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Mechano-biology of skeletal muscle hypertrophy and regeneration: Possible mechanism of stretch-induced activation of resident myogenic stem cells

机译:骨骼肌肥大和再生的力学生物学:拉伸诱导驻留的成肌干细胞活化的可能机制

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In undamaged postnatal muscle fibers with normal contraction and relaxation activities, quiescent satellite cells of resident myogenic stem cells are interposed between the overlying external lamina and the sarcolemma of a subjacent mature muscle fiber. When muscle is injured, exercised, overused or mechanically stretched, these cells are activated to enter the cell proliferation cycle, divide, differentiate, and fuse with the adjacent muscle fiber, and are responsible for regeneration and work-induced hypertrophy of muscle fibers. Therefore, a mechanism must exist to translate mechanical changes in muscle tissue into chemical signals that can activate satellite cells. Recent studies of satellite cells or single muscle fibers in culture and in vivo demonstrated the essential role of hepatocyte growth factor (HGF) and nitric oxide ( NO) radical in the activation pathway. These experiments have also reported that mechanically stretching satellite cells or living skeletal muscles triggers the activation by rapid release of HGF from its extracellular tethering and the subsequent presentation to the receptor c-met. HGF release has been shown to rely on calcium-calmodulin formation and NO radical production in satellite cells and/or muscle fibers in response to the mechanical perturbation, and depend on the subsequent up-regulation of matrix metalloproteinase (MMP) activity. These results indicate that the activation mechanism is a cascade of events including calcium ion influx, calcium-calmodulin formation, NO synthase activation, NO radical production, MMP activation, HGF release and binding to c-met. Better understanding of 'mechano-biology' on the satellite cell activation is essential for designing procedures that could enhance muscle growth and repair activities in meat-animal agriculture and also in neuromuscular disease and aging in humans.
机译:在具有正常收缩和松弛活动的未受损产后肌纤维中,驻留的成肌干细胞的静止卫星细胞介于上层外层肌层和下层成熟肌纤维的肌膜之间。当肌肉受伤,运动,过度使用或机械拉伸时,这些细胞被激活进入细胞增殖周期,与相邻的肌纤维分裂,分化并融合,并负责肌肉纤维的再生和工作诱导的肥大。因此,必须存在一种将肌肉组织中的机械变化转化为可以激活卫星细胞的化学信号的机制。在培养物中和体内对卫星细胞或单条肌纤维的最新研究表明,肝细胞生长因子(HGF)和一氧化氮(NO)自由基在激活途径中具有重要作用。这些实验还报告说,机械拉伸卫星细胞或活的骨骼肌可通过从细胞外束缚中快速释放HGF并随后呈递给受体c-met来触发激活。已经表明,HGF的释放依赖于钙钙调蛋白的形成以及卫星细胞和/或肌纤维中NO自由基的产生,以响应机械扰动,并取决于随后基质金属蛋白酶(MMP)活性的上调。这些结果表明激活机制是一系列事件,包括钙离子流入,钙钙调蛋白形成,NO合酶激活,NO自由基产生,MMP激活,HGF释放以及与c-met的结合。更好地了解卫星细胞激活的“力学生物学”对于设计程序可以至关重要,该程序可以增强肉类动物农业以及神经肌肉疾病和人类衰老中的肌肉生长和修复活动。

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