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Dependence of Antimicrobial Selectivity and Potency on Oligomer Structure Investigated Using Substrate Supported Lipid Bilayers and Sum Frequency Generation Vibrational Spectroscopy

机译:抗菌素选择性和效能对低聚物结构的影响,使用底物支持的脂质双层和求和频率产生振动光谱法进行研究

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摘要

Sum frequency generation (SFG) vibrational spectroscopy was used to study interactions between solid-supported lipid bilayers mimicking microbial and erythrocyte cellular membranes and synthetic antimicrobial arylamide oligomers named 2, 3, and 4, designed with the facial amphiphilicity common to naturally occurring antimicrobial peptides. The three compounds have the same backbone structure but varied side chains. The inherent interfacial sensitivity of SFG allowed for simultaneous monitoring of lipid ordering in the individual bilayer leaflets and orientation of 2, 3, and 4 upon interaction with the bilayer. Critical concentrations at which the inner leaflet is disrupted were determined for each oligomer. Spectral evidence of the oligomers' interaction with the bilayer below the critical concentrations was also found. Oligomers 2 and 3 tilted toward the bilayer surface normal, in agreement with previous experimental and simulation results. These oligomers selectively interact with microbial membrane models over erythrocyte membrane models, correlating well to previously published SFG studies on antimicrobial oligomer 1. It was shown that the oligomers interact with the lipid bilayers differently, indicating their different activity and selectivity. This research further shows that SFG is a particularly useful technique for the investigation of interaction mechanisms between cell membranes and membrane-active molecules. Additionally, SFG provides details of the specific interactions between these novel antimicrobials and lipid bilayers.
机译:总和频率产生(SFG)振动光谱用于研究模拟微生物和红细胞细胞膜的固体支持脂质双层与名为2,3和4的合成抗微生物芳基酰胺低聚物的相互作用,该低聚物设计具有天然存在的抗微生物肽共有的面部两亲性。这三种化合物具有相同的主链结构,但侧链不同。 SFG固有的界面敏感性允许同时监测各个双层小叶中的脂质排列以及与双层相互作用时2、3和4的方向。对于每种低聚物,确定内部小叶被破坏的临界浓度。还发现了低于临界浓度的低聚物与双层相互作用的光谱证据。与先前的实验和模拟结果一致,低聚物2和3向双层表面法线倾斜。这些寡聚物与微生物膜模型相比于红细胞膜模型选择性地相互作用,这与先前发表的关于抗菌性寡聚物1的SFG研究密切相关。研究表明,寡聚物与脂质双层的相互作用不同,表明它们的活性和选择性不同。这项研究进一步表明,SFG是研究细胞膜与膜活性分子之间相互作用机制的一种特别有用的技术。另外,SFG提供了这些新型抗微生物剂和脂质双层之间特定相互作用的详细信息。

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