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一种嵌合日本脑炎疫苗可预防致死性黄热病病毒感染而不诱导中和抗体。

A Chimeric Japanese Encephalitis Vaccine Protects against Lethal Yellow Fever Virus Infection without Inducing Neutralizing Antibodies.

机构信息

KU Leuven Department of Microbiology, Immunology and Transplantation, Rega Institute, Laboratory of Virology and Chemotherapy, Molecular Vaccinology and Vaccine Discovery Group, Leuven, Belgium.

KU Leuven Department of Microbiology, Immunology and Transplantation, Rega Institute, Laboratory of Virology and Chemotherapy, Molecular Vaccinology and Vaccine Discovery Group, Leuven, Belgium

出版信息

mBio. 2020 Apr 7;11(2):e02494-19. doi: 10.1128/mBio.02494-19.

Abstract

Recent outbreaks of yellow fever virus (YFV) in West Africa and Brazil resulted in rapid depletion of global vaccine emergency stockpiles and raised concerns about being unprepared against future YFV epidemics. Here we report that a live attenuated virus similar to the Japanese encephalitis virus (JEV) vaccine JE-CVax/Imojev that consists of YFV-17D vaccine from which the structural (prM/E) genes have been replaced with those of the JEV SA14-14-2 vaccine strain confers full protection in mice against lethal YFV challenge. In contrast to the YFV-17D-mediated protection against YFV, this protection is not mediated by neutralizing antibodies but correlates with YFV-specific nonneutralizing antibodies and T cell responses against cell-associated YFV NS1 and other YFV nonstructural (NS) proteins. Our findings reveal the potential of YFV NS proteins to mediate protection and demonstrate that chimeric flavivirus vaccines, such as Imojev, could confer protection against two flaviviruses. This dual protection may have implications for the possible off-label use of JE-CVax in case of emergency and vaccine shortage during YFV outbreaks. In addition, populations in Asia that have been vaccinated with Imojev may already be protected against YFV should outbreaks ever occur on that continent, as several countries/regions in the Asia-Pacific are vulnerable to international spread of the YFV. Efficient and safe vaccines against yellow fever (e.g., YFV-17D) that provide long-lasting protection by rapidly inducing neutralizing antibody responses exist. However, the vaccine supply cannot cope with an increasing demand posed by urban outbreaks in recent years. Here we report that JE-CVax/Imojev, a YFV-17D-based chimeric Japanese encephalitis vaccine, also efficiently protects against YFV infection in mice. In case of shortage of the YFV vaccine during yellow fever outbreaks, (off-label) use of JE-CVax/Imojev may be considered. Moreover, wider use of JE-CVax/Imojev in Asia may lower the risk of the much-feared YFV spillover to the continent. More generally, chimeric vaccines that combine surface antigens and replication machineries of two distinct flaviviruses may be considered dual vaccines for the latter pathogen without induction of surface-specific antibodies. Following this rationale, novel flavivirus vaccines that do not hold a risk for antibody-dependent enhancement (ADE) of infection (inherent to current dengue vaccines and dengue vaccine candidates) could be designed.

摘要

最近,西非和巴西的黄热病病毒(YFV)爆发导致全球疫苗应急储备迅速耗尽,并引发了对未来 YFV 流行准备不足的担忧。在这里,我们报告称,类似于日本脑炎病毒(JEV)疫苗 JE-CVax/Imojev 的减毒活病毒由 YFV-17D 疫苗组成,其结构(prM/E)基因已被 JEV SA14-14-2 疫苗株的基因取代,可在小鼠中完全抵抗致命的 YFV 挑战。与 YFV-17D 介导的 YFV 保护作用不同,这种保护作用不是由中和抗体介导的,而是与 YFV 特异性非中和抗体和针对细胞相关 YFV NS1 和其他 YFV 非结构(NS)蛋白的 T 细胞反应相关。我们的研究结果揭示了 YFV NS 蛋白介导保护的潜力,并证明了嵌合黄病毒疫苗,如 Imojev,可能对两种黄病毒提供保护。这种双重保护可能对 YFV 爆发期间紧急情况下和疫苗短缺时 JE-CVax 的可能非标签使用产生影响。此外,在亚洲接种过 Imojev 的人群如果该大陆发生疫情,可能已经受到 YFV 的保护,因为亚太地区的几个国家/地区易受 YFV 的国际传播影响。存在针对黄热病(例如 YFV-17D)的高效和安全疫苗,它们通过快速诱导中和抗体反应提供持久保护。然而,疫苗供应无法应对近年来城市爆发带来的日益增长的需求。在这里,我们报告称,基于 YFV-17D 的嵌合日本脑炎疫苗 JE-CVax/Imojev 也能有效地保护小鼠免受 YFV 感染。在黄热病爆发期间 YFV 疫苗短缺的情况下,(非标签)使用 JE-CVax/Imojev 可能被考虑。此外,在亚洲更广泛地使用 JE-CVax/Imojev 可能会降低人们对 YFV 溢出到该大陆的恐惧风险。更一般地说,将两种不同黄病毒的表面抗原和复制机制结合在一起的嵌合疫苗可被视为后者病原体的双价疫苗,而不会诱导表面特异性抗体。根据这一原理,可以设计不具有感染抗体依赖性增强(ADE)风险的新型黄病毒疫苗(固有于当前登革热疫苗和登革热候选疫苗)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fe13/7157777/d7f3bde8d67b/mBio.02494-19-f0001.jpg

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