Immunogenicity and protection of a triple repeat domain III mRNA vaccine against Zika virus

IF 4.5 3区医学 Q2 IMMUNOLOGY

Vaccine Pub Date : 2024-11-14 DOI:10.1016/j.vaccine.2024.126518

Yu-Sun Lee , Mi Sun Cheong , Jisun Lee , Eun-Kyoung Bang , Sang In Park , Hyo-Jung Park , Seo-Hyeon Bae , Subin Yoon , Gahyun Roh , Seonghyun Lee , Youngran Cho , Dahyeon Ha , Ayoung Oh , Soo-Yeon Lee , Eun-Jin Choi , Huijeong Choi , Sohee Jo , Yeeun Lee , Jungmin Kim , Hye Won Kwak , Wonil Kim

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引用次数: 0

Abstract

Zika virus (ZIKV) infection is primarily transmitted by mosquitoes and often asymptomatic in most individuals. Infection during pregnancy can lead to severe birth defects such as congenital microcephaly, and currently, there is no approved vaccine for ZIKV. Several studies are investigating the development of ZIKV vaccine using DNA and RNA as well as recombinant protein technologies; however, the outcomes thus far have not been consistently noteworthy. In this study, we designed an mRNA vaccine for ZIKV and evaluated its immunogenicity using a mouse model. Our vaccine, termed 3xEIII, encodes a triple repeat of domain III from the ZIKV E protein. We effectively encapsulated the mRNA within lipid nanoparticles (LNPs), administered 3xEIII to mice via two intramuscular injections, and assessed the induced humoral and cellular immune responses. Specifically, the vaccine elicited neutralizing antibodies that effectively eliminated ZIKV from the organs of challenged mice. Notably, 3xEIII conferred both protective effects and long-term immunity. In subsequent challenges conducted 40 weeks after boosting, immunized mice experienced temporary weight loss but showed significantly reduced viral titers in target organs by the 9th day post-infection. Conclusively from these findings, 3xEIII stands out as a promising noteworthy mRNA vaccine candidate for Zika virus.

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三重重复结构域 III mRNA 疫苗对寨卡病毒的免疫原性和保护作用。

寨卡病毒（ZIKV）感染主要通过蚊子传播，大多数人通常没有症状。怀孕期间感染寨卡病毒可导致严重的先天缺陷，如先天性小头畸形。有几项研究正在利用 DNA 和 RNA 以及重组蛋白技术开发 ZIKV 疫苗，但迄今为止尚未取得显著成果。在本研究中，我们设计了一种针对 ZIKV 的 mRNA 疫苗，并利用小鼠模型评估了其免疫原性。我们的疫苗被称为 3xEIII，它编码了 ZIKV E 蛋白结构域 III 的三重重复。我们将 mRNA 有效地封装在脂质纳米颗粒（LNPs）中，通过两次肌肉注射给小鼠注射 3xEIII，并评估了诱导的体液和细胞免疫反应。具体来说，疫苗激发的中和抗体能有效清除受试小鼠器官中的 ZIKV。值得注意的是，3xEIII 可产生保护作用和长期免疫力。在强化 40 周后进行的后续挑战中，免疫小鼠出现暂时性体重减轻，但在感染后第 9 天，目标器官中的病毒滴度显著降低。这些研究结果表明，3xEIII 是一种很有前景的寨卡病毒 mRNA 候选疫苗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Vaccine 医学-免疫学

CiteScore

8.70

自引率

5.50%

发文量

992

审稿时长

131 days

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