佩洛利昔德、劳拉昔利德和诺斯卡品与微管蛋白的相互作用。

Peloruside, laulimalide, and noscapine interactions with beta-tubulin.

机构信息

Department of Oncology, University of Alberta, Edmonton, Alberta, Canada.

出版信息

Pharm Res. 2012 Nov;29(11):2985-93. doi: 10.1007/s11095-012-0809-2. Epub 2012 Jun 26.

Abstract

This article reviews the recent findings regarding the binding sites, binding modes and binding affinities of three novel antimitotic drugs peloruside, laulimalide and noscapine with respect to tubulin as the target of their action. These natural compounds are shown to bind to β-tubulin and stabilize microtubules for the cases of peloruside A and laulimalide, and prolong the time spent in pause for noscapine. Particular attention is focused on β-tubulin isotypes as targets for new cancer chemotherapy agents and the amino acid differences in the binding site for these compounds between isotypes. We propose a new strategy for antimitotic drug design that exploits differential distributions of tubulin isotypes between normal and cancer cells and corresponding differential affinities between various drug molecules and tubulin isotypes.

摘要

本文综述了三种新型抗有丝分裂药物——peloruside、laulimalide 和 noscapine 与微管蛋白（其作用靶点）结合的结合部位、结合方式和结合亲和力的最新研究发现。这些天然化合物被证明能够与β-微管蛋白结合，并稳定微管，peloruside A 和 laulimalide 就是这种情况，而 noscapine 则延长了微管的暂停时间。特别关注β-微管蛋白同工型作为新型癌症化疗药物的靶点，以及这些化合物在同工型之间结合部位的氨基酸差异。我们提出了一种新的抗有丝分裂药物设计策略，该策略利用了正常细胞和癌细胞之间微管蛋白同工型的不同分布以及各种药物分子与微管蛋白同工型之间的相应差异亲和力。

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佩洛利昔德、劳拉昔利德和诺斯卡品与微管蛋白的相互作用。

Peloruside, laulimalide, and noscapine interactions with beta-tubulin.

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