Autophagy plays a role in skeletal muscle mitochondrial biogenesis in an endurance exercise-trained condition

被引:0
作者
Jeong-sun Ju
Sei-il Jeon
Je-young Park
Jong-young Lee
Seong-cheol Lee
Ki-jung Cho
Jong-moon Jeong
机构
[1] Department of Exercise Science and Research Institute of Sports Science,Department of Life Science
[2] The University of Suwon,undefined
来源
The Journal of Physiological Sciences | 2016年 / 66卷
关键词
Autophagy; Mitochondrial biogenesis; Mitophagy; Exercise; Skeletal muscle;
D O I
暂无
中图分类号
学科分类号
摘要
Mitochondrial homeostasis is tightly regulated by two major processes: mitochondrial biogenesis and mitochondrial degradation by autophagy (mitophagy). Research in mitochondrial biogenesis in skeletal muscle in response to endurance exercise training has been well established, while the mechanisms regulating mitophagy and the interplay between mitochondrial biogenesis and degradation following endurance exercise training are not yet well defined. The purpose of this study was to examine the effects of a short-term inhibition of autophagy in response to acute endurance exercise on skeletal muscle mitochondrial biogenesis and dynamics in an exercise-trained condition. Male wild-type C57BL/6 mice performed five daily bouts of 1-h swimming per week for 8 weeks. In order to measure autophagy flux in mouse skeletal muscle, mice were treated with or without 2 days of 0.4 mg/kg/day intraperitoneal colchicine (blocking the degradation of autophagosomes) following swimming exercise training. The autophagic flux assay demonstrated that swimming training resulted in an increase in the autophagic flux (~100 % increase in LC3-II) in mouse skeletal muscle. Mitochondrial fusion proteins, Opa1 and MFN2, were significantly elevated, and mitochondrial fission protein, Drp1, was also increased in trained mouse skeletal muscle, suggesting that endurance exercise training promotes both mitochondrial fusion and fission processes. A mitochondrial receptor, Bnip3, was further increased in exercised muscle when treated with colchicine while Pink/Parkin protein levels were unchanged. The endurance exercise training induced increases in mitochondrial biogenesis marker proteins, SDH, COX IV, and a mitochondrial biogenesis promoting factor, PGC-1α but this effect was abolished in colchicine-treated mouse skeletal muscle. This suggests that autophagy plays an important role in mitochondrial biogenesis and this coordination between these opposing processes is involved in the cellular adaptation to endurance exercise training.
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页码:417 / 430
页数:13
相关论文
共 223 条
  • [1] Rubinsztein DC(2009)In search of an ‘‘autophagomometer” Autophagy 5 585-589
  • [2] Cuervo AM(2013)Increased autophagy accelerates colchicine-induced muscle toxicity Autophagy 12 2115-2125
  • [3] Ravikumar B(2012)Skeletal muscle mitochondria and aging: a review J Aging Res 2012 194821-C210
  • [4] Sarkar S(2010)Autophagy in health and disease. 5. Mitophagy as a way of life Am J Physiol Cell Physiol 299 C203-547
  • [5] Korolchuk V(2010)Regulation of skeletal muscle mitochondrial function: genes to proteins Acta Physiol (Oxf) 199 529-1371
  • [6] Kaushik S(1999)Activation of PPARγ coactivator-1 through transcription factor docking Science 286 1368-20
  • [7] Klionsky DJ(2015)Routine Western blot to check autophagic flux: cautions and recommendations Anal Biochem 477 13-970
  • [8] Ching JK(2013)Expression of mitochondrial fission and fusion regulatory proteins in skeletal muscle during chronic use and disuse Muscle Nerve 48 963-4810
  • [9] Ju JS(2010)Repeated transient mRNA bursts precede increases in transcriptional and mitochondrial proteins during training in human skeletal muscle J Physiol 588 4795-1097
  • [10] Pittman SK(2008)Mitochondrial fusion, fission and autophagy as a quality control axis: the bioenergetic view Biochim Biophys Acta 1777 1092-R969
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