新的康普他汀A4系列抗微管蛋白衍生物：合成与生物学评价。

New antitubulin derivatives in the combretastatin A4 series: synthesis and biological evaluation.

作者信息

Borrel Christine, Thoret Sylviane, Cachet Xavier, Guénard Daniel, Tillequin François, Koch Michel, Michel Sylvie

机构信息

Laboratoire de Pharmacognosie, Université René Descartes (Paris 5), CNRS UMR 8638, Faculté des Sciences Pharmaceutiques et Biologiques, 4 avenue de l'Observatoire, 75270 Paris cedex 06, France.

出版信息

Bioorg Med Chem. 2005 Jun 1;13(11):3853-64. doi: 10.1016/j.bmc.2005.02.039.

DOI:10.1016/j.bmc.2005.02.039

PMID:15863010

Abstract

Two series of combretastatin A4 derivatives (acrylamide=carboxamide and carbamate) were synthesized in order to improve the water solubility and stabilize the cis-configuration of the double bond. Their cytotoxic effects were evaluated against MCF-7, KB-3-1 and IGROV human cancer cell lines, as well as their inhibitory activity on tubulin polymerization. Results were compared to those of carboxamide 1, chosen as reference. Potent inhibitions were observed on both tests in the carboxamide series, particularly for compound 4d bearing a fluorine group in replacement of the 3-hydroxyl of CA4. In contrast, most of the carbamates were either inactive or displayed only moderate cytotoxicities. Interestingly, a submicromolar IC(50) was measured on MCF-7 cells for 6g, although this compound was totally devoid of antitubulin activity.

摘要

为了提高水溶性并稳定双键的顺式构型，合成了两类康普瑞他汀A4衍生物（丙烯酰胺=羧酰胺和氨基甲酸酯）。评估了它们对MCF-7、KB-3-1和IGROV人癌细胞系的细胞毒性作用，以及它们对微管蛋白聚合的抑制活性。将结果与选为参考的羧酰胺1的结果进行比较。在羧酰胺系列的两项测试中均观察到强效抑制作用，特别是对于在CA4的3-羟基位置带有氟基团的化合物4d。相比之下，大多数氨基甲酸酯要么无活性，要么仅表现出中等细胞毒性。有趣的是，尽管化合物6g完全没有抗微管蛋白活性，但在MCF-7细胞上测得其IC(50)为亚微摩尔级。

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新的康普他汀A4系列抗微管蛋白衍生物：合成与生物学评价。

New antitubulin derivatives in the combretastatin A4 series: synthesis and biological evaluation.

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