首页> 外文期刊>Frontiers in Physiology >Overexpression of Striated Muscle Activator of Rho Signaling (STARS) Increases C2C12 Skeletal Muscle Cell Differentiation
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Overexpression of Striated Muscle Activator of Rho Signaling (STARS) Increases C2C12 Skeletal Muscle Cell Differentiation

机译:Rho信号(STARS)的横纹肌激活剂的过表达增加C2C12骨骼肌细胞分化

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Background: Skeletal muscle growth and regeneration depend on the activation of satellite cells, which leads to myocyte proliferation, differentiation and fusion with existing muscle fibers. Skeletal muscle cell proliferation and differentiation are tightly coordinated by a continuum of molecular signaling pathways. The striated muscle activator of Rho signaling (STARS) is an actin binding protein that regulates the transcription of genes involved in muscle cell growth, structure and function via the stimulation of actin polymerization and activation of serum-response factor (SRF) signaling. STARS mediates cell proliferation in smooth and cardiac muscle models; however, whether STARS overexpression enhances cell proliferation and differentiation has not been investigated in skeletal muscle cells. Results: We demonstrate for the first time that STARS overexpression enhances differentiation but not proliferation in C2C12 mouse skeletal muscle cells. Increased differentiation was associated with an increase in the gene levels of the myogenic differentiation markers Ckm, Ckmt2 and Myh4 , the differentiation factor Igf2 and the myogenic regulatory factors (MRFs) Myf5 and Myf6 . Exposing C2C12 cells to CCG-1423, a pharmacological inhibitor of SRF preventing the nuclear translocation of its co-factor MRTF-A, had no effect on myotube differentiation rate, suggesting that STARS regulates differentiation via a MRTF-A independent mechanism. Conclusion: These findings position STARS as an important regulator of skeletal muscle growth and regeneration.
机译:背景:骨骼肌的生长和再生取决于卫星细胞的激活,这会导致肌细胞增殖,分化以及与现有肌纤维的融合。骨骼肌细胞的增殖和分化通过连续的分子信号通路紧密协调。 Rho信号的横纹肌激活剂(STARS)是一种肌动蛋白结合蛋白,可通过刺激肌动蛋白聚合和激活血清反应因子(SRF)信号来调节参与肌肉细胞生长,结构和功能的基因的转录。 STARS在平滑肌和心肌模型中介导细胞增殖;但是,尚未在骨骼肌细胞中研究STARS是否过表达增强细胞增殖和分化。结果:我们首次证明STARS过表达可增强C2C12小鼠骨骼肌细胞的分化能力,但不增强其增殖能力。分化增加与肌源性分化标志物Ckm,Ckmt2和Myh4,分化因子Igf2以及肌源性调节因子(MRF)Myf5和Myf6的基因水平升高相关。将C2C12细胞暴露于CCF-1423(一种SRF的药理抑制剂,可防止其辅因子MRTF-A的核转位)对肌管分化率没有影响,这表明STARS通过MRTF-A独立机制调节分化。结论:这些发现将STARS定位为骨骼肌生长和再生的重要调节剂。

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