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色氨酸和精氨酸丰富的抗菌肽与外膜的相互作用——一种分子模拟方法。

Interaction of Tryptophan- and Arginine-Rich Antimicrobial Peptide with Outer Membrane-A Molecular Simulation Approach.

机构信息

Department of Computational Physics and Information Technologies, Horia Hulubei National Institute for R&D in Physics and Nuclear Engineering, 077125 Magurele, Romania.

Department of Life and Environmental Physics, Horia Hulubei National Institute for R&D in Physics and Nuclear Engineering, 077125 Magurele, Romania.

出版信息

Int J Mol Sci. 2023 Jan 19;24(3):2005. doi: 10.3390/ijms24032005.

Abstract

A short antimicrobial peptide (AMP), rich in tryptophan and arginine (P6-HRWWRWWRR-NH2), was used in molecular dynamics (MD) simulations to investigate the interaction between AMPs and lipopolysaccharides (LPS) from two outer membrane (OM) membrane models. The OM of Gram-negative bacteria is an asymmetric bilayer, with the outer layer consisting exclusively of lipopolysaccharide molecules and the lower leaflet made up of phospholipids. The mechanisms by which short AMPs permeate the OM of Gram-negative bacteria are not well understood at the moment. For this study, two types of OM membrane models were built with () smooth LPS composed of lipid A, K12 core and O21 O-antigen, and () rough type LPS composed of lipid A and R1 core. An OmpF monomer from was embedded in both membrane models. MD trajectories revealed that AMP insertion in the LPS layer was facilitated by the OmpF-created gap and allowed AMPs to form hydrogen bonds with the phosphate groups of inner core oligosaccharides. OM proteins such as OmpF may be essential for the permeation of short AMPs such as P6 by exposing the LPS binding site or even by direct translocation of AMPs across the OM.

摘要

一种富含色氨酸和精氨酸的短抗菌肽(AMP)(P6-HRWWRWWRR-NH2),被用于分子动力学(MD)模拟,以研究 AMP 与来自两种外膜(OM)膜模型的脂多糖(LPS)之间的相互作用。革兰氏阴性菌的外膜是一种不对称双层结构,外层仅由脂多糖分子组成,而下层由磷脂组成。目前,人们对短 AMP 如何穿透革兰氏阴性菌的 OM 还不太了解。在这项研究中,使用两种类型的 OM 膜模型进行构建:()由脂多糖 A、K12 核心和 O21 O-抗原组成的平滑 LPS,和()由脂多糖 A 和 R1 核心组成的粗糙 LPS。来自 的一个 OmpF 单体被嵌入这两种膜模型中。MD 轨迹表明,OmpF 形成的间隙促进了 AMP 插入 LPS 层,使 AMP 能够与内部核心寡糖的磷酸基团形成氢键。OmpF 等 OM 蛋白对于短 AMP 如 P6 的渗透可能是必不可少的,它可以暴露 LPS 结合位点,甚至可以通过直接将 AMP 穿过 OM 进行转运。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47ff/9916935/6a8a499429b7/ijms-24-02005-g001.jpg

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