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首页> 外文期刊>Stem Cell Reports >Direct Reprogramming of Mouse Fibroblasts into Functional Skeletal Muscle Progenitors
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Direct Reprogramming of Mouse Fibroblasts into Functional Skeletal Muscle Progenitors

机译:将小鼠成纤维细胞直接重编程为功能性骨骼肌祖细胞

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Summary Skeletal muscle harbors quiescent stem cells termed satellite cells and proliferative progenitors termed myoblasts, which play pivotal roles during muscle regeneration. However, current technology does not allow permanent capture of these cell populations in?vitro . Here, we show that ectopic expression of the myogenic transcription factor MyoD, combined with exposure to small molecules, reprograms mouse fibroblasts into expandable induced myogenic progenitor cells (iMPCs). iMPCs express key skeletal muscle stem and progenitor cell markers including Pax7 and Myf5 and give rise to dystrophin-expressing myofibers upon transplantation in vivo . Notably, a subset of transplanted iMPCs maintain Pax7 expression and sustain serial regenerative responses. Similar to satellite cells, iMPCs originate from Pax7+ cells and require Pax7 itself for maintenance. Finally, we show that myogenic progenitor cell lines can be established from muscle tissue following small-molecule exposure alone. This study thus reports on a robust approach to derive expandable myogenic stem/progenitor-like cells from multiple cell types.
机译:小结骨骼肌具有被称为卫星细胞的静止干细胞和被称为成肌细胞的增殖祖细胞,它们在肌肉再生过程中起关键作用。但是,当前技术不允许在体外永久捕获这些细胞群。在这里,我们显示了肌转录因子MyoD的异位表达,并与暴露于小分子的结合,将小鼠成纤维细胞重编程为可扩展的诱导性成肌祖细胞(iMPCs)。 iMPCs表达关键的骨骼肌干和祖细胞标志物,包括Pax7和Myf5,并在体内移植后产生表达肌营养不良蛋白的肌纤维。值得注意的是,移植的iMPC的一个子集可维持Pax7表达并维持系列再生反应。与卫星小区相似,iMPC源自Pax7 + 小区,需要Pax7本身进行维护。最后,我们表明,仅在小分子暴露后,肌肉组织即可建立成肌祖细胞系。因此,这项研究报告了一种从多种细胞类型衍生出可扩展的成肌干/祖细胞样细胞的可靠方法。

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