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第二代抗菌苯并咪唑脲类化合物:发现一种具有降低代谢风险的临床前候选药物。

Second-generation antibacterial benzimidazole ureas: discovery of a preclinical candidate with reduced metabolic liability.

机构信息

Vertex Pharmaceuticals Incorporated , 50 Northern Avenue, Boston, Massachusetts 02210, United States.

出版信息

J Med Chem. 2014 Nov 13;57(21):8792-816. doi: 10.1021/jm500563g. Epub 2014 Oct 28.

Abstract

Compound 3 is a potent aminobenzimidazole urea with broad-spectrum Gram-positive antibacterial activity resulting from dual inhibition of bacterial gyrase (GyrB) and topoisomerase IV (ParE), and it demonstrates efficacy in rodent models of bacterial infection. Preclinical in vitro and in vivo studies showed that compound 3 covalently labels liver proteins, presumably via formation of a reactive metabolite, and hence presented a potential safety liability. The urea moiety in compound 3 was identified as being potentially responsible for reactive metabolite formation, but its replacement resulted in loss of antibacterial activity and/or oral exposure due to poor physicochemical parameters. To identify second-generation aminobenzimidazole ureas devoid of reactive metabolite formation potential, we implemented a metabolic shift strategy, which focused on shifting metabolism away from the urea moiety by introducing metabolic soft spots elsewhere in the molecule. Aminobenzimidazole urea 34, identified through this strategy, exhibits similar antibacterial activity as that of 3 and did not label liver proteins in vivo, indicating reduced/no potential for reactive metabolite formation.

摘要

化合物 3 是一种强效的苯并咪唑脲类化合物,具有广谱的革兰氏阳性菌抗菌活性,这是由于其对细菌拓扑异构酶 II(GyrB)和拓扑异构酶 IV(ParE)的双重抑制作用所致,并且在细菌感染的啮齿动物模型中表现出疗效。临床前体外和体内研究表明,化合物 3 通过形成反应性代谢物共价标记肝蛋白,因此存在潜在的安全隐患。化合物 3 中的脲部分被认为是形成反应性代谢物的潜在原因,但由于其较差的理化参数,其取代导致失去抗菌活性和/或口服暴露。为了鉴定无反应性代谢物形成潜力的第二代苯并咪唑脲类化合物,我们实施了一种代谢转变策略,该策略侧重于通过在分子的其他部位引入代谢弱点来使代谢远离脲部分。通过这种策略鉴定的苯并咪唑脲 34 表现出与 3 相似的抗菌活性,并且在体内不标记肝蛋白,表明形成反应性代谢物的潜力降低/不存在。

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