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The Final Link: Tapping the Power of Chemical Genetics to Connect the Molecular and Biologic Functions of Mitotic Protein Kinases

机译:最后一个环节:利用化学遗传学的力量来连接有丝分裂蛋白激酶的分子和生物学功能

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摘要

During mitosis, protein kinases coordinate cellular reorganization and chromosome segregation to ensure accurate distribution of genetic information into daughter cells. Multiple protein kinases contribute to mitotic regulation, modulating molecular signaling more rapidly than possible with gene expression. However, a comprehensive understanding of how kinases regulate mitotic progression remains elusive. The challenge arises from multiple functions and substrates, a large number of “bystander” phosphorylation events, and the brief window in which all mitotic events transpire. Analog-sensitive alleles of protein kinases are powerful chemical genetic tools for rapid and specific interrogation of kinase function. Moreover, combining these tools with advanced proteomics and substrate labeling has identified phosphorylation sites on numerous protein targets. Here, we review the chemical genetic tools available to study kinase function and identify substrates. We describe how chemical genetics can also be used to link kinase function with cognate phosphorylation events to provide mechanistic detail. This can be accomplished by dissecting subsets of kinase functions and chemical genetic complementation. We believe a complete “chemical genetic toolbox” will ultimately allow a comprehensive understanding of how protein kinases regulate mitosis.
机译:在有丝分裂期间,蛋白激酶协调细胞重组和染色体分离,以确保遗传信息准确地分布到子细胞中。多种蛋白激酶可促进有丝分裂调节,从而比基因表达更快地调节分子信号传导。但是,对激酶如何调节有丝分裂进程的全面了解仍然难以捉摸。挑战来自多种功能和底物,大量“旁观者”磷酸化事件,以及所有有丝分裂事件都在其中发生的短暂窗口。蛋白激酶的类似物敏感等位基因是用于快速和特异地研究激酶功能的强大化学遗传工具。此外,将这些工具与先进的蛋白质组学和底物标记相结合,已鉴定出许多蛋白质靶标上的磷酸化位点。在这里,我们回顾了可用于研究激酶功能和鉴定底物的化学遗传工具。我们描述了如何化学遗传学也可以用来关联关联的磷酸化事件激酶功能,以提供机制的详细信息。这可以通过解剖激酶功能和化学遗传互补的子集来实现。我们相信,完整的“化学遗传工具箱”将最终使人们全面了解蛋白激酶如何调控有丝分裂。

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