Kohn K W, Pommier Y
Laboratory of Molecular Pharmacology, Division of Basic Sciences, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892, USA.
Ann N Y Acad Sci. 2000;922:11-26. doi: 10.1111/j.1749-6632.2000.tb07021.x.
Camptothecin, originally discovered in 1957 as an antitumor activity in plant extracts, has recently become one of the most promising leads to new anticancer drugs. After lingering for many years, interest in camptothecin was revitalized in 1985 upon discovery of its specific action on topoisomerase I. Detailed elucidation of action mechanisms at the molecular, cellular, and pharmacologic levels has made camptothecin and its congeners perhaps the best understood among clinical anticancer drugs. Promising chemical variants of camptothecin, and recently other chemical categories of topoisomerase I-targeted drugs, provide unusually rich opportunities for rational drug selection and design. This is made possible by current concepts based, for the most part, on a sound experimental foundation, which points the way towards optimally effective therapy.
喜树碱最初于1957年在植物提取物中被发现具有抗肿瘤活性,最近已成为最有前景的新型抗癌药物先导物之一。在沉寂多年之后,1985年对喜树碱的兴趣因发现其对拓扑异构酶I的特异性作用而重新燃起。在分子、细胞和药理学水平上对作用机制的详细阐明,使喜树碱及其同类物可能成为临床抗癌药物中理解最透彻的药物。喜树碱有前景的化学变体以及最近其他化学类别的拓扑异构酶I靶向药物,为合理的药物选择和设计提供了异常丰富的机会。这在很大程度上基于坚实实验基础的当前概念得以实现,这些概念为最佳有效治疗指明了方向。
Zotero 插件