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一种驱动蛋白抑制剂的抗肿瘤活性

Antitumor activity of a kinesin inhibitor.

作者信息

Sakowicz Roman, Finer Jeffrey T, Beraud Christophe, Crompton Anne, Lewis Evan, Fritsch Alex, Lee Yan, Mak John, Moody Robert, Turincio Rebecca, Chabala John C, Gonzales Paul, Roth Stephanie, Weitman Steve, Wood Kenneth W

机构信息

Cytokinetics, Inc., South San Francisco, California 94080, USA.

出版信息

Cancer Res. 2004 May 1;64(9):3276-80. doi: 10.1158/0008-5472.can-03-3839.

Abstract

Several members of the kinesin family of microtubule motor proteins play essential roles in mitotic spindle function and are potential targets for the discovery of novel antimitotic cancer therapies. KSP, also known as HsEg5, is a kinesin that plays an essential role in formation of a bipolar mitotic spindle and is required for cell cycle progression through mitosis. We identified a potent inhibitor of KSP, CK0106023, which causes mitotic arrest and growth inhibition in several human tumor cell lines. Here we show that CK0106023 is an allosteric inhibitor of KSP motor domain ATPase with a Ki of 12 nM. Among five kinesins tested, CK0106023 was specific for KSP. In tumor-bearing mice, CK0106023 exhibited antitumor activity comparable to or exceeding that of paclitaxel and caused the formation of monopolar mitotic figures identical to those produced in cultured cells. KSP was most abundant in proliferating human tissues and was absent from cultured postmitotic neurons. These findings are the first to demonstrate the feasibility of targeting mitotic kinesins for the treatment of cancer.

摘要

微管运动蛋白驱动蛋白家族的几个成员在有丝分裂纺锤体功能中发挥着重要作用,是发现新型抗有丝分裂癌症疗法的潜在靶点。KSP,也称为HsEg5,是一种驱动蛋白,在双极有丝分裂纺锤体的形成中起重要作用,是细胞周期通过有丝分裂进展所必需的。我们鉴定出一种有效的KSP抑制剂CK0106023,它能在几种人类肿瘤细胞系中引起有丝分裂停滞和生长抑制。在此我们表明,CK0106023是KSP运动结构域ATP酶的变构抑制剂,其Ki为12 nM。在所测试的五种驱动蛋白中,CK0106023对KSP具有特异性。在荷瘤小鼠中,CK0106023表现出与紫杉醇相当或超过紫杉醇的抗肿瘤活性,并导致形成与培养细胞中产生的单极有丝分裂图像相同的图像。KSP在增殖的人体组织中含量最高,而在培养的有丝分裂后神经元中不存在。这些发现首次证明了靶向有丝分裂驱动蛋白治疗癌症的可行性。

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