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The possible role of Myosin light chain in myoblast proliferation

机译:肌球蛋白轻链在成肌细胞增殖中的可能作用

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摘要

Skeletal muscles have the potential to regenerate by activation of quiescent satellite cells, however, the molecular signature that governs satellite cells during muscle regeneration is not well defined. Myosin light chains (Myls) are sarcomere-related proteins as traditional regulator of muscle contraction. In this report, we studied the possible role of Myl in the proliferation of skeletal muscle-derived myoblasts. Compared to diaphragm-derived myoblasts, the extraocular muscle-derived myoblasts with lower levels of Myl proliferated faster, maintained a longer proliferation phase, and formed more final myotubes. It was found that blockading Myl with anti-Myl antibody or knockdown of Myll by siRNA targeted against Myll could enhance the myoblast proliferation and delay the differentiation of myoblasts. Our results suggested that Myl, likely Myll, can negatively affect myoblast proliferation by facilitating myoblast withdrawal from cell cycle and differentiation.
机译:骨骼肌具有通过激活静止的卫星细胞进行再生的潜力,但是,在肌肉再生过程中控制卫星细胞的分子标记尚不明确。肌球蛋白轻链(Myls)是与肌节相关的蛋白质,是传统的肌肉收缩调节剂。在本报告中,我们研究了Myl在骨骼肌来源的成肌细胞增殖中的可能作用。与diaphragm肌来源的成肌细胞相比,Myl含量较低的眼外肌来源的成肌细胞增殖更快,维持更长的增殖期并形成更多的最终肌管。发现用抗Myl抗体阻断Myl或通过靶向Myll的siRNA敲低Myll可以增强成肌细胞增殖并延迟成肌细胞的分化。我们的结果表明,Myl(可能是Myll)可以通过促进成肌细胞退出细胞周期和分化而对成肌细胞增殖产生负面影响。

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