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Human ES- and iPS-derived myogenic progenitors restore DYSTROPHIN and improve contractility upon transplantation in dystrophic mice

机译:人类ES和iPS衍生的成肌祖细胞在营养不良小鼠移植后可恢复肌张力障碍并改善收缩力

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A major obstacle in the application of cell-based therapies for the treatment of neuromuscular disorders is obtaining the appropriate number of stem/progenitor cells to produce effective engraftment. The use of embryonic stem (ES) or induced pluripotent stem (iPS) cells could overcome this hurdle. However, to date, derivation of engraftable skeletal muscle precursors that can restore muscle function from human pluripotent cells has not been achieved. Here we applied conditional expression of PAX7 in human ES/iPS cells to successfully derive large quantities of myogenic precursors, which, upon transplantation into dystrophic muscle, are able to engraft efficiently, producing abundant human-derived DYSTROPHIN-positive myofibers that exhibit superior strength. Importantly, transplanted cells also seed the muscle satellite cell compartment, and engraftment is present over 11 months posttransplant. This study provides the proof of principle for the derivation of functional skeletal myogenic progenitors from human ES/iPS cells and highlights their potential for future therapeutic application in muscular dystrophies.
机译:应用基于细胞的疗法治疗神经肌肉疾病的主要障碍是获得适当数量的干/祖细胞以产生有效的植入。胚胎干细胞(ES)或诱导多能干细胞(iPS)的使用可以克服这一障碍。然而,迄今为止,尚未实现可从人多能细胞恢复肌肉功能的可植入骨骼肌前体的衍生。在这里,我们应用了PAX7在人ES / iPS细胞中的条件表达,以成功地衍生出大量的成肌前体,这些前体在移植到营养不良的肌肉中后能够有效植入,从而产生出大量的人源性DYSTROPHIN阳性肌纤维,这些肌纤维具有出众的强度。重要的是,移植的细胞也播种了肌肉卫星细胞区,移植后11个月内出现了移入。这项研究提供了从人ES / iPS细胞衍生功能性骨骼肌成肌祖细胞的原理证明,并突出了它们在肌肉营养不良症中未来治疗应用的潜力。

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