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艾司西匹宁对人KSP的抑制机制。

Mechanism of inhibition of human KSP by ispinesib.

作者信息

Lad Latesh, Luo Lusong, Carson Jeffrey D, Wood Kenneth W, Hartman James J, Copeland Robert A, Sakowicz Roman

机构信息

Cytokinetics Inc., 280 East Grand Avenue, South San Francisco, California 94080, USA.

出版信息

Biochemistry. 2008 Mar 18;47(11):3576-85. doi: 10.1021/bi702061g. Epub 2008 Feb 22.

Abstract

KSP, also known as HsEg5, is a kinesin that plays an essential role in the formation of a bipolar mitotic spindle and is required for cell cycle progression through mitosis. Ispinesib is the first potent, highly specific small-molecule inhibitor of KSP tested for the treatment of human disease. This novel anticancer agent causes mitotic arrest and growth inhibition in several human tumor cell lines and is currently being tested in multiple phase II clinical trials. In this study we have used steady-state and pre-steady-state kinetic assays to define the mechanism of KSP inhibition by ispinesib. Our data show that ispinesib alters the ability of KSP to bind to microtubules and inhibits its movement by preventing the release of ADP without preventing the release of the KSP-ADP complex from the microtubule. This type of inhibition is consistent with the physiological effect of ispinesib on cells, which is to prevent KSP-driven mitotic spindle pole separation. A comparison of ispinesib to monastrol, another small-molecule inhibitor of KSP, reveals that both inhibitors share a common mode of inhibition.

摘要

驱动蛋白样蛋白(KSP),也被称为HsEg5,是一种驱动蛋白,在双极有丝分裂纺锤体的形成中发挥着重要作用,并且是细胞通过有丝分裂进行细胞周期进程所必需的。艾司匹那司(Ispinesib)是首个经测试用于治疗人类疾病的强效、高特异性KSP小分子抑制剂。这种新型抗癌药物在多种人类肿瘤细胞系中引起有丝分裂停滞和生长抑制,目前正在多个II期临床试验中进行测试。在本研究中,我们使用稳态和预稳态动力学分析来确定艾司匹那司对KSP的抑制机制。我们的数据表明,艾司匹那司改变了KSP与微管结合的能力,并通过阻止ADP的释放来抑制其运动,而不阻止KSP-ADP复合物从微管上释放。这种抑制类型与艾司匹那司对细胞的生理作用一致,即防止KSP驱动的有丝分裂纺锤体极分离。将艾司匹那司与另一种KSP小分子抑制剂莫那可林(monastrol)进行比较,发现这两种抑制剂具有共同的抑制模式。

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