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调节肽-脂质界面上电荷依赖性和折叠介导的抗菌相互作用。

Modulating charge-dependent and folding-mediated antimicrobial interactions at peptide-lipid interfaces.

作者信息

Iavicoli Patrizia, Rossi François, Lamarre Baptiste, Bella Angelo, Ryadnov Maxim G, Calzolai Luigi

机构信息

European Commission, DG Joint Research Centre, Via Enrico Fermi, 2749, Ispra, VA, 21027, Italy.

National Physical Laboratory, Teddington, TW11 0LW, UK.

出版信息

Eur Biophys J. 2017 May;46(4):375-382. doi: 10.1007/s00249-016-1180-8. Epub 2016 Nov 10.

Abstract

Peptide-lipid interactions support a variety of biological functions. Of particular interest are those that underpin fundamental mechanisms of innate immunity that are programmed in host defense or antimicrobial peptide sequences found virtually in all multicellular organisms. Here we synthetically modulate antimicrobial peptide-lipid interactions using an archetypal helical antimicrobial peptide and synthetic membranes mimicking bacterial and mammalian membranes in solution. We probe these interactions as a function of membrane-induced folding, membrane stability and peptide-lipid ratios using a correlative approach encompassing light scattering and spectroscopy measurements such as circular dichroism spectroscopy, fluorescence and nuclear magnetic resonance spectroscopy. The peptide behavior is assessed against that of its anionic counterpart having similar propensities for α-helical folding. The results indicate strong correlations between peptide folding and membrane type, supporting folding-responsive binding of antimicrobial peptides to bacterial membranes. The study provides a straightforward approach for modulating structure-activity relationships in the context of membrane-induced antimicrobial action, thus holding promise for the rational design of potent antimicrobial agents.

摘要

肽 - 脂质相互作用支持多种生物学功能。特别令人感兴趣的是那些支撑先天免疫基本机制的相互作用,这些机制在宿主防御中被编程,或者存在于几乎所有多细胞生物中的抗菌肽序列中。在这里,我们使用一种典型的螺旋抗菌肽和模拟溶液中细菌和哺乳动物膜的合成膜,对抗菌肽 - 脂质相互作用进行合成调节。我们使用包括光散射和光谱测量(如圆二色光谱、荧光和核磁共振光谱)的相关方法,探究这些相互作用与膜诱导折叠、膜稳定性和肽 - 脂质比率的关系。将该肽的行为与其具有相似α - 螺旋折叠倾向的阴离子对应物的行为进行评估比较。结果表明肽折叠与膜类型之间存在强相关性,支持抗菌肽与细菌膜的折叠响应性结合。该研究为在膜诱导抗菌作用的背景下调节构效关系提供了一种直接方法,因此有望合理设计强效抗菌剂。

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