一种经工程改造的日本脑炎病毒信使核糖核酸-脂质纳米颗粒免疫制剂可在小鼠体内诱导保护性免疫。
An engineered Japanese encephalitis virus mRNA-lipid nanoparticle immunization induces protective immunity in mice.
作者信息
Zhu Jiayang, He Caiying, Liu Yusha, Chen Min, Zhang Jiayi, Chen Dong, Ni Hongxia, Wen Jinsheng
机构信息
School of Basic Medical Sciences, Health Science Center, Ningbo University, Ningbo, China.
Wenzhou Central Blood Station, Wenzhou, China.
出版信息
Front Microbiol. 2024 Nov 11;15:1472824. doi: 10.3389/fmicb.2024.1472824. eCollection 2024.
INTRODUCTION
Japanese encephalitis virus (JEV) and Zika virus (ZIKV) pose a severe threat to human health. Our previous research results, as well as those of other research groups, indicated that antibodies (Abs) induced by JEV infection or JEV vaccine vaccination could enhance ZIKV infection and exacerbate the mortality of ZIKV-infected mice, vice versa, which is known as antibody-dependent enhancement (ADE). Although studies on other flaviviruses revealed that altering the amino acid residues located in the fusion loop (FL) of envelope (E) protein can reduce the level of flavivirus-cross-reactive Abs, thereby abating the ADE of heterologous flavivirus infection, it is unclear whether this strategy is equally applicable to JEV.
METHODS
In this study, we constructed recombinant adenoviruses and nucleotide-modified mRNA-lipid nanoparticle (LNP) encoding JEV wild-type E protein or E protein mutant (designated as Ad5-JEV-E and Ad5-JEV-E; JEV-E mRNA-LNP, and JEV-E mRNA-LNP). We evaluated the immunogenicity of these vaccine candidates in mice and the capacity of vaccine-immune mouse sera to neutralize JEV infection or mediate ADE of ZIKV infection and .
RESULTS
Ad5-JEV-E or JEV-E mRNA-LNP immunization induced ZIKV-cross-reactive Ab response which is dramatically lower than that induced by Ad5-JEV-E and JEV-E mRNA-LNP, respectively. The levels of JEV-neutralizing Abs induced by Ad5-JEV-E or JEV-E mRNA-LNP are comparable to that induced by Ad5-JEV-E and JEV-E mRNA-LNP, respectively. The ability of Abs induced by Ad5-JEV-E to enhance ZIKV infection is attenuated as compared with that induced by Ad5-JEV-E. Moreover, JEV-E mRNA-LNP immunization elicited potent T cell response similar to JEV-E mRNA-LNP in mice. Mice immunized with each mRNA-LNP exhibited lower level of serum viral load than the mock-immunized mice post JEV challenge. Mice receiving JEV-E mRNA-LNP-immune mouse sera exhibited ADE post ZIKV challenge whereas passively transferred JEV-E mRNA-LNP-immune mouse sera did not lead to obvious ADE of ZIKV infection in recipient mice. Most importantly, maternally acquired Abs did not enhance the mortality of 1-day-old neonates born to JEV-E mRNA-LNP-immunized mice post ZIKV challenge.
DISCUSSION
These results suggest that optimizing the FL sequence of JEV could significantly reduce the level of JEV/ZIKV-cross-reactive Abs and abrogate the ADE of ZIKV infection, providing a promising strategy to develop effective and safety JEV vaccine.
引言
日本脑炎病毒(JEV)和寨卡病毒(ZIKV)对人类健康构成严重威胁。我们之前的研究结果以及其他研究小组的结果表明,JEV感染或JEV疫苗接种诱导产生的抗体(Abs)可增强ZIKV感染并加剧ZIKV感染小鼠的死亡率,反之亦然,这被称为抗体依赖性增强(ADE)。尽管对其他黄病毒的研究表明,改变包膜(E)蛋白融合环(FL)中的氨基酸残基可降低黄病毒交叉反应性抗体的水平,从而减轻异源黄病毒感染的ADE,但尚不清楚该策略是否同样适用于JEV。
方法
在本研究中,我们构建了编码JEV野生型E蛋白或E蛋白突变体的重组腺病毒和核苷酸修饰的mRNA-脂质纳米颗粒(LNP)(分别命名为Ad5-JEV-E和Ad5-JEV-E;JEV-E mRNA-LNP和JEV-E mRNA-LNP)。我们评估了这些候选疫苗在小鼠中的免疫原性以及疫苗免疫小鼠血清中和JEV感染或介导ZIKV感染ADE的能力。
结果
Ad5-JEV-E或JEV-E mRNA-LNP免疫诱导的ZIKV交叉反应性抗体反应分别明显低于Ad5-JEV-E和JEV-E mRNA-LNP诱导的反应。Ad5-JEV-E或JEV-E mRNA-LNP诱导的JEV中和抗体水平分别与Ad5-JEV-E和JEV-E mRNA-LNP诱导的相当。与Ad5-JEV-E诱导的抗体相比,Ad5-JEV-E诱导的抗体增强ZIKV感染的能力减弱。此外,JEV-E mRNA-LNP免疫在小鼠中引发了与JEV-E mRNA-LNP相似的强效T细胞反应。用每种mRNA-LNP免疫的小鼠在JEV攻击后血清病毒载量水平低于 mock免疫小鼠。接受JEV-E mRNA-LNP免疫小鼠血清的小鼠在ZIKV攻击后表现出ADE,而被动转移的JEV-E mRNA-LNP免疫小鼠血清在受体小鼠中未导致明显的ZIKV感染ADE。最重要的是,母体获得的抗体并未增加JEV-E mRNA-LNP免疫小鼠产下的1日龄新生儿在ZIKV攻击后的死亡率。
讨论
这些结果表明,优化JEV的FL序列可显著降低JEV/ZIKV交叉反应性抗体的水平并消除ZIKV感染的ADE,为开发有效且安全的JEV疫苗提供了一种有前景的策略。
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