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首页> 外文期刊>Anti-Cancer Drug Design >Synthesis and cytotoxic activity of carboxamide derivatives of benzimidazo(2,1-a)isoquinoline and pyrido(3',2':4,5)imidazo(2,1-a)isoquinoline.
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Synthesis and cytotoxic activity of carboxamide derivatives of benzimidazo(2,1-a)isoquinoline and pyrido(3',2':4,5)imidazo(2,1-a)isoquinoline.

机译:苯并咪唑并(2,1-a)异喹啉和吡啶并(3',2':4,5)咪唑并(2,1-a)异喹啉的羧酰胺衍生物的合成和细胞毒性活性。

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摘要

A series of benzimidazo[2,1-a]isoquinolines with carboxamide side chains at the 1-, 6-, 9- and 11-positions were prepared, in order to study the biological effects of varying the position of the side chain in this tetracyclic series. The 6-, 9- and 11-analogues were obtained by modifications to published chemistry. The 1-carboxamide analogue was obtained via a one-pot isocoumarin/isoquinolone conversion of 3-methylisocoumarin-8-carboxylic acid with o-phenylenediamine in buffered aqueous acid, which gave the required 1-acid. The compounds were evaluated in a panel of cell lines in culture. The 6-carboxamides, where the side chain is attached to one of the central rings, were not active, but the 1- and 11-carboxamides, where the side chain is attached to one of the terminal rings off the chromophore short axis, were reasonably cytotoxic (IC50s < 1 microM). Overall, the structure-activity relationships are broadly in line with those seen with other tri- and tetracyclic carboxamides, and are consistent with recent crystal structure studies of acridine-4-carboxamides bound to DNA. The most potent 1-carboxamide was highly active in vivo against s.c. colon 38 tumours in mice, providing a growth delay of 12 days.
机译:制备了一系列在1、6、9和11位带有羧酰胺侧链的苯并咪唑并[2,1-a]异喹啉,以研究改变侧链位置的生物学效应。四环系列。 6、9和11类似物是通过对已发表化学方法的修改而获得的。通过在缓冲的含水酸中将3-甲基异香豆素-8-羧酸与邻苯二胺进行一锅异香豆素/异喹诺酮转化来获得1-羧酰胺类似物,得到所需的1-酸。在一组培养的细胞系中评估化合物。侧链连接到一个中心环上的6-羧酰胺没有活性,但是侧链连接在生色团短轴上的一个末端环上的1-和11-羧酰胺却没有活性。具有一定的细胞毒性(IC50 <1 microM)。总体而言,其结构活性关系与其他三环和四环羧酰胺的结构关系基本一致,并且与近期结合到DNA上的a啶-4-羧酰胺的晶体结构研究一致。最有效的1-羧酰胺在体内对s.c具有很高的活性。小鼠中出现38个结肠癌肿瘤,提供了12天的生长延迟。

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