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Efficient derivation and inducible differentiation of expandable skeletal myogenic cells from human ES and patient-specific iPS cells

机译:从人胚胎干细胞和患者特异性iPS细胞有效衍生和诱导分化可扩展骨骼肌细胞

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摘要

keletal muscle is the most abundant human tissue; therefore, an unlimited availability of myogenic cells has applications in regenerative medicine and drug development. Here we detail a protocol to derive myogenic cells from human embryonic stem (ESES) and induced pluripotent stem (iPSPS) cells, and we also provide evidence for its extension to human iPSPS cells cultured without feeder cells. The procedure, which does not require the generation of embryoid bodies or prospective cell isolation, entails four stages with different culture densities, media and surface coating. Pluripotent stem cells are disaggregated to single cells and then differentiated into expandable cells resembling human mesoangioblasts. Subsequently, transient Myod1 induction efficiently drives myogenic differentiation into multinucleated myotubes. Cells derived from patients with muscular dystrophy and differentiated using this protocol have been genetically corrected, and they were proven to have therapeutic potential in dystrophic mice. Thus, this platform has been demonstrated to be amenable to gene and cell therapy, and it could be extended to muscle tissue engineering and disease modeling.
机译:骨骼肌是人体最丰富的组织;因此,无限数量的成肌细胞可用于再生医学和药物开发。在这里,我们详细介绍了从人类胚胎干细胞(ESES)和诱导多能干细胞(iPSPS)衍生成肌细胞的方案,并且我们还提供了其扩展至无饲养细胞培养的人iPSPS细胞的证据。该过程不需要生成胚状体或不进行前瞻性细胞分离,需要四个阶段,每个阶段具有不同的培养密度,培养基和表面包被。多能干细胞分解为单个细胞,然后分化为类似于人中成血管细胞的可扩展细胞。随后,短暂的Myod1诱导有效地驱动成肌分化为多核肌管。从肌营养不良患者获得的细胞,并使用该方案分化后,已进行了遗传学校正,并被证明对营养不良的小鼠具有治疗潜力。因此,已经证明该平台适用于基因和细胞疗法,并且可以扩展到肌肉组织工程和疾病建模。

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