Dimeric analogues of non-cationic tricyclic aromatic carboxamides are a new class of cytotoxic agents.

Anti-cancer drug design Pub Date : 1999-06-01

J A Spicer, S A Gamage, G J Atwell, G J Finlay, B C Baguley, W A Denny

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Abstract

A series of tricyclic aromatic carboxamides, and their corresponding dimeric analogues, were prepared and their growth-inhibitory properties were evaluated in a series of cell lines. The dimeric compounds were prepared by reaction of the appropriate acids with carbonyl-1,1'-diimidazole, isolating the resulting imidazolides, and reacting these with a stoichiometric amount of the diamine. The monomeric carboxamides containing a (CH2)2NMe2 side chain had widely differing inhibitory potencies, with the known nitronaphthalimide (mitonafide) and acridine-4-carboxamide (DACA) being the most potent. The corresponding bis analogues, linked by a (CH2)3NMe(CH2)3 chain, were generally more potent, with the largest increases (dimer/monomer ratio 20- to 30-fold) seen for the nitronaphthalimides and the phenazines. Based on the intrinsic cytotoxicity of the monomers and the highest degree of increase in cytotoxicity on dimerization, the most interesting chromophores appear to be the acridine-4-carboxamide and phenazine-1-carboxamide. Both of these compounds showed significant growth delays (approximately 6 days) in an in vivo colon 38 tumour model in mice.

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非阳离子三环芳香族羧胺二聚体类似物是一类新的细胞毒性药物。

制备了一系列三环芳香族羧胺及其相应的二聚体类似物，并在一系列细胞系中评估了它们的生长抑制性能。二聚体化合物由适当的酸与羰基-1,1′-二咪唑反应，分离得到的咪唑类化合物，并与化学计量量的二胺反应。含有(CH2)2NMe2侧链的单体carboxamide具有广泛不同的抑制能力，其中已知的硝基萘酰亚胺(mitonafide)和吖啶-4-carboxamide (DACA)是最有效的。由(CH2)3NMe(CH2)3链连接的相应的bis类似物通常更有效，硝基萘酰亚胺和非那嗪的二聚体/单体比增加最大(20- 30倍)。基于单体固有的细胞毒性和二聚化时细胞毒性增加的最高程度，最有趣的发色团似乎是吖啶-4-羧酰胺和非那嗪-1-羧酰胺。在小鼠体内结肠肿瘤模型中，这两种化合物都显示出显著的生长延迟(约6天)。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Anti-cancer drug design

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