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Protection against Respiratory Syncytial Virus by Inactivated Influenza Virus Carrying a Fusion Protein Neutralizing Epitope in a chimeric hemagglutinin

机译:在嵌合血凝素中携带融合蛋白中和表位的灭活流感病毒对呼吸道合胞病毒的防护

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摘要

A desirable vaccine against respiratory syncytial virus (RSV) should induce neutralizing antibodies without eliciting abnormal T cell responses to avoid vaccine-enhanced pathology. In an approach to deliver RSV neutralizing epitopes without RSV-specific T cell antigens, we genetically engineered chimeric influenza virus expressing RSV F262-276 neutralizing epitopes in the globular head domain as a chimeric hemagglutinin (HA) protein. Immunization of mice with formalin-inactivated recombinant chimeric influenza/RSV F262-276 was able to induce RSV protective neutralizing antibodies and lower lung viral loads after challenge. Formalin-inactivated RSV immune mice showed high levels of pulmonary inflammatory cytokines, macrophages, IL-4-producing T cells, and extensive histopathology. However, RSV-specific T cell responses and enhancement of pulmonary histopathology were not observed after RSV infection of inactivated chimeric influenza/RSV F262-276. This study provides evidence that an inactivated vaccine platform of chimeric influenza/RSV virus can be developed into a safe RSV vaccine candidate without priming RSV-specific T cells and immunopathology.
机译:一种理想的抗呼吸道合胞病毒(RSV)的疫苗应诱导中和抗体而不会引起异常的T细胞应答,从而避免疫苗增强的病理。在不提供RSV特异性T细胞抗原的情况下提供RSV中和性抗原表位的方法中,我们对嵌合流感病毒进行了基因工程改造,在球状头部结构域中将RSV F262-276中和性表位表达为嵌合血凝素(HA)蛋白。用福尔马林灭活的重组嵌合流感/ RSV F262-276免疫小鼠能够诱导RSV保护性中和抗体并降低攻击后的肺病毒载量。福尔马林灭活的RSV免疫小鼠表现出高水平的肺炎性细胞因子,巨噬细胞,产生IL-4的T细胞和广泛的组织病理学。然而,灭活的嵌合流感/ RSV F262-276的RSV感染后,未观察到RSV特异性T细胞反应和肺组织病理学增强。这项研究提供的证据表明,无需启动RSV特异性T细胞和免疫病理学,就可以将嵌合流感/ RSV病毒的灭活疫苗平台开发成安全的RSV疫苗候选者。

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