Chikungunya virus E2 B domain nanoparticle immunogen elicits homotypic neutralizing antibody in mice

IF 4.5 3区 医学 Q2 IMMUNOLOGY Vaccine Pub Date : 2024-10-15 DOI:10.1016/j.vaccine.2024.126405
Karen Tong , Erica M. Hernandez , Katherine Basore , Daved H. Fremont , Jonathan R. Lai
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Abstract

Alphaviruses are enveloped, positive-sense single-stranded RNA viruses that cause severe human and animal illness. Arthritogenic alphaviruses, such as Chikungunya virus (CHIKV) and Mayaro virus (MAYV), are globally distributed, transmitted by mosquitoes, and can cause rheumatic disease characterized by fever, rash, myalgia, and peripheral polyarthralgia that can persist for years post-infection. These infections can also result in more severe clinical manifestations such as hemorrhage, encephalopathy, and mortality. Several potent monoclonal antibodies (mAbs) with broad neutralizing activity have been shown to bind to the E2 B domain (E2-B) of the alphavirus glycoprotein, suggesting that E2-B epitopes are a site of susceptibility for multiple arthritogenic alphaviruses. However, it is unknown whether E2-B alone can elicit a broadly neutralizing humoral response. Here, we generate and characterize nanoparticle-based immunogens containing CHIKV and MAYV E2-B. Immunization with the CHIKV E2-B nanoparticle elicited sera that were cross-reactive toward CHIKV and MAYV E2-B, but had only homotypic neutralizing activity (serum titer of 1:512) against CHIKV vaccine strain 181/25. Furthermore, immunization with MAYV E2-B nanoparticles elicited non-neutralizing antibody, but sera were cross-reactive for both CHIKV and MAYV E2-B. Our findings suggest that the immunodominant epitopes within CHIKV and MAYV E2-B are bound by cross-reactive, but not cross-neutralizing antibody. Therefore, development of broad E2-B based vaccines that induce broadly neutralizing antibody responses will require engineering to alter the immunodominant landscape.
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奇昆古尼亚病毒 E2 B 结构域纳米颗粒免疫原在小鼠体内激发同型中和抗体
阿尔法病毒是有包膜的正义单链 RNA 病毒,可导致严重的人类和动物疾病。基孔肯雅病毒(CHIKV)和马雅罗病毒(MAYV)等致关节炎阿尔法病毒分布于全球各地,通过蚊子传播,可引起以发热、皮疹、肌痛和外周多关节痛为特征的风湿性疾病,感染后可持续数年。这些感染也可能导致更严重的临床表现,如出血、脑病和死亡。已证明几种具有广泛中和活性的强效单克隆抗体(mAbs)能与阿尔法病毒糖蛋白的 E2 B 结构域(E2-B)结合,这表明 E2-B 表位是多种致关节炎阿尔法病毒的易感位点。然而,E2-B本身是否能引起广泛的中和体液反应还不得而知。在这里,我们生成并鉴定了含有CHIKV和MAYV E2-B的纳米颗粒免疫原。用CHIKV E2-B纳米颗粒免疫可引起对CHIKV和MAYV E2-B交叉反应的血清,但对CHIKV疫苗株181/25只有同型中和活性(血清滴度为1:512)。此外,用 MAYV E2-B 纳米颗粒免疫可产生非中和抗体,但血清对 CHIKV 和 MAYV E2-B 均有交叉反应。我们的研究结果表明,CHIKV 和 MAYV E2-B 中的免疫优势表位会与交叉反应抗体结合,但不会与交叉中和抗体结合。因此,要开发能诱导广泛中和抗体反应的基于 E2-B 的广谱疫苗,就需要通过工程设计来改变免疫优势表位。
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来源期刊
Vaccine
Vaccine 医学-免疫学
CiteScore
8.70
自引率
5.50%
发文量
992
审稿时长
131 days
期刊介绍: Vaccine is unique in publishing the highest quality science across all disciplines relevant to the field of vaccinology - all original article submissions across basic and clinical research, vaccine manufacturing, history, public policy, behavioral science and ethics, social sciences, safety, and many other related areas are welcomed. The submission categories as given in the Guide for Authors indicate where we receive the most papers. Papers outside these major areas are also welcome and authors are encouraged to contact us with specific questions.
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