一氧化氮信号不足会损害骨骼肌生长和功能:线粒体失调的影响。
Deficient nitric oxide signalling impairs skeletal muscle growth and performance: involvement of mitochondrial dysregulation.
作者信息
De Palma Clara, Morisi Federica, Pambianco Sarah, Assi Emma, Touvier Thierry, Russo Stefania, Perrotta Cristiana, Romanello Vanina, Carnio Silvia, Cappello Valentina, Pellegrino Paolo, Moscheni Claudia, Bassi Maria Teresa, Sandri Marco, Cervia Davide, Clementi Emilio
机构信息
Unit of Clinical Pharmacology, National Research Council-Institute of Neuroscience, Department of Biomedical and Clinical Sciences "Luigi Sacco", University Hospital "Luigi Sacco", Università di Milano, Milano, Italy.
Scientific Institute IRCCS Eugenio Medea, Bosisio Parini, Italy.
出版信息
Skelet Muscle. 2014 Dec 12;4(1):22. doi: 10.1186/s13395-014-0022-6. eCollection 2014.
BACKGROUND
Nitric oxide (NO), generated in skeletal muscle mostly by the neuronal NO synthases (nNOSμ), has profound effects on both mitochondrial bioenergetics and muscle development and function. The importance of NO for muscle repair emerges from the observation that nNOS signalling is defective in many genetically diverse skeletal muscle diseases in which muscle repair is dysregulated. How the effects of NO/nNOSμ on mitochondria impact on muscle function, however, has not been investigated yet.
METHODS
In this study we have examined the relationship between the NO system, mitochondrial structure/activity and skeletal muscle phenotype/growth/functions using a mouse model in which nNOSμ is absent. Also, NO-induced effects and the NO pathway were dissected in myogenic precursor cells.
RESULTS
We show that nNOSμ deficiency in mouse skeletal muscle leads to altered mitochondrial bioenergetics and network remodelling, and increased mitochondrial unfolded protein response (UPR(mt)) and autophagy. The absence of nNOSμ is also accompanied by an altered mitochondrial homeostasis in myogenic precursor cells with a decrease in the number of myonuclei per fibre and impaired muscle development at early stages of perinatal growth. No alterations were observed, however, in the overall resting muscle structure, apart from a reduced specific muscle mass and cross sectional areas of the myofibres. Investigating the molecular mechanisms we found that nNOSμ deficiency was associated with an inhibition of the Akt-mammalian target of rapamycin pathway. Concomitantly, the Akt-FoxO3-mitochondrial E3 ubiquitin protein ligase 1 (Mul-1) axis was also dysregulated. In particular, inhibition of nNOS/NO/cyclic guanosine monophosphate (cGMP)/cGMP-dependent-protein kinases induced the transcriptional activity of FoxO3 and increased Mul-1 expression. nNOSμ deficiency was also accompanied by functional changes in muscle with reduced muscle force, decreased resistance to fatigue and increased degeneration/damage post-exercise.
CONCLUSIONS
Our results indicate that nNOSμ/NO is required to regulate key homeostatic mechanisms in skeletal muscle, namely mitochondrial bioenergetics and network remodelling, UPR(mt) and autophagy. These events are likely associated with nNOSμ-dependent impairments of muscle fibre growth resulting in a deficit of muscle performance.
背景
一氧化氮(NO)主要由神经元型一氧化氮合酶(nNOSμ)在骨骼肌中生成,对线粒体生物能量学以及肌肉发育和功能均有深远影响。NO对肌肉修复的重要性源于以下观察结果:在许多基因多样的骨骼肌疾病中,肌肉修复失调,nNOS信号传导存在缺陷。然而,NO/nNOSμ对线粒体的影响如何作用于肌肉功能,尚未得到研究。
方法
在本研究中,我们使用nNOSμ缺失的小鼠模型,研究了NO系统、线粒体结构/活性与骨骼肌表型/生长/功能之间的关系。此外,还在成肌前体细胞中剖析了NO诱导的效应和NO信号通路。
结果
我们发现,小鼠骨骼肌中nNOSμ的缺乏会导致线粒体生物能量学改变和网络重塑,线粒体未折叠蛋白反应(UPR(mt))和自噬增加。nNOSμ的缺失还伴随着成肌前体细胞中线粒体稳态的改变,每根肌纤维中的肌核数量减少,围产期生长早期肌肉发育受损。然而,除了特定肌肉质量和肌纤维横截面积减小外,未观察到整体静息肌肉结构的改变。在研究分子机制时,我们发现nNOSμ的缺乏与Akt-雷帕霉素哺乳动物靶标途径的抑制有关。同时,Akt-FoxO3-线粒体E3泛素蛋白连接酶1(Mul-1)轴也失调。特别是,抑制nNOS/NO/环磷酸鸟苷(cGMP)/cGMP依赖性蛋白激酶会诱导FoxO3的转录活性并增加Mul-1的表达。nNOSμ的缺乏还伴随着肌肉功能的变化,肌肉力量降低、抗疲劳能力下降以及运动后变性/损伤增加。
结论
我们的结果表明,nNOSμ/NO是调节骨骼肌关键稳态机制所必需的,即线粒体生物能量学和网络重塑、UPR(mt)和自噬。这些事件可能与nNOSμ依赖性的肌纤维生长受损有关,从而导致肌肉性能不足。
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