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A quantitative model for cyclin-dependent kinase control of the cell cycle: revisited

机译:重新研究细胞周期蛋白依赖性激酶控制的定量模型

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摘要

The eukaryotic cell division cycle encompasses an ordered series of events. Chromosomal DNA is replicated during S phase of the cell cycle before being distributed to daughter cells in mitosis. Both S phase and mitosis in turn consist of an intricately ordered sequence of molecular events. How cell cycle ordering is achieved, to promote healthy cell proliferation and avert insults on genomic integrity, has been a theme of Paul Nurse’s research. To explain a key aspect of cell cycle ordering, sequential S phase and mitosis, Stern & Nurse proposed ‘A quantitative model for cdc2 control of S phase and mitosis in fission yeast’. In this model, S phase and mitosis are ordered by their dependence on increasing levels of cyclin-dependent kinase (Cdk) activity. Alternative mechanisms for ordering have been proposed that rely on checkpoint controls or on sequential waves of cyclins with distinct substrate specificities. Here, we review these ideas in the light of experimental evidence that has meanwhile accumulated.Quantitative Cdk control emerges as the basis for cell cycle ordering, fine-tuned by cyclin specificity and checkpoints. We propose a molecular explanation for quantitative Cdk control, based on thresholds imposed by Cdk-counteracting phosphatases, and discuss its implications.
机译:真核细胞分裂周期包括一系列有序的事件。染色体DNA在细胞周期的S期复制,然后分配给有丝分裂的子代细胞。 S期和有丝分裂都由分子事件的错综复杂的顺序组成。如何实现细胞周期排序,以促进健康的细胞增殖并避免对基因组完整性的侮辱,一直是Paul Nurse研究的主题。为了解释细胞周期排序,顺序S期和有丝分裂的关键方面,Stern&Nurse提出了“裂变酵母中cdc2控制S期和有丝分裂的定量模型”。在此模型中,S期和有丝分裂取决于它们对细胞周期蛋白依赖性激酶(Cdk)活性水平的依赖性。已经提出了用于排序的替代机制,其依赖于检查点控制或具有不同底物特异性的细胞周期蛋白的连续波。在这里,我们将根据积累的实验证据对这些观点进行回顾。定量Cdk控制作为细胞周期有序化的基础出现,并通过细胞周期蛋白的特异性和检查点进行了微调。我们提出了基于Cdk抗磷酸酶强加的阈值的定量Cdk控制的分子解释,并讨论了其含义。

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