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创伤弧菌溶血素凝集素的聚糖特异性勾勒出一个毒素家族膜靶向的进化史。

Glycan specificity of the Vibrio vulnificus hemolysin lectin outlines evolutionary history of membrane targeting by a toxin family.

作者信息

Kaus Katherine, Lary Jeffrey W, Cole James L, Olson Rich

机构信息

Department of Molecular Biology and Biochemistry, Wesleyan University, 52 Lawn Avenue, Middletown, CT 06459, USA.

Biotechnology-Bioservices Center, University of Connecticut, Storrs, CT 06269, USA.

出版信息

J Mol Biol. 2014 Jul 29;426(15):2800-12. doi: 10.1016/j.jmb.2014.05.021. Epub 2014 May 24.

DOI:10.1016/j.jmb.2014.05.021
PMID:24862282
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4102649/
Abstract

Pore-forming toxins (PFTs) are a class of pathogen-secreted molecules that oligomerize to form transmembrane channels in cellular membranes. Determining the mechanism for how PFTs bind membranes is important in understanding their role in disease and for developing possible ways to block their action. Vibrio vulnificus, an aquatic pathogen responsible for severe food poisoning and septicemia in humans, secretes a PFT called V. vulnificus hemolysin (VVH), which contains a single C-terminal targeting domain predicted to resemble a β-trefoil lectin fold. In order to understand the selectivity of the lectin for glycan motifs, we expressed the isolated VVH β-trefoil domain and used glycan-chip screening to identify that VVH displays a preference for terminal galactosyl groups including N-acetyl-d-galactosamine and N-acetyl-d-lactosamine. The X-ray crystal structure of the VVH lectin domain solved to 2.0Å resolution reveals a heptameric ring arrangement similar to the oligomeric form of the related, but inactive, lectin from Vibrio cholerae cytolysin. Structures bound to glycerol, N-acetyl-d-galactosamine, and N-acetyl-d-lactosamine outline a common and versatile mode of recognition allowing VVH to target a wide variety of cell-surface ligands. Sequence analysis in light of our structural and functional data suggests that VVH may represent an earlier step in the evolution of Vibrio PFTs.

摘要

成孔毒素(PFTs)是一类由病原体分泌的分子,它们会寡聚化以在细胞膜中形成跨膜通道。确定PFTs与膜结合的机制对于理解它们在疾病中的作用以及开发可能的方法来阻断其作用至关重要。创伤弧菌是一种导致人类严重食物中毒和败血症的水生病原体,它会分泌一种名为创伤弧菌溶血素(VVH)的PFT,该毒素含有一个预测类似于β-三叶凝集素折叠的单一C末端靶向结构域。为了了解凝集素对聚糖基序的选择性,我们表达了分离的VVHβ-三叶结构域,并使用聚糖芯片筛选来确定VVH对包括N-乙酰-D-半乳糖胺和N-乙酰-D-乳糖胺在内的末端半乳糖基具有偏好性。解析到2.0Å分辨率的VVH凝集素结构域的X射线晶体结构揭示了一种七聚体环排列,类似于来自霍乱弧菌细胞毒素的相关但无活性的凝集素的寡聚形式。与甘油、N-乙酰-D-半乳糖胺和N-乙酰-D-乳糖胺结合的结构勾勒出一种常见且通用的识别模式,使VVH能够靶向多种细胞表面配体。根据我们的结构和功能数据进行的序列分析表明,VVH可能代表了弧菌PFTs进化的早期阶段。

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