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PBX同源结构域蛋白指导肌分化蛋白活性以促进快肌分化。

Pbx homeodomain proteins direct Myod activity to promote fast-muscle differentiation.

作者信息

Maves Lisa, Waskiewicz Andrew Jan, Paul Biswajit, Cao Yi, Tyler Ashlee, Moens Cecilia B, Tapscott Stephen J

机构信息

Division of Human Biology, Fred Hutchinson Cancer Research Center, Seattle, Washington 98109, USA.

出版信息

Development. 2007 Sep;134(18):3371-82. doi: 10.1242/dev.003905. Epub 2007 Aug 15.

Abstract

The basic helix-loop-helix (bHLH) transcription factor Myod directly regulates gene expression throughout the program of skeletal muscle differentiation. It is not known how a Myod-driven myogenic program is modulated to achieve muscle fiber-type-specific gene expression. Pbx homeodomain proteins mark promoters of a subset of Myod target genes, including myogenin (Myog); thus, Pbx proteins might modulate the program of myogenesis driven by Myod. By inhibiting Pbx function in zebrafish embryos, we show that Pbx proteins are required in order for Myod to induce the expression of a subset of muscle genes in the somites. In the absence of Pbx function, expression of myog and of fast-muscle genes is inhibited, whereas slow-muscle gene expression appears normal. By knocking down Pbx or Myod function in combination with another bHLH myogenic factor, Myf5, we show that Pbx is required for Myod to regulate fast-muscle, but not slow-muscle, development. Furthermore, we show that Sonic hedgehog requires Myod in order to induce both fast- and slow-muscle markers but requires Pbx only to induce fast-muscle markers. Our results reveal that Pbx proteins modulate Myod activity to drive fast-muscle gene expression, thus showing that homeodomain proteins can direct bHLH proteins to establish a specific cell-type identity.

摘要

基本螺旋-环-螺旋(bHLH)转录因子Myod在骨骼肌分化的整个过程中直接调控基因表达。目前尚不清楚由Myod驱动的成肌程序是如何被调节以实现肌肉纤维类型特异性基因表达的。Pbx同源域蛋白标记了Myod靶基因子集的启动子,包括肌细胞生成素(Myog);因此,Pbx蛋白可能会调节由Myod驱动的成肌程序。通过抑制斑马鱼胚胎中的Pbx功能,我们发现Pbx蛋白是Myod在体节中诱导一部分肌肉基因表达所必需的。在缺乏Pbx功能的情况下,myog和快肌基因的表达受到抑制,而慢肌基因表达看起来正常。通过与另一个bHLH成肌因子Myf5联合敲低Pbx或Myod功能,我们发现Pbx是Myod调节快肌而非慢肌发育所必需的。此外,我们发现音猬因子(Sonic hedgehog)诱导快肌和慢肌标记物都需要Myod,但仅诱导快肌标记物需要Pbx。我们的结果表明,Pbx蛋白调节Myod活性以驱动快肌基因表达,从而表明同源域蛋白可以指导bHLH蛋白建立特定的细胞类型特征。

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