摘要
背景:许多不同的化学物质与微管蛋白结合,通过破坏微管动力学抑制细胞增殖。有配体结合到微管蛋白的四个结合位点;紫杉醇/埃博霉素和laulimalide / peloruside结合配体稳定微管,长春花和秋水仙碱结合位点药物促进微管解聚作用。大多数的微管蛋白结合配体干扰微管蛋白微管的动态平衡,但这些可能通过不同的机制表现出抗癌活性。紫杉烷类,埃博霉素是广泛使用的针对不同类型恶性肿瘤的有效的细胞毒性药物。然而,紫杉烷类化合物容易导致糖蛋白介导的多药耐药,剂量限制性造血毒性和累积性神经毒性。长春花生物碱已经在运用到临床实践中,但是配体结合秋水仙碱位点仍处于临床试验的不同阶段。 目的:本综述里,描述了关于配体的结合口袋和随后的微管蛋白结构的变化的可信的机制细节。本文还说明了微管蛋白结合剂与其他化疗药物的不同配方和他们对各种人类恶性肿瘤的治疗潜力。 结论:微管蛋白靶向药物是最成功的抗癌药物之一,许多结构上不同的化合物正处于临床开发的高级阶段。
关键词: 微管蛋白抑制剂,微管稳定剂,微管蛋白聚合/解聚,抗癌,联合治疗,微管蛋白结合配体。
Current Cancer Drug Targets
Title:Mechanisms of Tubulin Binding Ligands to Target Cancer Cells: Updates on their Therapeutic Potential and Clinical Trials
Volume: 17 Issue: 4
关键词: 微管蛋白抑制剂,微管稳定剂,微管蛋白聚合/解聚,抗癌,联合治疗,微管蛋白结合配体。
摘要: Background: A number of chemically diverse substances bind to the tubulin and inhibit cell proliferation by disrupting microtubule dynamics. There are four binding sites for the ligands binding to the tubulin; taxane/epothilone and laulimalide/peloruside binding ligands stabilize microtubule while vinca and colchicine binding site agents promote microtubule depolymerization. Most of the tubulin binding ligands disturb the tubulin-microtubule dynamic equilibrium but these may exhibit anticancer activities through different mechanisms. Taxanes and epothilones are widely used cytotoxic agents and are found effective against different types of human malignancies. However, taxanes are susceptible to pgp mediated multi-drug resistance, dose limiting hematopoietic toxicity and cumulative neurotoxicity. Vinca alkaloids are already in clinical practice, but ligands binding to the colchicine site are still in the different stages of clinical trials.
Objective: In the current review article, plausible mechanistic details about the interactions of ligands at the binding pocket and subsequent changes in the tubulin structure are described. The review article also illustrated different formulations of the tubulin binding agents in combination with other chemotherapeutic agents and their therapeutic potential against various human malignancies. Conclusion: Tubulin targeting agents emerged as one of the most successful anticancer drugs and a number of structurally different chemical compounds are in advance stages of clinical development.Export Options
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Cite this article as:
Mechanisms of Tubulin Binding Ligands to Target Cancer Cells: Updates on their Therapeutic Potential and Clinical Trials, Current Cancer Drug Targets 2017; 17 (4) . https://dx.doi.org/10.2174/1568009616666160928110818
DOI https://dx.doi.org/10.2174/1568009616666160928110818 |
Print ISSN 1568-0096 |
Publisher Name Bentham Science Publisher |
Online ISSN 1873-5576 |
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