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Dissecting the role of MPS1 in chromosome biorientation and the spindle checkpoint through the small molecule inhibitor reversine

机译:通过小分子抑制剂逆转分析MPS1在染色体生物定向和纺锤体检查点中的作用

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摘要

The catalytic activity of the MPS1 kinase is crucial for the spindle assembly checkpoint and for chromosome biorientation on the mitotic spindle. We report that the small molecule reversine is a potent mitotic inhibitor of MPS1. Reversine inhibits the spindle assembly checkpoint in a dose-dependent manner. Its addition to mitotic HeLa cells causes the ejection of Mad1 and the ROD–ZWILCH–ZW10 complex, both of which are important for the spindle checkpoint, from unattached kinetochores. By using reversine, we also demonstrate that MPS1 is required for the correction of improper chromosome–microtubule attachments. We provide evidence that MPS1 acts downstream from the AURORA B kinase, another crucial component of the error correction pathway. Our experiments describe a very useful tool to interfere with MPS1 activity in human cells. They also shed light on the relationship between the error correction pathway and the spindle checkpoint and suggest that these processes are coregulated and are likely to share at least a subset of their catalytic machinery.
机译:MPS1激酶的催化活性对于纺锤体装配检查点和有丝分裂纺锤体上的染色体生物定向至关重要。我们报告说,小分子可逆性是MPS1的有效有丝分裂抑制剂。逆转抑制以剂量依赖的方式抑制主轴组件检查点。它添加到有丝分裂的HeLa细胞中会导致Mad1和ROD-ZWILCH-ZW10复合物从独立的动植物体内弹出,这对于纺锤体检查点都很重要。通过使用可逆性,我们还证明了MPS1是纠正不正确的染色体-微管附件的必要条件。我们提供的证据表明,MPS1在AURORA B激酶(错误纠正途径的另一个关键组成部分)的下游起作用。我们的实验描述了一种非常有用的工具,可以干扰人细胞中的MPS1活性。他们还阐明了错误校正路径与主轴检查点之间的关系,并暗示这些过程是相互关联的,并且可能至少共享其催化机制的一部分。

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