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ErbB3 binding protein-1 (Ebp1) controls proliferation and myogenic differentiation of muscle stem cells

机译:ErbB3结合蛋白1(Ebp1)控制肌肉干细胞的增殖和成肌分化

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摘要

Satellite cells are resident stem cells of skeletal muscle, supplying myoblasts for post-natal muscle growth, hypertrophy and repair. Many regulatory networks control satellite cell function, which includes EGF signalling via the ErbB family of receptors. Here we investigated the role of ErbB3 binding protein-1 (Ebp1) in regulation of myogenic stem cell proliferation and differentiation. Ebp1 is a well-conserved DNA/RNA binding protein that is implicated in cell growth, apoptosis and differentiation in many cell types. Of the two main Ebp1 isoforms, only p48 was expressed in satellite cells and C2C12 myoblasts. Although not present in quiescent satellite cells, p48 was strongly induced during activation, remaining at high levels during proliferation and differentiation. While retroviral-mediated over-expression of Ebp1 had only minor effects, siRNA-mediated Ebp1 knockdown inhibited both proliferation and differentiation of satellite cells and C2C12 myoblasts, with a clear failure of myotube formation. Ebp1-knockdown significantly reduced ErbB3 receptor levels, yet over-expression of ErbB3 in Ebp1 knockdown cells did not rescue differentiation. Ebp1 was also expressed by muscle cells during developmental myogenesis in mouse. Since Ebp1 is well-conserved between mouse and chick, we switched to chick to examine its role in muscle formation. In chick embryo, Ebp1 was expressed in the dermomyotome, and myogenic differentiation of muscle progenitors was inhibited by specific Ebp1 down-regulation using shRNA electroporation. These observations demonstrate a conserved function of Ebp1 in the regulation of embryonic muscle progenitors and adult muscle stem cells, which likely operates independently of ErbB3 signaling.
机译:卫星细胞是骨骼肌的固有干细胞,为成年后的肌肉生长,肥大和修复提供成肌细胞。许多调节网络控制卫星细胞功能,包括通过ErbB受体家族的EGF信号传导。在这里,我们研究了ErbB3结合蛋白1(Ebp1)在调节成肌干细胞增殖和分化中的作用。 Ebp1是一种保守的DNA / RNA结合蛋白,与许多细胞类型的细胞生长,凋亡和分化有关。在两个主要的Ebp1亚型中,仅p48在卫星细胞和C2C12成肌细胞中表达。尽管在静止的卫星细胞中不存在,但p48在激活过程中被强烈诱导,在增殖和分化过程中保持高水平。虽然逆转录病毒介导的Ebp1的过表达仅产生很小的作用,但siRNA介导的Ebp1的敲低同时抑制了卫星细胞和C2C12成肌细胞的增殖和分化,并且肌管形成明显失败。 Ebp1基因敲低显着降低了ErbB3受体水平,但Ebp1基因敲低细胞中ErbB3的过表达不能挽救分化。 Ebp1在小鼠发育性成肌过程中也由肌肉细胞表达。由于Ebp1在小鼠和雏鸡之间非常保守,因此我们选择雏鸡来研究其在肌肉形成中的作用。在雏鸡胚胎中,Ebp1在皮肌切膜刀中表达,并且使用shRNA电穿孔通过特异性Ebp1下调抑制了肌肉祖细胞的肌源性分化。这些观察结果表明,Ebp1在调节胚胎肌肉祖细胞和成年肌肉干细胞方面具有保守功能,而Ebp1可能独立于ErbB3信号传导而运作。

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