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Switching on pluripotency: a perspective on the biological requirement of Nanog

机译:开启多能性:Nanog生物学需求的视角

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摘要

Pluripotency is a transient cellular state during early development which can be recreated in vitro by direct reprogramming. The molecular mechanisms driving entry into and exit from the pluripotent state are the subject of intense research interest. Here, we review the role of the homeodomain-containing transcription factor Nanog in mammalian embryology and induced pluripotency. Nanog was originally thought to be confined to the maintenance of pluripotency, but recent insights from genetic studies uncovered a new biological function. Embryonic stem cells deficient in Nanog alleles are more prone to differentiate but do not lose pluripotency per se. Instead, Nanog is transiently required for the specification of the naive pluripotent epiblast and development of primordial germ cells. Nanog is also essential to finalize somatic cell reprogramming during induction of pluripotency. We propose that this unique transcription factor acts as a molecular switch to turn on the naive pluripotent programme in mammalian cells. In this context, the capacity of Nanog to resist differentiation can be regarded as recapitulation of effects normally associated with the specification of pluripotency. Pertinent questions are how Nanog specifies naive pluripotency and whether this mechanism is evolutionarily conserved.
机译:多能性是早期发育过程中的瞬时细胞状态,可以通过直接重编程在体外重建。驱动进入和离开多能态的分子机制是研究热点。在这里,我们综述了含同源结构域的转录因子Nanog在哺乳动物胚胎学和诱导多能性中的作用。 Nanog最初被认为仅限于维持多能性,但是遗传研究的最新见解揭示了一种新的生物学功能。缺乏Nanog等位基因的胚胎干细胞更易于分化,但本身不会丧失多能性。取而代之的是,Nanog是天真多能表皮细胞的规范和原始生殖细胞发育的短暂需要。在诱导多能性过程中,Nanog对完成体细胞重编程也至关重要。我们提出,这种独特的转录因子充当打开哺乳动物细胞中幼稚多能程序的分子开关。在这种情况下,Nanog抵抗分化的能力可被视为通常与多能性规范相关的效应的概括。有关的问题是,Nanog如何指定天真的多能性,以及该机制是否在进化上是保守的。

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