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通过BMP4和BMP8B信号通路的协同作用从小鼠上胚层诱导原始生殖细胞

Induction of primordial germ cells from murine epiblasts by synergistic action of BMP4 and BMP8B signaling pathways.

作者信息

Ying Y, Qi X, Zhao G Q

机构信息

Department of Pathobiology, University of Missouri College of Veterinary Medicine, Columbia, MO 65211, USA.

出版信息

Proc Natl Acad Sci U S A. 2001 Jul 3;98(14):7858-62. doi: 10.1073/pnas.151242798. Epub 2001 Jun 26.

Abstract

Extraembryonic ectoderm-derived factors instruct the pluripotent epiblast cells to develop toward a restricted primordial germ cell (PGC) fate during murine gastrulation. Genes encoding Bmp4 of the Dpp class and Bmp8b of the 60A class are expressed in the extraembryonic ectoderm and targeted mutation of either results in severe defects in PGC formation. It has been shown that heterodimers of DPP and 60A classes of bone morphogenetic proteins (BMPs) are more potent than each homodimers in bone and mesoderm induction in vitro, suggesting that BMP4 and BMP8B may form heterodimers to induce PGCs. To investigate how BMP4 and BMP8B interact and signal for PGC induction, we cocultured epiblasts of embryonic day 6.0--6.25 embryos with BMP4 and BMP8B proteins produced by COS cells. Our data show that BMP4 or BMP8B homodimers alone cannot induce PGCs whereas they can in combination, providing evidence that two BMP pathways are simultaneously required for the generation of a given cell type in mammals and also providing a prototype method for PGC induction in vitro. Furthermore, the PGC defects of Bmp8b mutants can be rescued by BMP8B homodimers whereas BMP4 homodimers cannot mitigate the PGC defects of Bmp4 null mutants, suggesting that BMP4 proteins are also required for epiblast cells to gain germ-line competency before the synergistic action of BMP4 and BMP8B.

摘要

在小鼠原肠胚形成过程中,胚外外胚层衍生因子指导多能性上胚层细胞向特定的原始生殖细胞(PGC)命运发展。编码Dpp类的Bmp4和60A类的Bmp8b的基因在胚外外胚层中表达,任一基因的靶向突变都会导致PGC形成严重缺陷。研究表明,骨形态发生蛋白(BMP)的DPP类和60A类异二聚体在体外诱导骨和中胚层方面比各自的同二聚体更有效,这表明BMP4和BMP8B可能形成异二聚体来诱导PGC。为了研究BMP4和BMP8B如何相互作用并为PGC诱导发出信号,我们将胚胎第6.0 - 6.25天胚胎的上胚层与COS细胞产生的BMP4和BMP8B蛋白共培养。我们的数据表明,单独的BMP4或BMP8B同二聚体不能诱导PGC,而它们联合时可以,这证明在哺乳动物中产生特定细胞类型同时需要两条BMP信号通路,也为体外诱导PGC提供了一种原型方法。此外,Bmp8b突变体的PGC缺陷可以被BMP8B同二聚体挽救,而BMP4同二聚体不能减轻Bmp4基因敲除突变体的PGC缺陷,这表明在BMP4和BMP8B协同作用之前,上胚层细胞获得种系能力也需要BMP4蛋白。

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