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Recent advances in the targeting of human DNA ligase I as a potential new strategy for cancer treatment

机译:人体DNA连接酶I作为潜在的癌症治疗策略的最新进展

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摘要

The emergence of drug resistance, coupled with the issue of low tumor selectivity and toxicity is a major pitfall in cancer chemotherapy. It has necessitated the urgent need for the discovery of less toxic and more potent new anti-cancer pharmaceuticals, which target the interactive mechanisms involved in division and metastasis of cancer cells. Human DNA ligase I (hligI) plays an important role in DNA replication by linking Okazaki fragments on the lagging strand of DNA, and also participates in DNA damage repair processes. Dysregulation of the functioning of such ligases can severely impact DNA replication and repair pathways events that are generally targeted in cancer treatment. Although, several human DNA ligase inhibitors have been reported in the literature but unfortunately not a single inhibitor is currently being used in cancer chemotherapy. Results of pre-clinical studies also support the fact that human DNA ligases are an attractive target for the development of new anticancer agents which work by the selective inhibition of rapidly proliferating cancer cells. In this manuscript, we discuss, in brief, the structure, synthesis, structure-activity-relationship (SAR) and anticancer activity of recently reported hLigI inhibitors. (C) 2019 Elsevier Masson SAS. All rights reserved.
机译:耐药性的出现,加上低肿瘤选择性和毒性的问题是癌症化疗的主要缺陷。它需要迫切需要发现毒性较小,更有效的新抗癌药物,其靶向癌细胞分裂和转移的互动机制。人DNA连接酶I(hligI)播放由对DNA的后随链连接冈崎片段在DNA复制中起重要作用,并且也参与DNA损伤修复过程。这种连接酶的功能的失调可能严重影响DNA复制和修复途径事件,通常针对癌症治疗。虽然,在文献中报道了几种人类DNA连接酶抑制剂,但遗憾的是,目前没有单一抑制剂目前用于癌症化疗。临床前研究结果还支持人类DNA连接酶是一种有吸引力的靶向开发新的抗癌剂,其通过选择性抑制快速增殖的癌细胞。在该稿件中,我们简而言之,讨论最近报告的Hligi抑制剂的结构,合成,结构 - 活性 - 关系(SAR)和抗癌活性。 (c)2019年Elsevier Masson SAS。版权所有。

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