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首页> 外文期刊>Journal of Medicinal Chemistry >Identification, synthesis, and biological evaluation of metabolites of the experimental cancer treatment drugs indotecan (LMP400) and indimitecan (LMP776) and investigation of isomerically hydroxylated indenoisoquinoline analogues as topoisomerase i poisons
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Identification, synthesis, and biological evaluation of metabolites of the experimental cancer treatment drugs indotecan (LMP400) and indimitecan (LMP776) and investigation of isomerically hydroxylated indenoisoquinoline analogues as topoisomerase i poisons

机译:鉴定,合成和生物学评估实验性癌症治疗药物靛蓝(Indotecan(LMP400)和靛蓝(Indimitecan)(LMP776)的代谢产物以及研究异构化羟化茚并异喹啉类似物作为拓扑异构酶i毒物

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摘要

Hydroxylated analogues of the anticancer topoisomerase I (Top1) inhibitors indotecan (LMP400) and indimitecan (LMP776) have been prepared because (1) a variety of potent Top1 poisons are known that contain strategically placed hydroxyl groups, which provides a clear rationale for incorporating them in the present case, and (2) the hydroxylated compounds could conceivably serve as synthetic standards for the identification of metabolites. Indeed, incubating LMP400 and LMP776 with human liver microsomes resulted in two major metabolites of each drug, which had HPLC retention times and mass fragmentation patterns identical to those of the synthetic standards. The hydroxylated indotecan and indimitecan metabolites and analogues were tested as Top1 poisons and for antiproliferative activity in a variety of human cancer cell cultures and in general were found to be very potent. Differences in activity resulting from the placement of the hydroxyl group are explained by molecular modeling analyses.
机译:已经制备了抗癌拓扑异构酶I(Top1)抑制剂靛蓝(LMP400)和靛蓝(LMP776)的羟基类似物,因为(1)已知有多种强效的Top1毒物,它们含有策略性放置的羟基,为掺入它们提供了明确的理由在目前情况下,(2)羟基化的化合物可以作为合成代谢产物鉴定的标准。实际上,将LMP400和LMP776与人肝微粒体一起孵育会导致每种药物的两种主要代谢产物,其HPLC保留时间和质量碎片模式与合成标准品相同。羟基化的吲哚can和indimitecan代谢产物和类似物作为Top1毒剂进行了测试,并在多种人类癌细胞培养物中具有抗增殖活性,通常被认为具有很强的效力。由羟基位置引起的活性差异通过分子模型分析来解释。

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