生理Ca2+瞬态缺失是去神经支配后骨骼肌线粒体功能障碍的初始触发。

IF 5.3 2区医学 Q2 CELL BIOLOGY

Skeletal Muscle Pub Date : 2017-04-10 DOI:10.1186/s13395-017-0123-0

Chehade Karam, Jianxun Yi, Yajuan Xiao, Kamal Dhakal, Lin Zhang, Xuejun Li, Carlo Manno, Jiejia Xu, Kaitao Li, Heping Cheng, Jianjie Ma, Jingsong Zhou

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引用次数: 35

摘要

背景:运动神经元通过启动肌肉的动作电位来控制肌肉收缩。运动神经元的肌肉去神经支配导致肌肉萎缩，这与线粒体功能障碍有关。众所周知，去神经支配促进肌肉中线粒体活性氧(ROS)的产生，而去神经支配肌肉中线粒体ROS产生的最初原因尚不清楚。由于去神经支配使肌肉与运动神经元分离，并使其不受任何电刺激，因此没有动作电位被启动，因此，在去神经支配的肌纤维内不会产生生理Ca2+瞬态。我们测试了生理Ca2+瞬态的丧失是否是导致失神经骨骼肌线粒体功能障碍的初始原因。方法:一种表达线粒体靶向生物传感器(mt-cpYFP)的转基因小鼠模型可以实时测量去神经支配后ros相关的线粒体代谢功能，称为mitoflash。通过活细胞成像、电生理、药理学和生化研究，我们研究了去神经控制后引发ros相关线粒体功能障碍的潜在分子机制。结果:我们发现肌纤维在去神经支配后24小时有丝分裂活性增加了4倍。去神经支配诱导的丝裂闪活性可能与线粒体通透性过渡孔(mPTP)活性的增加有关，因为应用环孢素a可减弱丝裂闪活性。电刺激可迅速降低假手术和去神经支配肌纤维的丝裂闪活性。我们进一步证明，线粒体内的Ca2+水平遵循细胞质内Ca2+瞬态的时间过程，Ru360对线粒体Ca2+摄取的抑制阻断了电刺激对mitoflash活性的影响。结论:由于去神经支配导致细胞质内Ca2+瞬态的损失导致下游线粒体Ca2+摄取的缺失。我们的研究表明，这可能是骨骼肌中mptp相关线粒体ROS生成增强的初始触发因素。

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Absence of physiological Ca²⁺ transients is an initial trigger for mitochondrial dysfunction in skeletal muscle following denervation.

Background: Motor neurons control muscle contraction by initiating action potentials in muscle. Denervation of muscle from motor neurons leads to muscle atrophy, which is linked to mitochondrial dysfunction. It is known that denervation promotes mitochondrial reactive oxygen species (ROS) production in muscle, whereas the initial cause of mitochondrial ROS production in denervated muscle remains elusive. Since denervation isolates muscle from motor neurons and deprives it from any electric stimulation, no action potentials are initiated, and therefore, no physiological Ca²⁺ transients are generated inside denervated muscle fibers. We tested whether loss of physiological Ca²⁺ transients is an initial cause leading to mitochondrial dysfunction in denervated skeletal muscle.

Methods: A transgenic mouse model expressing a mitochondrial targeted biosensor (mt-cpYFP) allowed a real-time measurement of the ROS-related mitochondrial metabolic function following denervation, termed "mitoflash." Using live cell imaging, electrophysiological, pharmacological, and biochemical studies, we examined a potential molecular mechanism that initiates ROS-related mitochondrial dysfunction following denervation.

Results: We found that muscle fibers showed a fourfold increase in mitoflash activity 24 h after denervation. The denervation-induced mitoflash activity was likely associated with an increased activity of mitochondrial permeability transition pore (mPTP), as the mitoflash activity was attenuated by application of cyclosporine A. Electrical stimulation rapidly reduced mitoflash activity in both sham and denervated muscle fibers. We further demonstrated that the Ca²⁺ level inside mitochondria follows the time course of the cytosolic Ca²⁺ transient and that inhibition of mitochondrial Ca²⁺ uptake by Ru360 blocks the effect of electric stimulation on mitoflash activity.

Conclusions: The loss of cytosolic Ca²⁺ transients due to denervation results in the downstream absence of mitochondrial Ca²⁺ uptake. Our studies suggest that this could be an initial trigger for enhanced mPTP-related mitochondrial ROS generation in skeletal muscle.

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来源期刊

Skeletal Muscle CELL BIOLOGY-

CiteScore

9.10

自引率

0.00%

发文量

审稿时长

12 weeks

期刊介绍： The only open access journal in its field, Skeletal Muscle publishes novel, cutting-edge research and technological advancements that investigate the molecular mechanisms underlying the biology of skeletal muscle. Reflecting the breadth of research in this area, the journal welcomes manuscripts about the development, metabolism, the regulation of mass and function, aging, degeneration, dystrophy and regeneration of skeletal muscle, with an emphasis on understanding adult skeletal muscle, its maintenance, and its interactions with non-muscle cell types and regulatory modulators. Main areas of interest include: -differentiation of skeletal muscle- atrophy and hypertrophy of skeletal muscle- aging of skeletal muscle- regeneration and degeneration of skeletal muscle- biology of satellite and satellite-like cells- dystrophic degeneration of skeletal muscle- energy and glucose homeostasis in skeletal muscle- non-dystrophic genetic diseases of skeletal muscle, such as Spinal Muscular Atrophy and myopathies- maintenance of neuromuscular junctions- roles of ryanodine receptors and calcium signaling in skeletal muscle- roles of nuclear receptors in skeletal muscle- roles of GPCRs and GPCR signaling in skeletal muscle- other relevant aspects of skeletal muscle biology. In addition, articles on translational clinical studies that address molecular and cellular mechanisms of skeletal muscle will be published. Case reports are also encouraged for submission. Skeletal Muscle reflects the breadth of research on skeletal muscle and bridges gaps between diverse areas of science for example cardiac cell biology and neurobiology, which share common features with respect to cell differentiation, excitatory membranes, cell-cell communication, and maintenance. Suitable articles are model and mechanism-driven, and apply statistical principles where appropriate; purely descriptive studies are of lesser interest.