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RSPO1/β-catenin signaling pathway regulates oogonia differentiation and entry into meiosis in the mouse fetal ovary

机译:RspO1 /β-catenin信号通路调节卵巢分化并进入小鼠胎儿卵巢的减数分裂

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摘要

Differentiation of germ cells into male gonocytes or female oocytes is a central event in sexual reproduction. Proliferation and differentiation of fetal germ cells depend on the sex of the embryo. In male mouse embryos, germ cell proliferation is regulated by the RNA helicase Mouse Vasa homolog gene and factors synthesized by the somatic Sertoli cells promote gonocyte differentiation. In the female, ovarian differentiation requires activation of the WNT/β-catenin signaling pathway in the somatic cells by the secreted protein RSPO1. Using mouse models, we now show that Rspo1 also activates the WNT/β-catenin signaling pathway in germ cells. In XX Rspo1(-/-) gonads, germ cell proliferation, expression of the early meiotic marker Stra8, and entry into meiosis are all impaired. In these gonads, impaired entry into meiosis and germ cell sex reversal occur prior to detectable Sertoli cell differentiation, suggesting that β-catenin signaling acts within the germ cells to promote oogonial differentiation and entry into meiosis. Our results demonstrate that RSPO1/β-catenin signaling is involved in meiosis in fetal germ cells and contributes to the cellular decision of germ cells to differentiate into oocyte or sperm.
机译:生殖细胞分化为雄性母细胞或雌性卵母细胞是有性生殖的重要事件。胎儿生殖细胞的增殖和分化取决于胚胎的性别。在雄性小鼠胚胎中,生殖细胞的增殖受RNA解旋酶Mouse Vasa同源基因的调控,而体细胞的支持细胞合成的因子则促进了生殖细胞的分化。在雌性中,卵巢分化需要通过分泌的蛋白质RSPO1激活体细胞中的WNT /β-catenin信号通路。使用小鼠模型,我们现在显示Rspo1还激活生殖细胞中的WNT /β-catenin信号通路。在XX Rspo1(-/-)性腺中,生殖细胞增殖,早期减数分裂标记Stra8的表达以及进入减数分裂均受到损害。在这些性腺中,减数分裂进入减数分裂和生殖细胞性逆转发生在可检测到的支持细胞分化之前,这表明β-catenin信号在生殖细胞内起作用,促进卵母细胞分化和减数分裂。我们的结果表明,RSPO1 /β-catenin信号传导参与胎儿生殖细胞的减数分裂,并有助于生殖细胞的细胞决定分化为卵母细胞或精子。

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