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Antifungal activity, mode of action variability, and subcellular distribution of coumarin-based antifungal azoles

机译:抗真菌活性,作用模式可变性和基于香豆素的抗真菌唑的亚细胞分布

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Azole antifungals inhibit the biosynthesis of ergosterol, the fungal equivalent of cholesterol in mammalian cells. Here we report an investigation of the activity of coumarin-substituted azole antifungals. Screening against a panel of Candida pathogens, including a mutant lacking CYP51, the target of antifungal azoles, revealed that this enzyme is inhibited by triazole-based antifungals, whereas imidazole-based derivatives have more than one mode of action. The imidazole-bearing antifungals more effectively reduced trailing growth associated with persistence and/or recurrence of fungal infections than triazole-based derivatives. The imidazole derivatives were more toxic to mammalian cells and more potently inhibited the activity of CYP3A4, which is one of the main causes of azole toxicity. Using live cell imaging, we showed that regardless of the type of azole ring fluorescent 7-diethylaminocoumarin-based azoles localized to the endoplasmic reticulum, the organelle that harbors CYP51. This study suggests that the coumarin is a promising scaffold for development of novel azole-based antifungals that effectively localize to the fungal cell endoplasmic reticulum. (C) 2019 Elsevier Masson SAS. All rights reserved.
机译:唑脂肪酶抑制Ergosterol的生物合成,哺乳动物细胞中的真菌等同物的胆固醇。在这里,我们报告了对香豆素取代的唑唑抗真菌活性的研究。筛选念珠菌病原体,包括缺乏CYP51的突变体,抗真菌唑的靶标显示,基于三唑基的抗真菌抑制该酶,而基于咪唑基的衍生物具有多于一种动作模式。含咪唑的抗真菌更有效地减少了与真菌感染的持续和/或复发相关的尾后生长,而不是基于三唑基衍生物。咪唑衍生物对哺乳动物细胞的毒性更大,并且更棘手抑制CYP3A4的活性,这是唑唑毒性的主要原因之一。使用直播细胞成像,我们表明,无论均唑环荧光7-二乙基氨基脲素marin的基于内质网的吡啉,内部质子,哈勃CYP51的细胞器。本研究表明,香豆素是一种有前途的支架,用于开发新型唑类抗真菌的抗真菌,有效地定位于真菌细胞内质网。 (c)2019年Elsevier Masson SAS。版权所有。

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