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首页> 外文期刊>Cell >Regulation of MBK-2/DYRK by CDK-1 and the Pseudophosphatases EGG-4 and EGG-5 during the Oocyte-to-Embryo Transition
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Regulation of MBK-2/DYRK by CDK-1 and the Pseudophosphatases EGG-4 and EGG-5 during the Oocyte-to-Embryo Transition

机译:在卵母细胞-胚胎过渡过程中,CDK-1和伪磷酸酶EGG-4和EGG-5对MBK-2 / DYRK的调节。

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摘要

DYRKs are kinases that self-activate in vitro by autophosphorylation of a YTY motif in the kinase domain, but their regulation in vivo is not well understood. In C. elegans zygotes, MBK-2/DYRK phosphorylates oocyte proteins at the end of the meiotic divisions to promote the oocyte-to-embryo transition. Here we demonstrate that MBK-2 is under both positive and negative regulation during the transition. MBK-2 is activated during oocyte maturation by CDK-1-dependent phosphorylation of serine 68, a residue outside of the kinase domain required for full activity in vivo. The pseudotyrosine phosphatases EGG-4 and EGG-5 sequester activated MBK-2 until the meiotic divisions by binding to the YTY motif and inhibiting MBK-20s kinase activity directly, using a mixed-inhibition mechanism that does not involve tyrosine dephosphorylation. Our findings link cell-cycle progression to MBK-2/DYRK activation and the oocyte-to-embryo transition.
机译:DYRKs是在激酶结构域中通过YTY基序的自身磷酸化在体外自我激活的激酶,但它们在体内的调节尚不十分清楚。在秀丽隐杆线虫合子中,MBK-2 / DYRK在减数分裂分裂的末端使卵母细胞蛋白磷酸化,从而促进卵母细胞向胚胎的过渡。在这里,我们证明了MBK-2在过渡过程中处于正调控和负调控之间。在卵母细胞成熟过程中,MBK-2通过丝氨酸68的CDK-1依赖性磷酸化而被激活,丝氨酸68是体内完整活性所需的激酶结构域之外的残基。伪酪氨酸磷酸化酶EGG-4和EGG-5螯合剂通过结合到YTY基序并直接抑制MBK-20s激酶活性而激活了MBK-2,直到减数分裂分裂为止,采用了不涉及酪氨酸去磷酸化的混合抑制机制。我们的发现将细胞周期进程与MBK-2 / DYRK激活以及卵母细胞向胚胎的转化联系起来。

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