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首页> 外文期刊>Molecular human reproduction. >The role of the reprogramming method and pluripotency state in gamete differentiation from patient-specific human pluripotent stem cells
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The role of the reprogramming method and pluripotency state in gamete differentiation from patient-specific human pluripotent stem cells

机译:重编程方法和多能性状态在患者特异性人多能干细胞的配子分化中的作用

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摘要

The derivation of gametes from patient-specific pluripotent stem cells may provide new perspectives for genetic parenthood for patients currently facing sterility. We use current data to assess the gamete differentiation potential of patient-specific pluripotent stem cells and to determine which reprogramming strategy holds the greatest promise for future clinical applications. First, we compare the two best established somatic cell reprogramming strategies: the production of induced pluripotent stem cells (iPSC) and somatic cell nuclear transfer followed by embryonic stem cell derivation (SCNT-ESC). Recent reports have indicated that these stem cells, though displaying a similar pluripotency potential, show important differences at the epigenomic level, which may have repercussions on their applicability. By comparing data on the genetic and epigenetic stability of these cell types during derivation and in-vitro culture, we assess the reprogramming efficiency of both technologies and possible effects on the subsequent differentiation potential of these cells. Moreover, we discuss possible implications of mitochondrial heteroplasmy. We also address the ethical aspects of both cell types, as well as the safety considerations associated with clinical applications using these cells, e.g. the known genomic instability of human PSCs during long-term culture. Secondly, we discuss the role of the stem cell pluripotency state in germ cell differentiation. In mice, success in germ cell development from pluripotent stem cells could only be achieved when starting from a naive state of pluripotency. It remains to be investigated if the naive state is also crucial for germ cell differentiation in human cells and to what extent human naive pluripotency resembles the naive state in mouse.
机译:来自患者特异性多能干细胞的配子的衍生可以为目前面临无菌的患者提供新的遗传患者患者的新视角。我们使用当前数据来评估患者特异性多能干细胞的配子分化潜力,并确定哪些重编程策略对未来的临床应用具有最大的承诺。首先,我们比较两种最佳既定的躯体细胞重编程策略:产生诱导的多能干细胞(IPSC)和体细胞核转移,然后进行胚胎干细胞衍生物(SCNT-ESC)。最近的报道表明,这些干细胞虽然显示了类似的多能性潜力,但表现出上表观形式的重要差异,这可能对其适用性产生影响。通过比较衍生和体外培养过程中这些细胞类型的遗传和表观遗传稳定性的数据,我们评估了两种技术的重编程效率和对随后的这些细胞的分化潜力的影响。此外,我们讨论了线粒体异质的可能影响。我们还解决了两种细胞类型的伦理方面,以及使用这些细胞的临床应用相关的安全考虑,例如,长期培养期间人PSC的已知基因组不稳定性。其次,我们讨论干细胞多能态状态在生殖细胞分化中的作用。在小鼠中,只能在从多能性的幼稚状态开始时从多能干细胞的生殖细胞发育中的成功。如果天真的状态对人体细胞的生殖细胞分化也至关重要,并且在多大程度上是对小鼠中的幼稚状态的影响仍然有待调查。

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