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利用脂质单分子层和支持的仿生膜探索生物活性肽菌素a的膜机制。

Exploring the membrane mechanism of the bioactive peptaibol ampullosporin a using lipid monolayers and supported biomimetic membranes.

作者信息

Eid Marguerita, Rippa Sonia, Castano Sabine, Desbat Bernard, Chopineau Joël, Rossi Claire, Béven Laure

机构信息

UMR 6022 CNRS Génie Enzymatique et Cellulaire, Université de Technologie de Compiègne, BP 20529, 60205 Compiègne Cedex, France.

出版信息

J Biophys. 2010;2010:179641. doi: 10.1155/2010/179641. Epub 2011 Feb 17.

Abstract

Ampullosporin A is an antimicrobial, neuroleptic peptaibol, the behavior of which was investigated in different membrane mimetic environments made of egg yolk L-α-phosphatidylcholine. In monolayers, the peptaibol adopted a mixed α/3(10)-helical structure with an in-plane orientation. The binding step was followed by the peptide insertion into the lipid monolayer core. The relevance of the inner lipid leaflet nature was studied by comparing ampullosporin binding on a hybrid bilayer, in which this leaflet was a rigid alkane layer, and on supported fluid lipid bilayers. The membrane binding was examined by surface plasmon resonance spectroscopy and the effect on lipid dynamics was explored using fluorescence recovery after photobleaching. In the absence of voltage and at low concentration, ampullosporin A substantially adsorbed onto lipid surfaces and its interaction with biomimetic models was strongly modified depending on the inner leaflet structure. At high concentration, ampullosporin A addition led to the lipid bilayers disruption.

摘要

安普洛孢菌素A是一种抗菌、抗精神病的肽抗生素,其行为在由蛋黄L-α-磷脂酰胆碱制成的不同膜模拟环境中进行了研究。在单层膜中,该肽抗生素采用了具有面内取向的混合α/3(10)-螺旋结构。结合步骤之后是肽插入脂质单层核心。通过比较安普洛孢菌素在混合双层膜(其中内层小叶为刚性烷烃层)和支持的流体脂质双层膜上的结合情况,研究了内层脂质小叶性质的相关性。通过表面等离子体共振光谱检查膜结合,并使用光漂白后的荧光恢复来探索对脂质动力学的影响。在没有电压且浓度较低的情况下,安普洛孢菌素A大量吸附在脂质表面,并且其与仿生模型的相互作用根据内层小叶结构而强烈改变。在高浓度下,添加安普洛孢菌素A会导致脂质双层膜破坏。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/23c2/3042626/d093f38d057a/JBP2010-179641.001.jpg

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