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F NMR 研究为李斯特菌溶血素 O(一种来自李斯特菌的孔形成毒素)与脂质膜相互作用提供了深入了解。

F NMR studies provide insights into lipid membrane interactions of listeriolysin O, a pore forming toxin from Listeria monocytogenes.

机构信息

Department of Molecular Biology and Nanobiotechnology, National Institute of Chemistry, Hajdrihova 19, 1000, Ljubljana, Slovenia.

Graduate School of Biomedicine, Medical faculty, University of Ljubljana, 1000, Ljubljana, Slovenia.

出版信息

Sci Rep. 2018 May 2;8(1):6894. doi: 10.1038/s41598-018-24692-6.

Abstract

Listeria monocytogenes is a mammalian pathogen that causes gastroenteritis, miscarriages and infections of the central nervous system in immunocompromised individuals. Its main virulence factor is listeriolysin O (LLO), a pore-forming cholesterol-dependent cytolysin (CDC), which enables bacterial escape from the phagolysosome and contributes to bacterial pathogenicity. Details of cholesterol (Chol) recognition and membrane binding mechanisms by LLO are still not known. Here we used F-NMR spectroscopy in order to assess LLO-Chol interactions in solution and in a Chol-rich membrane environment. LLO has six tryptophan residues located in the region of the molecule that is first in contact with lipid membranes. F-LLO, which contained 5-fluoro-tryptophans, was prepared by using isotopic labelling in an E. coli expression system. Signals in the F-NMR spectrum of F-LLO were unambiguously assigned by using a series of single Trp → Phe point mutations. The results employing various cholesterol preparations in solution indicate that tryptophan residues are not directly involved in Chol binding in solution. However, significant chemical shift changes were observed upon LLO binding to Chol-rich membranes, highlighting the role of tryptophan residues in membrane interactions (W512) and oligomerisation (W189 and W489).

摘要

李斯特菌是一种哺乳动物病原体,可引起免疫功能低下个体的肠胃炎、流产和中枢神经系统感染。其主要毒力因子是溶血素 O(LLO),一种形成孔的胆固醇依赖性细胞溶素(CDC),可使细菌从吞噬体中逃脱,并有助于细菌的致病性。LLO 识别胆固醇(Chol)和与膜结合的机制的细节尚不清楚。在这里,我们使用 F-NMR 光谱来评估 LLO-Chol 在溶液中和富含 Chol 的膜环境中的相互作用。LLO 有六个色氨酸残基位于与脂质膜首先接触的分子区域。通过在大肠杆菌表达系统中使用同位素标记制备了含有 5-氟色氨酸的 F-LLO。通过使用一系列单色氨酸到苯丙氨酸点突变,F-NMR 光谱中的信号得到了明确的归属。在溶液中使用各种胆固醇制剂的结果表明,色氨酸残基在溶液中不直接参与 Chol 结合。然而,LLO 与富含 Chol 的膜结合时观察到明显的化学位移变化,突出了色氨酸残基在膜相互作用(W512)和寡聚化(W189 和 W489)中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b186/5931962/49cae8f94198/41598_2018_24692_Fig1_HTML.jpg

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