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微管与化学性质多样的稳定剂的相互作用:与紫杉醇位点结合的热力学预测细胞毒性。

Microtubule interactions with chemically diverse stabilizing agents: thermodynamics of binding to the paclitaxel site predicts cytotoxicity.

作者信息

Buey Rubén M, Barasoain Isabel, Jackson Evelyn, Meyer Arndt, Giannakakou Paraskevi, Paterson Ian, Mooberry Susan, Andreu José M, Díaz J Fernando

机构信息

Centro de Investigaciones Biológicas, Consejo Superior de Investigaciones Científicas, Ramiro de Maeztu 9, 28040 Madrid, Spain.

出版信息

Chem Biol. 2005 Dec;12(12):1269-79. doi: 10.1016/j.chembiol.2005.09.010.

Abstract

The interactions of microtubules with most compounds described as stabilizing agents have been studied. Several of them (lonafarnib, dicumarol, lutein, and jatrophane polyesters) did not show any stabilizing effect on microtubules. Taccalonolides A and E show paclitaxel-like effects in cells, but they were not able to modulate in vitro tubulin assembly or to bind microtubules, which suggests that other factors are involved in their cellular effects. The binding constants of epothilones, eleutherobin, discodermolide, sarcodictyins, 3,17beta-diacetoxy-2-ethoxy-6-oxo-B-homo-estra-1,3,5(10)-triene, and dictyostatin to the paclitaxel site; the critical concentrations of ligand-induced assembly; and their cytotoxicity in carcinoma cells have been measured, and correlations between these parameters have been determined. The inhibition of cell proliferation correlates better with the binding enthalpy change than with the binding constants, suggesting that large, favorable enthalpic contribution to the binding is desired to design paclitaxel site drugs with higher cytotoxicity.

摘要

已对微管与大多数被描述为稳定剂的化合物之间的相互作用进行了研究。其中几种(洛那法尼、双香豆素、叶黄素和麻风树聚酯)对微管未显示出任何稳定作用。他卡诺内酯A和E在细胞中表现出类似紫杉醇的作用,但它们无法调节体外微管蛋白组装或结合微管,这表明其他因素参与了它们的细胞效应。已测量了埃坡霉素、刺参素、盘状海绵内酯、肉珊瑚素、3,17β - 二乙酰氧基 - 2 - 乙氧基 - 6 - 氧代 - B - 高 - 雌甾 - 1,3,5(10) - 三烯和双蒂斯塔丁与紫杉醇位点的结合常数、配体诱导组装的临界浓度及其在癌细胞中的细胞毒性,并确定了这些参数之间的相关性。细胞增殖的抑制与结合焓变的相关性比与结合常数的相关性更好,这表明为设计具有更高细胞毒性的紫杉醇位点药物,需要对结合有较大的、有利的焓贡献。

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