Rational Design of Zika Virus Subunit Vaccine with Enhanced Efficacy | Zendy

Wanbo Tai | Zendy; Jiawei Chen | Zendy; Guangyu Zhao | Zendy; Qibin Geng | Zendy; Lei He | Zendy; Yuehong Chen | Zendy; Yusen Zhou | Zendy; Fang Li | Zendy; Lanying Du | Zendy

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Rational Design of Zika Virus Subunit Vaccine with Enhanced Efficacy

Author(s) -

Wanbo Tai,

Jiawei Chen,

Guangyu Zhao,

Qibin Geng,

Lei He,

Yuehong Chen,

Yusen Zhou,

Fang Li,

Lanying Du

Publication year - 2019

Publication title -

journal of virology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 2.617

H-Index - 292

eISSN - 1070-6321

pISSN - 0022-538X

DOI - 10.1128/jvi.02187-18

Subject(s) - epitope , virology , biology , zika virus , protein subunit , virus , antigen , immunology , genetics , gene

Viral subunit vaccines generally show low efficacy. In this study, we revealed an intrinsic limitation of subunit vaccine designs: artificially exposed surfaces of subunit vaccines contain epitopes unfavorable for vaccine efficacy. More specifically, we identified an epitope on Zika virus (ZIKV) envelope protein domain III (EDIII) that is buried in the full-length envelope protein but becomes exposed in recombinant EDIII. We further shielded this epitope with a glycan, and the resulting mutant EDIII vaccine demonstrated significantly enhanced efficacy over the wild-type EDIII vaccine in protecting animal models from ZIKV infections. Therefore, the intrinsic limitation of subunit vaccines can be overcome through shielding these artificially exposed unfavorable epitopes. The engineered EDIII vaccine generated in this study is a promising vaccine candidate that can be further developed to battle ZIKV infections.

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