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Cationic Amphiphiles with Specificity against Gram-Positive and Gram-Negative Bacteria: Chemical Composition and Architecture Combat Bacterial Membranes

机译:特异性对革兰氏阳性和革兰氏阴性细菌的特异性阳离子两亲性:化学成分和建筑作战细菌膜

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摘要

Small-molecule cationic amphiphiles (CAms) were designed to combat the rapid rise in drug-resistant bacteria. CAms were designed to target and compromise the structural integrity of bacteria membranes, leading to cell rupture and death. Discrete structural features of CAms were varied, and structure-activity relationship studies were performed to guide the rational design of potent antimicrobials with desirable selectivity and cytocompatibility profiles. In particular, the effects of cationic conformational flexibility, hydrophobic domain flexibility, and hydrophobic domain architecture were evaluated. Their influence on antimicrobial efficacy in Gram-positive and Gram-negative bacteria was determined, and their safety profiles were established by assessing their impact on mammalian cells. All CAms have a potent activity against bacteria, and hydrophobic domain rigidity and branched architecture contribute to specificity. The insights gained from this project will aid in the optimization of CAm structures.
机译:小分子阳离子两亲(CAM)设计用于打击耐药细菌的快速升高。凸轮旨在瞄准和损害细菌膜的结构完整性,导致细胞破裂和死亡。变化凸轮的离散结构特征,进行结构 - 活性关系研究,以指导具有理想选择性和细胞相容性的有效抗微生物的合理设计。特别地,评估了阳离子构象灵活性,疏水结构域柔韧性和疏水结构域架构的影响。确定它们对革兰氏阳性和革兰氏阴性细菌的抗菌疗效的影响,并通过评估它们对哺乳动物细胞的影响来确定它们的安全性曲线。所有凸轮均有强效针对细菌的活性,疏水结构域刚度和分支架构有助于特异性。从该项目中获得的见解将有助于优化CAM结构。

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