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Alkylated histidine based short cationic antifungal peptides: synthesis, biological evaluation and mechanistic investigations

机译:基于烷基化的组氨酸短阳离子抗真菌肽:合成,生物评价和机械研究

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Current clinically used antifungal agents suffer from several drawbacks that have urgently necessitated the development of new antifungal agents with unusual mechanisms of action. In this context, antifungal peptides (AFPs) open up new perspectives in drug design by providing an entire range of highly selective and nontoxic pharmaceuticals. Here, we report the development of novel short AFPs with the synthesis of two series of tripeptide based compounds named as His(2-alkyl)-Arg-Lys (series I) and His(2-alkyl)-Arg-Arg (series II). The series II peptides were found to be selectively active against Cryptococcus neoformans whereas some peptides displayed encouraging activities against other fungal strains such as Candida albicans , Candida kyfer , Aspergillus niger and Neurospora crassa . The cytotoxic experiments were performed on active compounds using Hek-293 and HeLa cells which exhibited negligible cytotoxic effect up to the highest test concentration. Further, the most potent peptide was subjected to mechanistic studies using TEM analysis. Two sets of SUVs mimicking microbial membrane and mammalian membrane were treated with the most potent peptide. The results of this study were found to be perfectly in corroboration with the antifungal activity in relation to the differences between microbial and mammalian cell membrane composition, thereby, indicating that the reported peptides may also be less susceptible to the common mechanisms of drug resistance.
机译:目前的临床使用的抗真菌剂患有几种缺点,迫切需要具有具有不寻常的作用机制的新抗真菌剂。在这种情况下,通过提供全系列的高度选择性和无毒药物,抗真菌肽(AFP)通过提供药物设计中的新观点。在这里,我们报告了新型短篇小组的开发,合成了两系列的三肽基本的化合物,命名为他(2-烷基) - 氢(系列I)及其(2-烷基) - arg(II系列) )。发现II系列肽选择性针对隐性球菌的新族种,而一些肽展示令其他真菌菌株的令人愉快的活动,例如念珠菌,念珠菌,念珠菌Kyfer,Aspergillus Niger和神经孢子塔。使用HEK-293和HeLa细胞对活性化合物进行细胞毒性实验,其表现出可忽略不计的细胞毒性效应高达最高的测试浓度。此外,使用TEM分析对最有效的肽进行机械研究。用最有效的肽处理两组模仿微生物膜和哺乳动物膜的SUV。发现该研究的结果与微生物和哺乳动物细胞膜组合物之间的抗化活性有关的抗真菌活性,表明报道的肽也可能不易易受耐药机制的影响。

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