表达全长病毒蛋白的mcmv疫苗载体在单次接种后提供长期的体液免疫保护

Yeonsu Kim, Xiaoyan Zheng, K. Eschke, M. Chaudhry, F. Bertoglio, A. Tomic, Astrid Krmpotić, M. Hoffmann, Y. Bar-On, J. Boehme, D. Bruder, T. Ebensen, L. Brunotte, S. Ludwig, M. Messerle, Carlos Guzman, O. Mandelboim, Michael Hust, S. Pöhlmann, S. Jonjić, L. Čičin-Šain
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引用次数: 3

摘要

由流感或冠状病毒引起的全球大流行对公共卫生造成严重破坏,并导致高发病率和死亡率。医学上仍然需要针对这些病原体的疫苗。巨细胞病毒(CMV)是一种β-疱疹病毒,可诱导独特的强大免疫反应,在这种免疫反应中,大量抗原特异性CD8 + T细胞终生维持。因此,巨细胞病毒被提出并被研究作为一种新的疫苗载体,用于表达抗原肽或蛋白质,以引发针对许多病原体的保护性细胞免疫反应。制备了两种重组小鼠巨细胞病毒(MCMV)疫苗载体,分别表达甲型流感病毒(MCMV HA)血凝素(HA)和严重急性呼吸综合征冠状病毒2 (MCMV S)刺突蛋白。单次注射表达任一病毒蛋白的mcmv可诱导强效中和抗体反应,且随时间增强。重要的是,接种MCMV HA疫苗的小鼠在流感病毒攻击后免受疾病的保护,我们排除了这种保护是由于记忆T细胞的作用。最后,我们在这里表明,MCMV载体不仅诱导长期的细胞免疫,而且还诱导体液反应,提供长期的免疫保护,以对抗临床相关的呼吸道病原体。
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MCMV-based vaccine vectors expressing full-length viral proteins provide long-term humoral immune protection upon a single-shot vaccination
Global pandemics caused by influenza or coronaviruses cause severe disruptions to public health and lead to high morbidity and mortality. There remains a medical need for vaccines against these pathogens. CMV (cytomegalovirus) is a β-herpesvirus that induces uniquely robust immune responses in which remarkably large populations of antigen-specific CD8 + T cells are maintained for a lifetime. Hence, CMV has been proposed and investigated as a novel vaccine vector for expressing antigenic peptides or proteins to elicit protective cellular immune responses against numerous pathogens. We generated two recombinant murine CMV (MCMV) vaccine vectors expressing hemagglutinin (HA) of influenza A virus (MCMV HA ) or the spike protein of severe acute respiratory syndrome coronavirus 2 (MCMV S ). A single injection of MCMVs expressing either viral protein induced potent neutralizing antibody responses, which strengthened over time. Importantly, MCMV HA -vaccinated mice were protected from illness following challenge with the influenza virus, and we excluded that this protection was due to the effects of memory T cells. Conclusively, we show here that MCMV vectors induce not only long-term cellular immunity but also humoral responses that provide long-term immune protection against clinically relevant respiratory pathogens.
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