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流感病毒血凝素的构象调制:单体形式的特征描述和体内功效。

Conformational modulation of influenza virus hemagglutinin: characterization and in vivo efficacy of monomeric form.

机构信息

Department of Biotechnology & Bioinformatics, Korea University, Sejong, 30019, Korea.

Department of Food and Nutrition, Duksung Women's University, Seoul, 01369, Korea.

出版信息

Sci Rep. 2017 Aug 8;7(1):7540. doi: 10.1038/s41598-017-08021-x.

Abstract

Mutational changes that mostly occur at the head region of hemagglutinin (HA) lead to the emergence of new epidemic influenza viruses, whereas HA antigens have been modified to generate broadly neutralizing antibodies toward highly conserved epitopes in the HA stem. Interestingly, a recent analysis of serum antibody repertoires showed that broadly neutralizing antibodies bind to HA monomer at a conserved region occluded at the intermonomer interface of HA trimer and confer protection in animal models. We showed previously that the recombinant HA ectodomain from a pandemic strain A/Korea/01/2009 was monomeric in solution and crystal structure. In order to examine the potential antigenicity of a monomeric form, we designed HA monomer that incorporates mutations to destabilize trimer conformations. Starting with the HA trimer from a seasonal strain A/Thailand/CU44/2006, mutations were introduced at the intermonomer interface, Ser199 of HA1 and Gly47, Arg75, Phe88, Val91, and Arg106 of HA2. Two mutants, F88E and V91W, were characterized to form a monomer and their double mutant F88E/V91W monomer was selected as an antigen. Animal studies showed that the HA monomer induced protective immunity in vivo, comparable to the trimer, albeit low antibody titers in sera.

摘要

主要发生在血凝素 (HA) 头部区域的突变导致新的流行流感病毒的出现,而 HA 抗原已被修饰以产生针对 HA 茎中高度保守表位的广泛中和抗体。有趣的是,最近对血清抗体库的分析表明,广泛中和抗体结合到 HA 单体在 HA 三聚体的单体间界面被掩盖的保守区域,并在动物模型中赋予保护。我们之前表明,来自大流行株 A/Korea/01/2009 的重组 HA 外域在溶液中和晶体结构中是单体形式。为了检查单体形式的潜在抗原性,我们设计了包含突变以破坏三聚体构象的 HA 单体。从季节性株 A/Thailand/CU44/2006 的 HA 三聚体开始,在单体间界面、HA1 的 Ser199 和 HA2 的 Gly47、Arg75、Phe88、Val91 和 Arg106 处引入突变。两种突变体 F88E 和 V91W 被表征为形成单体,并且选择其双突变体 F88E/V91W 单体作为抗原。动物研究表明,HA 单体在体内诱导了保护性免疫,与三聚体相当,尽管血清中的抗体滴度较低。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a5c5/5548806/ddf71ca677d3/41598_2017_8021_Fig1_HTML.jpg

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