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Molecular systems biology of Sic1 in yeast cell cycle regulation through multiscale modeling.

机译:Sic1分子系统生物学中酵母细胞周期调控的多尺度建模。

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Cell cycle control is highly regulated to guarantee the precise timing of events essential for cell growth, i.e., DNA replication onset and cell division. Failure of this control plays a role in cancer and molecules called cyclin-dependent kinase (Cdk) inhibitors (Ckis) exploit a critical function in cell cycle timing. Here we present a multiscale modeling where experimental and computational studies have been employed to investigate structure, function and temporal dynamics of the Cki Sic1 that regulates cell cycle progression in Saccharomyces cerevisiae. Structural analyses reveal molecular details of the interaction between Sic1 and Cdk/cyclin complexes, and biochemical investigation reveals Sic1 function in analogy to its human counterpart p27(Kip1), whose deregulation leads to failure in timing of kinase activation and, therefore, to cancer. Following these findings, a bottom-up systems biology approach has been developed to characterize modular networks addressing Sic1 regulatory function. Through complementary experimentation and modeling, we suggest a mechanism that underlies Sic1 function in controlling temporal waves of cyclins to ensure correct timing of the phase-specific Cdk activities.
机译:严格控制细胞周期,以保证对细胞生长至关重要的事件的准确时间,即DNA复制开始和细胞分裂。这种控制的失败在癌症中起作用,称为细胞周期蛋白依赖性激酶(Cdk)抑制剂(Ckis)的分子在细胞周期计时中发挥了关键作用。在这里,我们提出了一种多尺度模型,其中已采用实验和计算研究来研究Cki Sic1的结构,功能和时间动态,该基因调节酿酒酵母中的细胞周期进程。结构分析揭示了Sic1与Cdk /细胞周期蛋白复合物之间相互作用的分子细节,生化研究显示Sic1类似于其人类对应物p27(Kip1)的功能,后者的失调导致激酶激活时间的失败,从而导致癌症。根据这些发现,开发了一种自下而上的系统生物学方法来表征解决Sic1调节功能的模块化网络。通过补充实验和建模,我们提出了一种机制,该机制是控制周期蛋白周期波的Sic1功能的基础,以确保特定阶段Cdk活动的正确时机。

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