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纺锤体组装检查点的时间演变建模及极光B激酶的作用。

Modeling the temporal evolution of the spindle assembly checkpoint and role of Aurora B kinase.

作者信息

Mistry Hitesh B, MacCallum David E, Jackson Robert C, Chaplain Mark A J, Davidson Fordyce A

机构信息

Division of Mathematics, University of Dundee, Dundee DD1 4HN, Scotland.

出版信息

Proc Natl Acad Sci U S A. 2008 Dec 23;105(51):20215-20. doi: 10.1073/pnas.0810706106. Epub 2008 Dec 17.

Abstract

Faithful separation of chromosomes prior to cell division at mitosis is a highly regulated process. One family of serine/threonine kinases that plays a central role in regulation is the Aurora family. Aurora B plays a role in the spindle assembly checkpoint, in part, by destabilizing the localization of BubR1 and Mad2 at centrosomes and responds to changes in tension caused by aberrant microtubule kinetochore attachments. Aurora B is overexpressed in a subset of cancers and is required for mitosis, making it an attractive anticancer target. Here, we use mathematical modeling to extend a current model of the spindle assembly checkpoint to incorporate all signaling kinetochores within a cell rather than just one and the role of Aurora B within the resulting model. We find that the current model of the spindle assembly checkpoint is robust to variation in its key diffusion-limited parameters. Furthermore, when Aurora B inhibition is considered within the model, for a certain range of inhibitor concentrations, a prolonged prometaphase/metaphase is observed. This level of inhibitor concentrations has not yet been studied experimentally, to the authors' best knowledge. Therefore, experimental verification of the results discussed here could provide a deeper understanding of how kinetochores and Aurora B cooperate in the spindle assembly checkpoint.

摘要

在有丝分裂的细胞分裂之前,染色体的忠实分离是一个受到高度调控的过程。在调控中起核心作用的一类丝氨酸/苏氨酸激酶是Aurora家族。Aurora B在纺锤体组装检查点中发挥作用,部分原因是通过破坏BubR1和Mad2在中心体的定位,并对异常微管动粒附着引起的张力变化做出反应。Aurora B在一部分癌症中过度表达,并且是有丝分裂所必需的,这使其成为一个有吸引力的抗癌靶点。在这里,我们使用数学建模来扩展当前的纺锤体组装检查点模型,以纳入细胞内所有的信号动粒,而不仅仅是一个,以及Aurora B在所得模型中的作用。我们发现,当前的纺锤体组装检查点模型对其关键的扩散限制参数的变化具有鲁棒性。此外,当在模型中考虑Aurora B抑制时,对于一定范围的抑制剂浓度,会观察到前中期/中期延长。据作者所知,尚未对该水平的抑制剂浓度进行实验研究。因此,对这里讨论的结果进行实验验证可以更深入地了解动粒和Aurora B在纺锤体组装检查点中是如何协作的。

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