首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Vertebrate Ctr1 coordinates morphogenesis and progenitor cell fate and regulates embryonic stem cell differentiation
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Vertebrate Ctr1 coordinates morphogenesis and progenitor cell fate and regulates embryonic stem cell differentiation

机译:脊椎动物Ctr1协调形态发生和祖细胞命运并调节胚胎干细胞分化

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摘要

Embryogenesis involves two distinct processes. On the one hand, cells must specialize, acquiring fates appropriate to their positions (differentiation); on the other hand, they must physically construct the embryo through coordinated mechanical activity (morphogenesis). In early vertebrate development, fibroblast growth factor (FGF) regulates multiple embryonic events, including germ layer differentiation and morphogenesis; the cellular components that direct FGF signaling to evoke these different responses remain largely unknown. We show here that the copper transporter 1 (Ctr1) protein is a critical router of FGF signals during early embryogenesis. Ctr1 both promotes the differentiation and inhibits the morphogenesis of mesoderm and neurectoderm in embryos of the frog Xenopus laevis, thereby coordinating normal development. Signal sorting by Ctr1 involves the activation of the Ras-MAP kinase cascade and appears to be independent of its role in copper transport. Mouse embryonic stem (ES) cells deficient for Ctr1 (Ctr1~(-/-)) retain characteristics of pluripotency under conditions that favor differentiation in wild-type ES cells, indicating a conserved role for Ctr1 during amphibian and mammalian cell fate determination. Our studies support a model in which vertebrate Ctr1 functions as a key regulator of the differentiation capacity of both stem and progenitor cell populations.
机译:胚胎发生涉及两个不同的过程。一方面,细胞必须专门化,获得适合其位置的命运(分化)。另一方面,它们必须通过协调的机械活动(形态发生)在物理上构建胚胎。在脊椎动物的早期发育中,成纤维细胞生长因子(FGF)调节多种胚胎事件,包括胚层分化和形态发生。指导FGF信号转导这些不同反应的细胞成分仍然未知。我们在这里显示铜转运蛋白1(Ctr1)蛋白是早期胚胎发生过程中FGF信号的关键路由器。 Ctr1既促进蛙爪蟾胚胎中胚层和中胚层的分化,又抑制其形态发生,从而协调正常发育。通过Ctr1进行的信号分选涉及Ras-MAP激酶级联反应的激活,并且似乎与其在铜转运中的作用无关。缺乏Ctr1(Ctr1〜(-/-))的小鼠胚胎干(ES)细胞在有利于野生型ES细胞分化的条件下保留了多能性特征,表明Ctr1在两栖动物和哺乳动物细胞命运确定过程中的保守作用。我们的研究支持一种模型,其中脊椎动物Ctr1充当干细胞和祖细胞群体分化能力的关键调节剂。

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