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Characterization of a new family of cyclin-dependent kinase activators

机译:新的细胞周期蛋白依赖性激酶激活剂家族的表征

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摘要

Progression through the cell cycle is regulated by CDKs (cyclin-dependent kinases), which associate with activating partners, named cyclins, to efficiently phosphorylate substrates. We previously reported the identification of RINGO, a Xenopus protein that can activate CDK1 and CDK2 despite lack of sequence similarity to cyclins, which plays a role in the regulation of the meiotic cell cycle in oocytes. In the present study we report the characterization of four mammalian RINGO proteins, which are 53–68% identical with Xenopus RINGO in a central core of about 75 residues. We show that all RINGO family members can bind to and activate CDK1 and CDK2, albeit with different efficiencies, but they do not bind to CDK4 or CDK6. The core RINGO sequences are critical for CDK activation. We also identified key residues in CDK2 that are required for RINGO binding. All RINGO proteins can also bind the CDK inhibitor p27Kip1, but with an inverse efficiency of their ability to bind to CDK1. Our results identify a new family of mammalian proteins that can activate CDKs and therefore potentially function as cell cycle regulators. The ability of RINGO proteins to activate CDK1 and CDK2 suggest also cyclin-independent roles for these kinases.
机译:整个细胞周期的进程受CDK(细胞周期蛋白依赖性激酶)调节,该CDK与激活伴侣(称为细胞周期蛋白)相关联,以有效地磷酸化底物。我们之前曾报道过RINGO的鉴定,这是一种爪蟾蛋白质,尽管与细胞周期蛋白缺乏序列相似性,但仍可以激活CDK1和CDK2,后者在卵母细胞减数分裂细胞周期的调节中发挥作用。在本研究中,我们报告了四种哺乳动物RINGO蛋白的表征,它们在大约75个残基的中央核心中与非洲爪蟾RINGO的53–68%相同。我们显示,所有RINGO家族成员都可以结合并激活CDK1和CDK2,尽管效率不同,但它们并不结合CDK4或CDK6。核心RINGO序列对于CDK激活至关重要。我们还确定了RINGO结合所需的CDK2中的关键残基。所有RINGO蛋白也可以结合CDK抑制剂p27 Kip1 ,但是其结合CDK1的能力却相反。我们的结果确定了一个新的哺乳动物蛋白家族,它们可以激活CDK,因此有可能充当细胞周期调节剂。 RINGO蛋白激活CDK1和CDK2的能力也暗示了这些激酶的细胞周期蛋白非依赖性作用。

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