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Lipid membrane-binding properties of tryptophan analogues of linear amphipathic beta-sheet cationic antimicrobial peptides using surface plasmon resonance.

机译:线性两亲性β-片状阳离子抗菌肽的色氨酸类似物的脂质膜结合特性,使用表面等离振子共振。

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摘要

Using a surface plasmon resonance (SPR) system, we investigated the lipid membrane-binding properties of four analogues of the 18-residue linear amphipathic beta-sheet cationic antimicrobial peptide (KIGAKI)3-NH2, each of which contains a single isoleucine-to-tryptophan substitution. The results of the SPR study revealed significant differences in the binding characteristics of the peptides depending upon the position of tryptophan residues. These peptides showed higher binding affinity to membranes containing acidic phospholipids than zwitterionic phospholipids. The addition of dimethylsulfoxide to the running buffer was effective in maintaining the solubility of these peptide solutions and obtaining concentration-dependent sensorgrams for the kinetic analysis in this study. The kinetic binding data of SPR correlated closely with both the ability of the peptides to lyse liposomes with the same phospholipid composition and bactericidal activity. The results demonstrate that SPR may be a valuable tool to predict the membrane lytic properties of antimicrobial peptides.
机译:我们使用表面等离振子共振(SPR)系统,调查了18个残基的线性两亲性β-折叠阳离子抗菌肽(KIGAKI)3-NH2的四个类似物的四个脂质膜结合特性,其中每个都包含一个异亮氨酸-色氨酸取代。 SPR研究的结果表明,取决于色氨酸残基的位置,肽的结合特性存在显着差异。与两性离子磷脂相比,这些肽对包含酸性磷脂的膜显示出更高的结合亲和力。向运行缓冲液中添加二甲亚砜可有效维持这些肽溶液的溶解度,并获得用于本研究动力学分析的浓度依赖性传感图。 SPR的动力学结合数据与肽裂解具有相同磷脂组成的脂质体的能力和杀菌活性密切相关。结果表明,SPR可能是预测抗菌肽膜溶解特性的有价值的工具。

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