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A Signaling Principle for the Specification of the Germ Cell Lineage in Mice

机译:小鼠生殖细胞谱系规范的信号传导原理

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Specification of the germ cell lineage is vital to development and heredity. In mice, the germ cell fate is induced in pluripotent epiblast cells by signaling molecules, yet the underlying mechanism remains unknown. Here we demonstrate that germ cell fate in the epiblast is a direct consequence of Bmp4 signaling from the extraembryonic ectoderm (ExE), which is antagonized by the anterior visceral endoderm (AVE). Strikingly, Bmp8b from the ExE restricts AVE development, thereby contributing to Bmp4 signaling. Furthermore, Wnt3 in the epiblast ensures its responsiveness to Bmp4. Serum-free, defined cultures revealed that, in response to Bmp4, competent epiblast cells uniformly expressed key transcriptional regulators Blimp1 and Prdm14 and acquired germ-cell properties, including genome-wide epigenetic reprogramming, in an orderly fashion. Notably, the induced cells contributed to both spermatogenesis and fertility of offspring. By identifying a signaling principle in germ cell specification, our study establishes a robust strategy for reconstituting the mammalian germ cell lineage in vitro.
机译:生殖细胞谱系的规范对于发育和遗传至关重要。在小鼠中,多能表皮细胞通过信号分子诱导生殖细胞命运,但其潜在机制尚不清楚。在这里,我们证明上皮细胞的生殖细胞命运是胚外外胚层(ExE)受到Bmp4信号传导的直接结果,而胚前内胚层(AVE)拮抗了Bmp4信号。引人注目的是,来自ExE的Bmp8b限制了AVE的发展,从而促进了Bmp4信令。此外,上皮细胞中的Wnt3确保了其对Bmp4的反应能力。不含血清的明确培养物显示,响应Bmp4,感受态的成骨细胞均匀表达关键的转录调节因子Blimp1和Prdm14,并获得了生殖细胞特性,包括全基因组表观遗传重编程。值得注意的是,诱导的细胞有助于子代的精子发生和繁殖。通过确定生殖细胞规范中的信号传导原理,我们的研究建立了一种在体外重建哺乳动物生殖细胞谱系的可靠策略。

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