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首页> 外文期刊>Molecular and Cellular Biology >Increase in p202 Expression during Skeletal Muscle Differentiation: Inhibition of MyoD Protein Expression and Activity by p202
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Increase in p202 Expression during Skeletal Muscle Differentiation: Inhibition of MyoD Protein Expression and Activity by p202

机译:骨骼肌分化过程中p202表达的增加:p202对MyoD蛋白表达和活性的抑制

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摘要

p202 is a primarily nuclear, interferon-inducible murine protein that is encoded by the Ifi 202 gene. Overexpression of p202 in transfected cells retards cell proliferation. p202 modulates the pattern of gene expression by inhibiting the activity of various transcription factors including NF-κB, c-Fos, c-Jun, E2F-1, and p53. Here we report that p202 was constitutively expressed in mouse skeletal muscle and that the levels of 202 RNA and p202 greatly increased during the differentiation of cultured C2C12 myoblasts to myotubes. When overexpressed in transfected myoblasts, p202 inhibited the expression of one muscle protein (MyoD) without affecting the expression of a second one (myogenin). Thus, the decrease in the level of MyoD (but not of myogenin) during muscle differentiation may be the consequence of the increase in p202 level. Overexpressed p202 also inhibited the transcriptional activity of both MyoD and myogenin. This inhibition was correlated with an interaction of p202 with both proteins, as well as the inhibition by p202 of the sequence-specific binding of both proteins to DNA. This inhibition of the expression of MyoD and of the transcriptional activity of MyoD and myogenin may account for the inhibition of the induction of myoblast differentiation by premature overexpression of p202.
机译:p202是一种主要的核干扰素诱导型鼠蛋白,由 Ifi 202 基因编码。 p202在转染细胞中的过表达可抑制细胞增殖。 p202通过抑制各种转录因子(包括NF-κB,c-Fos,c-Jun,E2F-1和p53)的活性来调节基因表达模式。在这里,我们报道p202在小鼠骨骼肌中组成性表达,在将C2C12成肌细胞分化为肌管的过程中,202 RNA和p202的水平大大增加。当在转染的成肌细胞中过度表达时,p202会抑制一种肌肉蛋白(MyoD)的表达,而不会影响另一种肌肉蛋白(myogenin)的表达。因此,在肌肉分化过程中,MyoD(而非肌生成素)水平的降低可能是p202水平升高的结果。过表达的p202也抑制了MyoD和肌生成素的转录活性。这种抑制与p202与两种蛋白质的相互作用以及p202对两种蛋白质与DNA的序列特异性结合的抑制相关。这种对MyoD表达以及MyoD和肌生成素的转录活性的抑制作用可能是由于过早表达p202而抑制了成肌细胞分化的原因。

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