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首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Structure-activity relationship (SAR) and preliminary mode of action studies of 3-substituted benzylthioquinolinium iodide as anti-opportunistic infection agents
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Structure-activity relationship (SAR) and preliminary mode of action studies of 3-substituted benzylthioquinolinium iodide as anti-opportunistic infection agents

机译:结构-活性关系(SAR)和3-取代的碘化苄基硫喹啉鎓碘作为抗机会感染剂的初步作用方式研究

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摘要

Opportunistic infections are devastating to immunocompromised patients. And in especially sub-Saharan Africa where the AIDS epidemic is still raging, the mortality rate was recently as high as 70%. The paucity of anti-opportunistic drugs, the decreasing efficacy and the development of resistance against the azoles and even amphotericin B have stimulated the search for new drugs with new mechanisms of action. In a previous work, we showed that a new chemotype derived from the natural product cryptolepine displayed selective toxicity against opportunistic pathogens with minimal cytotoxicity to normal cells. In this manuscript, we report the design and synthesis of substituted benzylthioquinolinium iodides, evaluated their anti-infective properties and formulated some initial structure-activity relationships around phenyl ring A from the original natural product. The sensitivity of the most potent analog 10l, to selected strains of C. cerevisiae was also evaluated leading to the observation that this scaffold may have a different mode of action from its predecessor, cryptolepine.
机译:机会感染对免疫功能低下的患者具有毁灭性的影响。在艾滋病流行仍在肆虐的特别是撒哈拉以南非洲地区,死亡率最近高达70%。抗机会药物的匮乏,功效的下降以及对唑类甚至两性霉素B的耐药性的发展刺激了对具有新作用机理的新药物的寻求。在以前的工作中,我们显示了一种衍生自天然产物隐氯平的新化学型,它对机会性病原体具有选择性毒性,对正常细胞的细胞毒性最小。在这份手稿中,我们报告了碘化苄基硫代喹啉鎓碘化物的设计与合成,评估了它们的抗感染性能,并从原始天然产物中围绕苯环A制定了一些初始的结构活性关系。还评估了最有效的类似物10l对啤酒酵母的选定菌株的敏感性,从而导致观察到该支架可能与其前身隐血平具有不同的作用方式。

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