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工程化流感病毒粒子揭示了非血凝素结构蛋白对疫苗介导的保护作用的贡献。

Engineered influenza virions reveal the contributions of non-hemagglutinin structural proteins to vaccine mediated protection.

作者信息

Luo Zhaochen, Girton Alanson W, Heaton Brook E, Heaton Nicholas S

机构信息

Department of Molecular Genetics and Microbiology, Duke University School of Medicine, Durham, North Carolina, USA.

Department of Molecular Genetics and Microbiology, Duke University School of Medicine, Durham, North Carolina, USA

出版信息

J Virol. 2021 Apr 26;95(10). doi: 10.1128/JVI.02021-20. Epub 2021 Mar 3.

Abstract

The development of improved and universal anti-influenza vaccines would represent a major advance in the protection of human health. In order to facilitate the development of such vaccines, understanding how viral proteins can contribute to protection from disease is critical. Much of the previous work to address these questions relied on reductionist systems (i.e. vaccinating with individual proteins or VLPs that contain only a few viral proteins); thus we have an incomplete understanding of how immunity to different subsets of viral proteins contribute to protection. Here, we report the development of a platform in which a single viral protein can be deleted from an authentic viral particle that retains the remaining full complement of structural proteins and viral RNA. As a first study with this system, we chose to delete the major IAV antigen, the hemagglutinin protein, to evaluate how the other components of the viral particle contribute to protection from influenza disease. Our results show that while anti-HA immunity plays a major role in protection from challenge with a vaccine-matched strain, the contributions from other structural proteins were the major drivers of protection against highly antigenically drifted, homosubtypic strains. This work highlights the importance of evaluating the inclusion of non-HA viral proteins in the development of broadly efficacious and long-lasting influenza vaccines.Influenza virus vaccines currently afford short-term protection from viruses that are closely related to the vaccine strains. There is currently much effort to develop improved, next-generation influenza vaccines that elicit broader and longer-lasting protection. While the hemagglutinin protein is the major viral antigen, in this work, we developed an approach with which to evaluate the contributions of the non-hemagglutinin proteins to vaccine mediated protection. Our results indicate that other structural proteins together may help to mediate broad antiviral protection and should be considered in the development of more universal influenza vaccines.

摘要

研发改良型通用抗流感疫苗将是人类健康保护领域的一项重大进展。为推动此类疫苗的研发,了解病毒蛋白如何有助于预防疾病至关重要。此前解决这些问题的许多工作都依赖于简化系统(即接种仅含几种病毒蛋白的单个蛋白或病毒样颗粒);因此,我们对针对病毒蛋白不同亚群的免疫如何促成保护的理解并不完整。在此,我们报告了一个平台的开发,在该平台中可以从保留其余完整结构蛋白和病毒RNA的真实病毒颗粒中删除单个病毒蛋白。作为对该系统的首次研究,我们选择删除主要的甲型流感病毒抗原血凝素蛋白,以评估病毒颗粒的其他成分如何有助于预防流感疾病。我们的结果表明,虽然抗血凝素免疫在预防与疫苗匹配毒株的攻击中起主要作用,但其他结构蛋白的作用是预防高度抗原漂移的同亚型毒株的主要驱动因素。这项工作凸显了在研发广泛有效的长效流感疫苗时评估纳入非血凝素病毒蛋白的重要性。

流感病毒疫苗目前只能对与疫苗毒株密切相关的病毒提供短期保护。目前人们正在大力研发改良型下一代流感疫苗,以引发更广泛、更持久的保护。虽然血凝素蛋白是主要的病毒抗原,但在这项工作中,我们开发了一种方法来评估非血凝素蛋白对疫苗介导保护的贡献。我们的结果表明,其他结构蛋白共同作用可能有助于介导广泛的抗病毒保护,在研发更通用的流感疫苗时应予以考虑。

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