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激活型FcγR在M2e特异性IgG1和IgG2a抗体预防流感疾病中的分层和冗余作用

Hierarchical and Redundant Roles of Activating FcγRs in Protection against Influenza Disease by M2e-Specific IgG1 and IgG2a Antibodies.

作者信息

Van den Hoecke Silvie, Ehrhardt Katrin, Kolpe Annasaheb, El Bakkouri Karim, Deng Lei, Grootaert Hendrik, Schoonooghe Steve, Smet Anouk, Bentahir Mostafa, Roose Kenny, Schotsaert Michael, Schepens Bert, Callewaert Nico, Nimmerjahn Falk, Staeheli Peter, Hengel Hartmut, Saelens Xavier

机构信息

Medical Biotechnology Center, VIB, Ghent, Belgium.

Department of Biomedical Molecular Biology, Ghent University, Ghent, Belgium.

出版信息

J Virol. 2017 Mar 13;91(7). doi: 10.1128/JVI.02500-16. Print 2017 Apr 1.

Abstract

The ectodomain of matrix protein 2 is a universal influenza A virus vaccine candidate that provides protection through antibody-dependent effector mechanisms. Here we compared the functional engagement of Fcγ receptor (FcγR) family members by two M2e-specific monoclonal antibodies (MAbs), MAb 37 (IgG1) and MAb 65 (IgG2a), which recognize a similar epitope in M2e with similar affinities. The binding of MAb 65 to influenza A virus-infected cells triggered all three activating mouse Fcγ receptors , whereas MAb 37 activated only FcγRIII. The passive transfer of MAb 37 or MAb 65 in wild-type, , , and BALB/c mice revealed the importance of these receptors for protection against influenza A virus challenge, with a clear requirement of FcγRIII for IgG1 MAb 37 being found. We also report that FcγRIV contributes to protection by M2e-specific IgG2a antibodies. There is increased awareness that protection by antibodies directed against viral antigens is also mediated by the Fc domain of these antibodies. These Fc-mediated effector functions are often missed in clinical assays, which are used, for example, to define correlates of protection induced by vaccines. The use of antibodies to prevent and treat infectious diseases is on the rise and has proven to be a promising approach in our battle against newly emerging viral infections. It is now also realized that Fcγ receptors significantly enhance the protective effect of broadly neutralizing antibodies directed against the conserved parts of the influenza virus hemagglutinin. We show here that two M2e-specific monoclonal antibodies with close to identical antigen-binding specificities and affinities have a very different protective potential that is controlled by their capacity to interact with activating Fcγ receptors.

摘要

基质蛋白2的胞外结构域是一种通用的甲型流感病毒疫苗候选物,可通过抗体依赖性效应机制提供保护。在此,我们比较了两种M2e特异性单克隆抗体(MAb),即MAb 37(IgG1)和MAb 65(IgG2a)对Fcγ受体(FcγR)家族成员的功能参与情况,这两种抗体以相似的亲和力识别M2e中相似的表位。MAb 65与甲型流感病毒感染细胞的结合触发了所有三种活化的小鼠Fcγ受体,而MAb 37仅激活FcγRIII。在野生型、、和BALB/c小鼠中被动转移MAb 37或MAb 65揭示了这些受体对抵抗甲型流感病毒攻击的保护作用的重要性,发现IgG1 MAb 37对FcγRIII有明确需求。我们还报告说,FcγRIV有助于M2e特异性IgG2a抗体提供保护。人们越来越意识到,针对病毒抗原的抗体所提供的保护也由这些抗体的Fc结构域介导。这些Fc介导的效应功能在临床检测中常常被忽视,例如,临床检测用于定义疫苗诱导的保护相关性。使用抗体预防和治疗传染病的情况正在增加,并且已被证明是我们对抗新出现的病毒感染的一种有前景的方法。现在人们还认识到,Fcγ受体显著增强了针对流感病毒血凝素保守部分的广泛中和抗体的保护作用。我们在此表明,两种具有几乎相同抗原结合特异性和亲和力的M2e特异性单克隆抗体具有非常不同的保护潜力,这由它们与活化Fcγ受体相互作用的能力所控制。

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