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新型微管抑制剂类抗癌药物。

New microtubule-inhibiting anticancer agents.

机构信息

Shanghai Institute of Materia Medica, Chinese Academy of Sciences, Division of Antitumor Pharmacology, State Key Laboratory of Drug Research, 555 Zu Chong Zhi Road, Zhangjiang Hi-Tech Park, Shanghai 201203, People's Republic of China.

出版信息

Expert Opin Investig Drugs. 2010 Mar;19(3):329-43. doi: 10.1517/13543780903571631.

Abstract

UNLABELLED

IMPORTANCE OF THIS FIELD: Microtubule-inhibiting drugs are among the most commonly prescribed agents in the combat against cancer, though the clinical use of these drugs is limited by acquired resistance, risk of hypersensitivity reactions and intolerable toxicity. With progress in our understanding of cytoskeleton structure and its related signaling pathways, a number of new microtubule-inhibiting agents with diversified structures and modes of action have emerged.

WHAT THE READER WILL GAIN

This review mainly describes new microtubule-targeting anticancer agents that have been discovered (especially over the past 2 years), with emphasis on their diversity of structures and distinct modes of action.

AREAS COVERED IN THIS REVIEW

Data were obtained exclusively from public sources, including journals and scientific meeting abstracts, up to September 2009.

TAKE HOME MESSAGE

A number of new agents have been discovered, and some have entered clinical trials. Even though most of these agents stabilize or destabilize tubulin via binding on the recognized tubulin binding sites, a few compounds bind to tubulin on undefined sites or interrupt microtubule in diverse ways. Moreover, some agents target microtubule indirectly such that they alter the post-translational modification of tubulin. Further investigation into their mechanism of action and evaluation of their anticancer efficacy will help to develop novel regimens that are superior to existing approaches.

摘要

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本领域的重要性

尽管这些药物的临床应用受到获得性耐药性、过敏反应风险和无法耐受的毒性的限制,但微管抑制药物仍是对抗癌症最常开的药物之一。随着我们对细胞骨架结构及其相关信号通路的理解的进展,许多新的具有不同结构和作用方式的微管抑制药物已经出现。

读者将获得什么

这篇综述主要描述了新发现的(特别是过去 2 年中)针对微管的抗癌药物,重点介绍它们结构的多样性和不同的作用方式。

本篇综述涵盖的领域

数据完全来自公共资源,包括期刊和科学会议摘要,截至 2009 年 9 月。

要点

已经发现了一些新的药物,其中一些已经进入临床试验。尽管这些药物中的大多数通过与已识别的微管结合部位结合来稳定或不稳定微管,但少数化合物与微管在未定义的部位结合或以不同的方式打断微管。此外,一些药物间接靶向微管,从而改变微管蛋白的翻译后修饰。进一步研究它们的作用机制和评估它们的抗癌疗效将有助于开发优于现有方法的新方案。

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