenesis.

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