首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >Pax3 regulation of FGF signaling affects the progression of embryonic progenitor cells into the myogenic program.
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Pax3 regulation of FGF signaling affects the progression of embryonic progenitor cells into the myogenic program.

机译:FGF信号转导的Pax3调节影响胚胎祖细胞进入成肌程序的进程。

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摘要

Pax3/7-dependent stem cells play an essential role in skeletal muscle development. We now show that Fgfr4 lies genetically downstream from Pax3 and is a direct target. In chromatin immunoprecipitation (ChIP)-on-chip experiments, Pax3 binds to a sequence 3' of the Fgfr4 gene that directs Pax3-dependent expression at sites of myogenesis in transgenic mouse embryos. The activity of this regulatory element is also partially dependent on E-boxes, targets of the myogenic regulatory factors, which are expressed as progenitor cells enter the myogenic program. Other FGF signaling components, notably Sprouty1, are also regulated by Pax3. In vivo manipulation of Sprouty expression reveals that FGF signaling affects the balance between Pax-positive progenitor cells and committed myoblasts. These results provide new insight into the Pax-initiated regulatory network that modulates stem cell maintenance versus tissue differentiation.
机译:Pax3 / 7依赖性干细胞在骨骼肌发育中起重要作用。现在,我们显示Fgfr4在基因上位于Pax3的下游,并且是直接目标。在芯片上的染色质免疫沉淀(ChIP)实验中,Pax3与Fgfr4基因的3'序列结合,该序列指导Pax3依赖性表达在转基因小鼠胚胎的肌生成部位。该调节元件的活性还部分取决于E-box,即成肌调节因子的靶标,其在祖细胞进入成肌程序时表达。其他FGF信号转导成分,特别是Sprouty1,也受Pax3调控。 Sprouty表达的体内操作表明FGF信号传导影响Pax阳性祖细胞和定型成肌细胞之间的平衡。这些结果为Pax启动的调节网络提供了新的见解,该调节网络调节干细胞维持与组织分化之间的关系。

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