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细胞周期蛋白依赖性激酶底物磷酸化中的细胞周期蛋白特异性

Cyclin specificity in the phosphorylation of cyclin-dependent kinase substrates.

作者信息

Loog Mart, Morgan David O

机构信息

Department of Physiology, University of California, San Francisco, California 94143-2200, USA.

出版信息

Nature. 2005 Mar 3;434(7029):104-8. doi: 10.1038/nature03329.

Abstract

Cell-cycle events are controlled by cyclin-dependent kinases (CDKs), whose periodic activation is driven by cyclins. Different cyclins promote distinct cell-cycle events, but the molecular basis for these differences remains unclear. Here we compare the specificity of two budding yeast cyclins, the S-phase cyclin Clb5 and the M-phase cyclin Clb2, in the phosphorylation of 150 Cdk1 (Cdc28) substrates. About 24% of these proteins were phosphorylated more efficiently by Clb5-Cdk1 than Clb2-Cdk1. The Clb5-specific targets include several proteins (Sld2, Cdc6, Orc6, Mcm3 and Cdh1) involved in early S-phase events. Clb5 specificity depended on an interaction between a hydrophobic patch in Clb5 and a short sequence in the substrate (the RXL or Cy motif). Phosphorylation of Clb5-specific targets during S phase was reduced by replacing Clb5 with Clb2 or by mutating the substrate RXL motif, confirming the importance of Clb5 specificity in vivo. Although we did not identify any highly Clb2-specific substrates, we found that Clb2-Cdk1 possessed higher intrinsic kinase activity than Clb5-Cdk1, enabling efficient phosphorylation of a broad range of mitotic Cdk1 targets. Thus, Clb5 and Clb2 use distinct mechanisms to enhance the phosphorylation of S-phase and M-phase substrates.

摘要

细胞周期事件由细胞周期蛋白依赖性激酶(CDK)控制,其周期性激活由细胞周期蛋白驱动。不同的细胞周期蛋白促进不同的细胞周期事件,但其差异的分子基础仍不清楚。在这里,我们比较了两种芽殖酵母细胞周期蛋白,即S期细胞周期蛋白Clb5和M期细胞周期蛋白Clb2,对150种Cdk1(Cdc28)底物的磷酸化特异性。这些蛋白质中约24%被Clb5-Cdk1磷酸化的效率高于Clb2-Cdk1。Clb5特异性靶点包括几种参与早期S期事件的蛋白质(Sld2、Cdc6、Orc6、Mcm3和Cdh1)。Clb5的特异性取决于Clb5中的一个疏水区域与底物中的一个短序列(RXL或Cy基序)之间的相互作用。在S期,通过用Clb2替换Clb5或突变底物RXL基序,可降低Clb5特异性靶点的磷酸化,这证实了Clb5特异性在体内的重要性。虽然我们没有鉴定出任何高度特异性的Clb2底物,但我们发现Clb2-Cdk1比Clb5-Cdk1具有更高的内在激酶活性,能够有效磷酸化广泛的有丝分裂Cdk1靶点。因此,Clb5和Clb2利用不同的机制增强S期和M期底物的磷酸化。

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