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Induced pluripotent stem (iPS) cells as in vitro models of human neurogenetic disorders.

机译:诱导多能干(iPS)细胞作为人类神经遗传性疾病的体外模型。

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摘要

The recent discovery of genomic reprogramming of human somatic cells into induced pluripotent stem cells offers an innovative and relevant approach to the study of human genetic and neurogenetic diseases. By reprogramming somatic cells from patient samples, cell lines can be isolated that self-renew indefinitely and have the potential to develop into multiple different tissue lineages. Additionally, the rapid progress of research on human embryonic stem cells has led to the development of sophisticated in vitro differentiation protocols that closely mimic mammalian development. In particular, there have been significant advances in differentiating human pluripotent stem cells into defined neuronal types. Here, we summarize the experimental approaches employed in the rapidly evolving area of somatic cell reprogramming and the methodologies for differentiating human pluripotent cells into neurons. We also discuss how the availability of patient-specific fibroblasts offers a unique opportunity for studying and modeling the effects of specific gene defects on human neuronal development in vitro and for testing small molecules or other potential therapies for the relevant neurogenetic disorders.
机译:人类体细胞基因组重编程为诱导性多能干细胞的最新发现为研究人类遗传和神经遗传疾病提供了一种创新且相关的方法。通过对患者样品中的体细胞进行重新编程,可以分离出无限期自我更新的细胞系,并具有发展为多种不同组织谱系的潜力。另外,人类胚胎干细胞研究的迅速进展导致了精密模仿哺乳动物发育的复杂体外分化方案的发展。特别地,在将人多能干细胞分化成确定的神经元类型方面取得了重大进展。在这里,我们总结了在体细胞重编程迅速发展的领域中使用的实验方法,以及将人类多能细胞分化为神经元的方法。我们还将讨论患者特异性成纤维细胞的可用性如何为研究和建模特定基因缺陷对体外人类神经元发育的影响以及为相关神经遗传学疾病测试小分子或其他潜在疗法提供独特的机会。

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