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The p38 MAPK signaling pathway: a major regulator of skeletal muscle development.

机译:p38 MAPK信号传导途径:骨骼肌发育的主要调节剂。

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摘要

Skeletal muscle development is regulated by extracellular growth factors that transmit largely unknown signals into the cell affecting the muscle-transcription program. One intracellular signaling pathway activated during the differentiation of myogenic cell lines is p38 mitogen-activated protein kinase (MAPK). As a result of modifying the activity of p38 in myoblasts, the pathway proved essential for the expression of muscle-specific genes. P38 affects the activities of transcription factors from the MyoD and MEF2 families and participates in the remodeling of chromatin at specific muscle-regulatory regions. P38 cooperates with the myogenic transcription factors in the activation of a subset of late-transcribed genes, hence contributing to the temporal expression of genes during differentiation. Recent developmental studies with mouse and Xenopus embryos, substantiated and further extended the essential role of p38 in myogenesis. Evidence exists supporting the crucial role for p38 signaling in activating MEF2 transcription factors during somite development in mice. In Xenopus, p38 signaling was shown to be needed for the early expression of Myf5 and for the expression of several muscle structural genes. The emerging data indicate that p38 participates in several stages of the myogenic program.
机译:骨骼肌的发育受细胞外生长因子的调节,该因子将很大程度上未知的信号传递到影响肌肉转录程序的细胞中。在成肌细胞系分化过程中激活的一种细胞内信号传导途径是p38丝裂原激活的蛋白激酶(MAPK)。由于修饰了成肌细胞中p38的活性,该途径被证明对表达肌肉特异性基因至关重要。 P38影响来自MyoD和MEF2家族的转录因子的活性,并参与特定肌肉调节区域的染色质重塑。 P38与肌原性转录因子协同作用,激活了一部分后期转录的基因,从而在分化过程中促进了基因的瞬时表达。最近关于小鼠和非洲爪蟾胚胎的发育研究证实并进一步扩展了p38在肌发生中的重要作用。有证据支持p38信号在小鼠的somite发育过程中激活MEF2转录因子中的关键作用。在非洲爪蟾中,p38信号显示出Myf5的早期表达和一些肌肉结构基因的表达是必需的。新出现的数据表明,p38参与了肌源性程序的多个阶段。

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