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评估 Pax3/Pax7 诱导的胚胎干细胞衍生祖细胞移植后的成肌干细胞隔室。

Assessment of the myogenic stem cell compartment following transplantation of Pax3/Pax7-induced embryonic stem cell-derived progenitors.

机构信息

Lillehei Heart Institute, Department of Medicine, University of Minnesota, Minneapolis, Minnesota 55455, USA.

出版信息

Stem Cells. 2011 May;29(5):777-90. doi: 10.1002/stem.625.

Abstract

An effective long-term cell therapy for skeletal muscle regeneration requires donor contribution to both muscle fibers and the muscle stem cell pool. Although satellite cells have these abilities, their therapeutic potential so far has been limited due to their scarcity in adult muscle. Myogenic progenitors obtained from Pax3-engineered mouse embryonic stem (ES) cells have the ability to generate myofibers and to improve the contractility of transplanted muscles in vivo, however, whether these cells contribute to the muscle stem cell pool and are able to self-renew in vivo are still unknown. Here, we addressed this question by investigating the ability of Pax3, which plays a critical role in embryonic muscle formation, and Pax7, which is important for maintenance of the muscle satellite cell pool, to promote the derivation of self-renewing functional myogenic progenitors from ES cells. We show that Pax7, like Pax3, can drive the expansion of an ES-derived myogenic progenitor with significant muscle regenerative potential. We further demonstrate that a fraction of transplanted cells remains mononuclear, and displays key features of skeletal muscle stem cells, including satellite cell localization, response to reinjury, and contribution to muscle regeneration in secondary transplantation assays. The ability to engraft, self-renew, and respond to injury provide foundation for the future therapeutic application of ES-derived myogenic progenitors in muscle disorders.

摘要

一种有效的骨骼肌再生长期细胞疗法需要供体对肌纤维和肌肉干细胞池都有贡献。尽管卫星细胞具有这些能力,但由于其在成年肌肉中的稀缺性,它们的治疗潜力迄今为止一直受到限制。从 Pax3 工程化的小鼠胚胎干细胞(ES 细胞)中获得的成肌祖细胞具有生成肌纤维的能力,并能改善体内移植肌肉的收缩性,然而,这些细胞是否能对肌肉干细胞池作出贡献并能在体内自我更新仍然未知。在这里,我们通过研究在胚胎肌肉形成中起关键作用的 Pax3 和对肌肉卫星细胞池的维持很重要的 Pax7,来探讨它们促进 ES 细胞来源的自我更新功能成肌祖细胞的衍生的能力。我们表明,Pax7 像 Pax3 一样,可以驱动具有显著肌肉再生潜力的 ES 细胞衍生的成肌祖细胞的扩增。我们进一步证明,一部分移植细胞保持单核状态,并显示出骨骼肌干细胞的关键特征,包括卫星细胞定位、对再损伤的反应以及在二次移植实验中对肌肉再生的贡献。植入、自我更新和对损伤的反应的能力为 ES 细胞来源的成肌祖细胞在肌肉疾病中的未来治疗应用提供了基础。

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