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Regulatory role of Klf5 in early mouse development and in embryonic stem cells.

机译:Klf5在小鼠早期发育和胚胎干细胞中的调节作用。

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Pluripotency and self-renewal of embryonic stem cells (ESCs) are maintained by regulatory mechanisms, based on a sophisticated network of transcription factors. Recently, a growing body of evidence has indicated that Klf5, a transcription factor highly expressed in mouse ESCs and during the early phases of mouse development, plays a crucial role in maintaining ESC self-renewal and pluripotency, in governing ESC fate decisions and proper development of blastocyst in vivo. Indeed, Klf5-null mice show developmental defects at blastocyst stage, due to the defective establishment of the inner cell mass. Moreover, Klf5 knockdown in ESCs results in the loss of undifferentiated phenotype, whereas its ectopic expression is sufficient to maintain ESC in the undifferentiated state, even in the absence of LIF. Finally, it has been recently reported that Klf5 activates the expression of self-renewal-promoting genes and, simultaneously, it inhibits the expression of differentiation-related genes. Here, we discuss the functional role of Klf5 in the control on ESC self-renewal and pluripotency and its integration in the core transcriptional network governing ESC state.
机译:胚胎干细胞(ESC)的多能性和自我更新通过转录因子复杂网络的调控机制来维持。最近,越来越多的证据表明,Klf5(一种在小鼠ESC中以及在小鼠发育的早期阶段高表达的转录因子)在维持ESC的自我更新和多能性,控制ESC的命运决定和正常发育中起着至关重要的作用。体内的胚泡。实际上,由于内部细胞团的缺陷,Klf5-null小鼠在胚泡期显示出发育缺陷。此外,ESC中的Klf5敲低导致未分化表型的丧失,而其异位表达足以将ESC维持在未分化状态,即使在没有LIF的情况下也是如此。最后,最近有报道称Klf5激活自我更新促进基因的表达,同时抑制分化相关基因的表达。在这里,我们讨论了Klf5在调控ESC自我更新和多能性中的功能性作用及其在调控ESC状态的核心转录网络中的整合。

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