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The molecular mechanism of induced pluripotency: A two-stage switch

机译:诱导多能性的分子机制:两阶段转换

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摘要

Pluripotent stem cells are basic cells with an indefinite self-renewal capacity and the potential to generate all the cell types of the three germinal layers. So far, the major source for pluripotent stem cells is the inner cell mass of the blastocysts: embryonic stem (ES) cells. Potential clinical application of ES cells is faced with many practical and ethical concerns. So, a major breakthrough was achieved in 2006, when it was shown that pluripotent stem cells could be obtained by transducing mouse embryonic and adult fibroblasts with a limited set of defined transcription factors. These reprogrammed cells, named induced pluripotent stem (iPS) cells, resembled ES cells in many of their characteristics. Since this initial study, iPS cell research has taken an incredible flight, and to date iPS cells have been generated from cells from several species using different sets of reprogramming factors. Given the potential to generate patient-specific cell populations without the need for human embryonic cells, iPS cell technology has been received with great excitement by research and medical communities. However, many questions regarding the actual molecular process of induced reprogramming remain unanswered and need to be addressed before iPS cells can go to the clinic. In this review, we start by summarizing recent advances in iPS cell research and inventory the hurdles that still need to be taken before safe clinical application. Our major aim, however, is to review the available data on the molecular processes underlying pluripotency reprogramming and present a two-stage switch model.
机译:多能干细胞是具有无限自我更新能力并具有产生三个生发层所有细胞类型的潜力的基本细胞。到目前为止,多能干细胞的主要来源是胚泡的内部细胞团:胚胎干(ES)细胞。 ES细胞的潜在临床应用面临许多实际和伦理问题。因此,在2006年取得了一项重大突破,当时证明可以通过转导具有有限定义的转录因子集的小鼠胚胎和成年成纤维细胞来获得多能干细胞。这些重新编程的细胞,称为诱导多能干(iPS)细胞,在许多方面与ES细胞相似。自从这项初步研究以来,iPS细胞研究取得了令人难以置信的飞跃,迄今为止,iPS细胞已经使用不同的重编程因子集从数个物种的细胞中产生。鉴于无需人胚胎细胞即可产生患者特异性细胞群的潜力,研究和医学界非常兴奋地接受了iPS细胞技术。但是,关于诱导的重新编程的实际分子过程的许多问题仍然没有答案,需要在iPS细胞进入临床之前解决。在本文中,我们首先总结了iPS细胞研究的最新进展,并概述了安全临床应用之前仍需克服的障碍。但是,我们的主要目的是审查有关多能性重编程基础上的分子过程的可用数据,并提出一个两阶段转换模型。

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