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Critical neutralizing fragment of Zika virus EDIII elicits cross-neutralization and protection against divergent Zika viruses

机译:寨卡病毒EDIII的关键中和片段引发交叉中和并抵抗不同的寨卡病毒

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摘要

Zika virus (ZIKV) infection remains a serious health threat due to its close association with congenital Zika syndrome (CZS), which includes microcephaly and other severe birth defects. As no vaccines are available for human use, continuous effort is needed to develop effective and safe vaccines to prevent ZIKV infection. In this study, we constructed three recombinant proteins comprising, respectively, residues 296–406 (E296-406), 298–409 (E298-409), and 301–404 (E301-404) of ZIKV envelope (E) protein domain III (EDIII) fused with a C-terminal Fc of human IgG. Our results demonstrated that E298-409 induced the highest titer of neutralizing antibodies against infection with nine ZIKV strains isolated from different hosts, countries, and time periods, and it maintained long-term anti-ZIKV immunogenicity to induce neutralizing antibodies. Pups born to mice immunized with E298-409 were fully protected against lethal challenge with two epidemic human ZIKV strains, 2015/Honduras (R103451) and 2015/Colombia (FLR). Passive transfer of anti-E298-409 mouse sera protected pups born to naive mice, as well as type I interferon receptor-deficient adult A129 mice, from lethal challenge with human ZIKV strains R103451 and FLR, and this protection was positively correlated with neutralizing antibodies. These data suggest that the critical neutralizing fragment (i.e., a fragment that can induce highly potent neutralizing antibodies against divergent ZIKV strains) of ZIKV EDIII is a good candidate for development as an effective and safe ZIKV subunit vaccine to protect pregnant mothers and their fetuses against ZIKV infection. The E298-409-specific antibodies can be used for passive immunization to prevent ZIKV infection in newborns or immunocompromised adults.
机译:由于寨卡病毒(ZIKV)与先天性寨卡综合征(CZS)(包括小头畸形和其他严重先天缺陷)密切相关,因此感染仍然是严重的健康威胁。由于没有可供人类使用的疫苗,因此需要持续的努力来开发有效和安全的疫苗以预防ZIKV感染。在这项研究中,我们构建了三种重组蛋白,分别包含ZIKV包膜(E)蛋白结构域III的残基296–406(E296-406),298–409(E298-409)和301–404(E301-404)。 (EDIII)与人IgG的C端Fc融合。我们的结果表明,E298-409诱导了针对来自不同宿主,国家和时间段的九株ZIKV菌株感染的最高效价的中和抗体,并保持了长期的抗ZIKV免疫原性以诱导中和抗体。用两种流行的人类ZIKV株2015 /洪都拉斯(R103451)和2015 /哥伦比亚(FLR),完全保护了用E298-409免疫的小鼠所生的幼仔免受致死性攻击。抗E298-409小鼠血清的被动转移保护了天真小鼠以及I型干扰素受体缺陷的成年A129小鼠出生的幼犬免受人类ZIKV株R103451和FLR的致命攻击,并且这种保护与中和抗体呈正相关。这些数据表明,ZIKV EDIII的关键中和片段(即可以诱导针对不同ZIKV株的高效中和抗体的片段)是发展成为一种有效且安全的ZIKV亚单位疫苗的良好候选者,可以保护孕妇及其胎儿免受ZIKV感染。 E298-409特异性抗体可用于被动免疫,以预防新生儿或免疫受损的成年人中的ZIKV感染。

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