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首页> 外文期刊>Molecular biology of the cell >A Highlights from MBoC Selection: A phosphatase threshold sets the level of Cdk1 activity in early mitosis in budding yeast
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A Highlights from MBoC Selection: A phosphatase threshold sets the level of Cdk1 activity in early mitosis in budding yeast

机译:MBoC选择的亮点:磷酸酶阈值可设定发芽酵母中有丝分裂早期Cdk1活性的水平

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摘要

Entry into mitosis is initiated by synthesis of cyclins, which bind and activate cyclin-dependent kinase 1 (Cdk1). Cyclin synthesis is gradual, yet activation of Cdk1 occurs in a stepwise manner: a low level of Cdk1 activity is initially generated that triggers early mitotic events, which is followed by full activation of Cdk1. Little is known about how stepwise activation of Cdk1 is achieved. A key regulator of Cdk1 is the Wee1 kinase, which phosphorylates and inhibits Cdk1. Wee1 and Cdk1 show mutual regulation: Cdk1 phosphorylates Wee1, which activates Wee1 to inhibit Cdk1. Further phosphorylation events inactivate Wee1. We discovered that a specific form of protein phosphatase 2A (PP2ACdc55) opposes the initial phosphorylation of Wee1 by Cdk1. In vivo analysis, in vitro reconstitution, and mathematical modeling suggest that PP2ACdc55 sets a threshold that limits activation of Wee1, thereby allowing a low constant level of Cdk1 activity to escape Wee1 inhibition in early mitosis. These results define a new role for PP2ACdc55 and reveal a systems-level mechanism by which dynamically opposed kinase and phosphatase activities can modulate signal strength.
机译:进入有丝分裂是由细胞周期蛋白的合成开始的,细胞周期蛋白结合并激活细胞周期蛋白依赖性激酶1(Cdk1)。细胞周期蛋白的合成是渐进的,但Cdk1的激活是逐步发生的:最初会产生低水平的Cdk1活性,这会触发早期的有丝分裂事件,然后完全激活Cdk1。关于如何实现Cdk1逐步激活知之甚少。 Cdk1的关键调控因子是Wee1激酶,该酶磷酸化并抑制Cdk1。 Wee1和Cdk1显示相互调节:Cdk1使Wee1磷酸化,从而激活Wee1以抑制Cdk1。进一步的磷酸化事件使Wee1失活。我们发现一种特定形式的蛋白质磷酸酶2A(PP2A Cdc55 )与Cdk1引起的Wee1的初始磷酸化相反。体内分析,体外重建和数学建模表明,PP2A Cdc55 设置了一个限制Wee1激活的阈值,从而允许较低的恒定Cdk1活性水平逃脱早期有丝分裂中对Wee1的抑制。这些结果为PP2A Cdc55 定义了新的作用,并揭示了系统级机制,通过该机制,动态相反的激酶和磷酸酶活性可以调节信号强度。

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