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Id3 Is a Direct Transcriptional Target of Pax7 in Quiescent Satellite Cells

机译:Id3是Pax7在静止卫星细胞中的直接转录靶标。

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Pax7 is a key regulator of skeletal muscle stem cells and is required along with Pax3 to generate skeletal muscle precursors. We have identified a collection of genes induced by either Pax3 or Pax7 in C2C12 muscle cells. Two notable Pax3/7 targets are the inhibitory helix-loop-helix (HLH) proteins inhibitor of DNA binding (Id) 2 and Id3, both of which are coordinately expressed with Pax7 in quiescent satellite cells and are induced in quiescent C2C12 myogenic cells after ectopic expression of either Pax3 or Pax7. Ectopic Pax7 activates expression of a luciferase reporter driven by the Id3 promoter, and maximal induction of this reporter requires a conserved Pax7 binding site located upstream of the Id3 gene. Chromatin immunoprecipitation indicated that Pax7 is bound upstream of the Id3 promoter in quiescent satellite cells. In addition, short hairpin RNA-mediated knockdown of Pax7 expression in cultured satellite cells coordinately decreased both Id2 and Id3 expression. Together, these findings indicate that Id3 is a direct transcriptional target for Pax7 in quiescent satellite cells, and they suggest that Pax7 acts to block premature differentiation of quiescent satellite cells by inducing the expression of Id2 and Id3, which in turn may act to block either the precocious induction of myogenic basic (b)HLH proteins, the activity of myogenic bHLH proteins, or both.
机译:Pax7是骨骼肌干细胞的关键调节剂,与Pax3一起需要以生成骨骼肌前体。我们已经确定了由Pax3或Pax7诱导的C2C12肌肉细胞中的基因集合。两个著名的Pax3 / 7靶标是DNA结合(Id)2和Id3的抑制性螺旋-环-螺旋(HLH)蛋白抑制剂,两者均在静止的卫星细胞中与Pax7协同表达,并在静止的C2C12成肌细胞中被诱导Pax3或Pax7的异位表达。异位Pax7激活由Id3启动子驱动的萤光素酶报告基因的表达,并且对该报告基因的最大诱导需要位于Id3基因上游的保守Pax7结合位点。染色质的免疫沉淀表明,Pax7结合在静止卫星细胞中Id3启动子的上游。此外,在培养的卫星细胞中短发夹RNA介导的Pax7表达的敲低协同降低了Id2和Id3的表达。在一起,这些发现表明,Id3是静止卫星细胞中Pax7的直接转录靶标,并且它们表明Pax7通过诱导Id2和Id3的表达来阻止静止卫星细胞的过早分化,进而可能阻止其中之一成肌碱性(b)HLH蛋白的早熟诱导,成肌bHLH蛋白的活性或两者兼有。

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