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拓扑异构酶 1B 抑制剂:半个多世纪的药物先导物、临床候选药物和偶然发现。

Topoisomerase 1B poisons: Over a half-century of drug leads, clinical candidates, and serendipitous discoveries.

机构信息

Department of Pharmacology and Toxicology, Michigan State University, East Lansing, Michigan.

出版信息

Med Res Rev. 2019 Jul;39(4):1294-1337. doi: 10.1002/med.21546. Epub 2018 Nov 19.

Abstract

Topoisomerases are DNA processing enzymes that relieve supercoiling (torsional strain) in DNA, are necessary for normal cellular division, and act by nicking (and then religating) DNA strands. Type 1B topoisomerase (Top1) is overexpressed in certain tumors, and the enzyme has been extensively investigated as a target for cancer chemotherapy. Various chemical agents can act as "poisons" of the enzyme's religation step, leading to Top1-DNA lesions, DNA breakage, and eventual cellular death. In this review, agents that poison Top1 (and have thus been investigated for their anticancer properties) are surveyed, including natural products (such as camptothecins and indolocarbazoles), semisynthetic camptothecin and luotonin derivatives, and synthetic compounds (such as benzonaphthyridines, aromathecins, and indenoisoquinolines), as well as targeted therapies and conjugates. Top1 has also been investigated as a therapeutic target in certain viral and parasitic infections, as well as autoimmune, inflammatory, and neurological disorders, and a summary of literature describing alternative indications is also provided. This review should provide both a reference for the medicinal chemist and potentially offer clues to aid in the development of new Top1 poisons.

摘要

拓扑异构酶是一种 DNA 加工酶,可缓解 DNA 的超螺旋(扭转应变),对于正常的细胞分裂是必需的,其作用方式是切割(然后重新连接)DNA 链。1B 型拓扑异构酶(Top1)在某些肿瘤中过度表达,该酶已被广泛研究作为癌症化疗的靶点。各种化学试剂可以作为酶的连接步骤的“毒物”,导致 Top1-DNA 损伤、DNA 断裂和最终的细胞死亡。在这篇综述中,调查了毒害 Top1 的试剂(因此已针对其抗癌特性进行了研究),包括天然产物(如喜树碱和吲哚咔唑)、半合成喜树碱和洛托汀衍生物以及合成化合物(如苯并萘啶、芳香霉素和吲哚异喹啉),以及靶向治疗和缀合物。Top1 还被研究用于某些病毒和寄生虫感染以及自身免疫、炎症和神经紊乱的治疗靶点,还提供了描述替代适应症的文献摘要。这篇综述应该为药物化学家提供参考,并为开发新的 Top1 毒物提供线索。

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