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呼吸道合胞病毒F蛋白在病毒样颗粒中的修饰影响B细胞记忆的产生。

Modification of the respiratory syncytial virus f protein in virus-like particles impacts generation of B cell memory.

作者信息

Schmidt Madelyn R, McGinnes-Cullen Lori W, Kenward Sarah A, Willems Kristin N, Woodland Robert T, Morrison Trudy G

机构信息

Department of Microbiology and Physiological Systems/Program in Immunology and Microbiology, University of Massachusetts Medical School, Worcester, Massachusetts, USA.

Department of Microbiology and Physiological Systems/Program in Immunology and Microbiology, University of Massachusetts Medical School, Worcester, Massachusetts, USA

出版信息

J Virol. 2014 Sep 1;88(17):10165-76. doi: 10.1128/JVI.01250-14. Epub 2014 Jun 25.

Abstract

UNLABELLED

Immunization with virus-like particles (VLPs) containing the Newcastle disease virus (NDV) core proteins, NP and M, and two chimera proteins (F/F and H/G) containing the respiratory syncytial virus (RSV) F- and G-protein ectodomains fused to the transmembrane and cytoplasmic domains of NDV F and HN proteins, respectively, stimulated durable RSV-neutralizing antibodies, F-protein-specific long-lived, bone marrow-associated plasma cells (LLPCs), and B cell memory, in striking contrast to RSV infection, which did not (M. R. Schmidt, L. W. McGinnes, S. A. Kenward, K. N. Willems, R. T. Woodland, and T. G. Morrison, J. Virol. 86:11654-11662, 2012). Here we report the characterization of a VLP with an RSV F-protein ectodomain fused to the NDV F-protein heptad repeat 2 (HR2), transmembrane, and cytoplasmic domain sequences, creating a chimera with two tandem HR2 domains, one from the RSV F protein and the other from the NDV F-protein ectodomain (F/HR2F). The F/HR2F chimera protein was efficiently assembled into VLPs along with the H/G chimera protein. This VLP (VLP-H/G+F/HR2F) stimulated anti-F-protein and anti-G-protein IgG, durable RSV-neutralizing antibodies, and anti-RSV F-protein-secreting LLPCs. However, the subtypes of anti-F-protein IgG induced were different from those elicited by VLPs containing the F/F chimera (VLP-H/G+F/F). Most importantly, VLP-H/G+F/HR2F did not induce RSV F-protein-specific B cell memory, as shown by the adoptive transfer of B cells from immunized animals to immunodeficient animals. The VLP did, however, induce B cell memory specific to the RSV G protein. Thus, the form of the F protein has a direct role in inducing anti-F-protein B cell memory.

IMPORTANCE

The development of vaccines for respiratory syncytial virus (RSV) is hampered by a lack of a clear understanding of the requirements for eliciting protective as well as durable human immune responses to virus antigens. The results of this study indicate that the form of the RSV F protein has a direct and significant impact on the type of anti-F-protein IgG antibodies induced and the generation of F-protein-specific memory. Identification of the conformation of the RSV F protein that most effectively stimulates not only LLPCs and but also memory B cells will be important in the future development of RSV vaccines.

摘要

未标记

用含有新城疫病毒(NDV)核心蛋白NP和M的病毒样颗粒(VLP),以及两种嵌合蛋白(F/F和H/G)进行免疫接种,其中F/F和H/G分别是将呼吸道合胞病毒(RSV)F蛋白和G蛋白的胞外结构域与NDV F蛋白和HN蛋白的跨膜及胞质结构域融合而成,可刺激产生持久的RSV中和抗体、F蛋白特异性的长寿骨髓相关浆细胞(LLPC)以及B细胞记忆,这与RSV感染形成鲜明对比,RSV感染不会产生上述结果(M. R. 施密特、L. W. 麦金尼斯、S. A. 肯沃德、K. N. 威廉姆斯、R. T. 伍德兰和T. G. 莫里森,《病毒学杂志》86:11654 - 11662,2012年)。在此,我们报告一种VLP的特性,该VLP将RSV F蛋白胞外结构域与NDV F蛋白七肽重复序列2(HR2)、跨膜及胞质结构域序列融合,形成一种具有两个串联HR2结构域的嵌合体,一个来自RSV F蛋白,另一个来自NDV F蛋白胞外结构域(F/HR2F)。F/HR2F嵌合蛋白与H/G嵌合蛋白一起高效组装成VLP。这种VLP(VLP - H/G + F/HR2F)刺激产生抗F蛋白和抗G蛋白IgG、持久的RSV中和抗体以及抗RSV F蛋白分泌的LLPC。然而,诱导产生的抗F蛋白IgG亚型与含有F/F嵌合体的VLP(VLP - H/G + F/F)所诱导的不同。最重要的是,如将免疫动物的B细胞过继转移至免疫缺陷动物所示,VLP - H/G + F/HR2F未诱导产生RSV F蛋白特异性B细胞记忆。不过,该VLP确实诱导产生了针对RSV G蛋白的B细胞记忆。因此,F蛋白的形式在诱导抗F蛋白B细胞记忆中具有直接作用。

重要性

呼吸道合胞病毒(RSV)疫苗的研发因缺乏对引发针对病毒抗原的保护性及持久人类免疫反应所需条件的清晰认识而受阻。本研究结果表明,RSV F蛋白的形式对诱导产生的抗F蛋白IgG抗体类型以及F蛋白特异性记忆的产生具有直接且显著的影响。鉴定最有效刺激LLPC以及记忆B细胞的RSV F蛋白构象,在RSV疫苗的未来研发中将具有重要意义。

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