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首页> 外文期刊>Molecular cell >Direct binding of CDC20 protein family members activates the anaphase-promoting complex in mitosis and G1.
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Direct binding of CDC20 protein family members activates the anaphase-promoting complex in mitosis and G1.

机译:CDC20蛋白家族成员的直接结合激活有丝分裂和G1后期促进复合物。

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摘要

Activation of the anaphase-promoting complex (APC) is required for anaphase initiation and for exit from mitosis. We show that APC is activated during mitosis and G1 by two regulatory factors, hCDC20 and hCDH1. These proteins directly bind to APC and activate its cyclin ubiquitination activity. hCDC20 confers a strict destruction-box (D-box) dependence on APC, while hCDH1 shows a much more relaxed specificity for the D-box. In HeLa cells, the protein levels of hCDC20 as well as its binding to APC peak in mitosis and decrease drastically at early G1. Thus, hCDC20 is the mitotic activator of APC and directs the degradation of substrates containing the D-box. The hCDH1 protein level remains constant during the cell cycle and may target specific substrates lacking the D-box in G1, such as polo-like kinase, for ubiquitination.
机译:后期启动和有丝分裂的退出都需要激活后期促进复合物(APC)。我们显示,APC在有丝分裂和G1期间被两个调节因子hCDC20和hCDH1激活。这些蛋白质直接结合APC并激活其细胞周期蛋白泛素化活性。 hCDC20赋予APC严格的破坏盒(D-box)依赖性,而hCDH1显示出对D-box更为宽松的特异性。在HeLa细胞中,hCDC20的蛋白质水平及其与APC的结合在有丝分裂中达到峰值,并在G1早期急剧下降。因此,hCDC20是APC的有丝分裂活化剂,并指导含有D-box的底物的降解。 hCDH1蛋白水平在细胞周期中保持恒定,并可能针对G1中缺少D-box的特定底物(如polo样激酶)进行泛素化。

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