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Myoblasts Derived From Normal hESCs and Dystrophic hiPSCs Efficiently Fuse With Existing Muscle Fibers Following Transplantation

机译:正常人胚胎干细胞和营养不良的hiPSC衍生的成肌细胞与移植后的现有肌纤维有效融合

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摘要

Human embryonic stem cells (hESCs) and human-induced pluripotent stem cells (hiPSCs) have an endless self-renewal capacity and can theoretically differentiate into all types of lineages. They thus represent an unlimited source of cells for therapies of regenerative diseases, such as Duchenne muscular dystrophy (DMD), and for tissue repair in specific medical fields. However, at the moment, the low number of efficient specific lineage differentiation protocols compromises their use in regenerative medicine. We developed a two-step procedure to differentiate hESCs and dystrophic hiPSCs in myogenic cells. The first step was a culture in a myogenic medium and the second step an infection with an adenovirus expressing the myogenic master gene MyoD. Following infection, the cells expressed several myogenic markers and formed abundant multinucleated myotubes in vitro. When transplanted in the muscle of Rag/mdx mice, these cells participated in muscle regeneration by fusing very well with existing muscle fibers. Our findings provide an effective method that will permit to use hESCs or hiPSCs for preclinical studies in muscle repair.
机译:人类胚胎干细胞(hESC)和人类诱导的多能干细胞(hiPSC)具有无限的自我更新能力,并且在理论上可以分化为所有类型的谱系。因此,它们代表了用于再生疾病(例如杜兴氏肌营养不良症(DMD))以及特定医学领域中组织修复的细胞的无限来源。然而,目前,有效的特定谱系分化方案的数量较少,损害了它们在再生医学中的应用。我们开发了两步程序来区分成肌细胞中的hESC和营养不良型hiPSC。第一步是在肌原性培养基中培养,第二步是用表达肌原性主基因MyoD的腺病毒感染。感染后,细胞表达几种肌原性标志物,并在体外形成丰富的多核肌管。当移植到Rag / mdx小鼠的肌肉中时,这些细胞通过与现有的肌肉纤维很好地融合来参与肌肉再生。我们的发现提供了一种有效的方法,可以将hESCs或hiPSCs用于肌肉修复的临床前研究。

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