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Residual pluripotency is required for inductive germ cell segregation

机译:诱导胚细胞分离需要残留多能性

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摘要

Fine‐tuned dissolution of pluripotency is critical for proper cell differentiation. Here we show that the mesodermal transcription factor, T, globally affects the properties of pluripotency through binding to Oct4 and to the loci of other pluripotency regulators. Strikingly, lower T levels coordinately affect naïve pluripotency, thereby directly activating the germ cell differentiation program, in contrast to the induction of germ cell fate of primed models. Contrary to the effect of lower T levels, higher T levels more severely affect the pluripotency state, concomitantly enhancing the somatic differentiation program and repressing the germ cell differentiation program. Consistent with such in vitro findings, nascent germ cells in vivo are detected in the region of lower T levels at the posterior primitive streak. Furthermore, T and core pluripotency regulators co‐localize at the loci of multiple germ cell determinants responsible for germ cell development. In conclusion, our findings indicate that residual pluripotency establishes the earliest and fundamental regulatory mechanism for inductive germline segregation from somatic lineages.
机译:多能性的微调溶解对于适当的细胞分化至关重要。在这里,我们表明,中胚层转录因子T全球通过结合到OCT4和其他多能性调节剂的基因座来影响多能性的性质。尖锐的,较低的T级别坐标,影响幼稚多能性,从而直接激活生殖细胞分化计划,与灌注模型的胚芽细胞命运诱导相反。与较低的T水平的影响相反,较高的T级别更严重地影响多能性状态,同时增强体细胞分化计划并压制生殖细胞分化计划。与这种体外发现一致,在后基原始条纹下的下T水平的区域中检测到体内的新生胚芽细胞。此外,T和核心多能调节剂在负责生殖细胞发育的多种生殖细胞决定簇的基因座上共定。总之,我们的研究结果表明,残留多能性为从躯体谱系中的归纳种系偏见建立了最早和最基本的监管机制。

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