Gold(I) Phosphine Derivatives with Improved Selectivity as Topically Active Drug Leads to Overcome 5-Nitroheterocyclic Drug Resistance in Trichomonas vaginalis

阴道毛滴虫 化学 抗药性 药品 滴虫性阴道炎 药理学 选择性 磷化氢 微生物学 立体化学 组合化学 有机化学 生物 医学 催化作用
作者
Yukiko Miyamoto,Shubhangi Aggarwal,Jeff Joseph A. Celaje,Sozaburo Ihara,Jonathan Ang,Dmitry B. Eremin,Kirkwood M. Land,Lisa A. Wrischnik,Liangfang Zhang,Valery V. Fokin,Lars Eckmann
出处
期刊:Journal of Medicinal Chemistry [American Chemical Society]
卷期号:64 (10): 6608-6620 被引量:11
标识
DOI:10.1021/acs.jmedchem.0c01926
摘要

Trichomonas vaginalis causes the most common, nonviral sexually transmitted infection. Only metronidazole (Mz) and tinidazole are approved for treating trichomoniasis, yet resistance is a clinical problem. The gold(I) complex, auranofin, is active against T. vaginalis and other protozoa but has significant human toxicity. In a systematic structure–activity exploration, we show here that diversification of gold(I) complexes, particularly as halides with simple C1–C3 trialkyl phosphines or as bistrialkyl phosphine complexes, can markedly improve potency against T. vaginalis and selectivity over human cells compared to that of the existing antirheumatic gold(I) drugs. All gold(I) complexes inhibited the two most abundant isoforms of the presumed target enzyme, thioredoxin reductase, but a subset of compounds were markedly more active against live T. vaginalis than the enzyme, suggesting that alternative targets exist. Furthermore, all tested gold(I) complexes acted independently of Mz and were able to overcome Mz resistance, making them candidates for the treatment of Mz-refractory trichomoniasis.

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