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Enhanced telomere rejuvenation in pluripotent cells reprogrammed via nuclear transfer relative to induced pluripotent stem cells

机译:通过相对于诱导多能干细胞通过核转移重新编程的多能细胞中增强的端粒恢复剂

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摘要

Although somatic cell nuclear transfer (SCNT) and induction of pluripotency (to form iPSCs) are both recognized reprogramming methods, there has been relatively little comparative analysis of the resulting pluripotent cells. Here, we examine the capacity of these two reprogramming approaches to rejuvenate telomeres using late-generation telomerase-deficient (Terc-/-) mice that exhibit telomere dysfunction and premature aging. We found that embryonic stem cells established from Terc-/- SCNT embryos (Terc-/- ntESCs) have greater differentiation potential and self-renewal capacity than Terc-/- iPSCs. Remarkably, SCNT results in extensive telomere lengthening in cloned embryos and improved telomere capping function in the established Terc-/- ntESCs. In addition, mitochondrial function is severely impaired in Terc-/- iPSCs and their differentiated derivatives but significantly improved in Terc-/- ntESCs. Thus, our results suggest that SCNT-mediated reprogramming mitigates telomere dysfunction and mitochondrial defects to a greater extent than iPSC-based reprogramming. Understanding the basis of this differential could help optimize reprogramming strategies.
机译:尽管体细胞核转移(SCNT)和多能性(形成IPSC)的诱导既公认的重编程方法,但对所得多能细胞的比较分析相对较少。在这里,我们使用表现出端粒功能障碍和过早衰老的晚期端粒酶缺陷(TERC - / - )小鼠来检查这两种重新编程方法的能力。我们发现从Terc - / - SCNT胚胎(TERC - / - NTESCs)建立的胚胎干细胞比Terc - / - IPSCs具有更大的分化潜力和自我更新能力。值得注意的是,SCNT导致克隆胚胎中的广泛的端粒延长,并在已建立的TERC - / - NTESC中改进了端粒封端功能。此外,在TERC - / - IPSCS及其差异化衍生物中严重受损,但在TERC - / - NTESCS中严重受损。因此,我们的结果表明,SCNT介导的重编程减轻了超越功能障碍和线粒体缺陷的程度,而不是基于IPSC的重新编程。了解这种差异的基础可以帮助优化重编程策略。

著录项

  • 来源
    《Cell stem cell》 |2014年第1期|共13页
  • 作者单位

    College of Biological Sciences China Agricultural University Beijing 100094 China National;

    National Institute of Biological Sciences NIBS Beijing 102206 China;

    College of Biological Sciences China Agricultural University Beijing 100094 China National;

    National Institute of Biological Sciences NIBS Beijing 102206 China;

    National Institute of Biological Sciences NIBS Beijing 102206 China;

    College of Biological Sciences China Agricultural University Beijing 100094 China National;

    Institute of Zoology Chinese Academy of Sciences Beijing 100101 China;

    National Institute of Biological Sciences NIBS Beijing 102206 China;

    National Institute of Biological Sciences NIBS Beijing 102206 China;

    Leibniz Institute for Age Research Fritz Lipmann Institute Jena 07745 Germany;

    Institute of Aging Research School of Medicine Hangzhou Normal University Hangzhou 310036 China;

    National Institute of Biological Sciences NIBS Beijing 102206 China School of Life Sciences and;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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