ZIKV-envelope proteins induce specific humoral and cellular immunity in distinct mice strains.
Victória Alves Santos LunardelliJuliana de Souza ApostolicoHigo Fernando Santos SouzaFernanda Caroline CoiradaJéssica Amaral MartinhoRenato Mancini AstraySilvia Beatriz BoscardinDaniela Santoro RosaPublished in: Scientific reports (2022)
Recent outbreaks of Zika virus (ZIKV) infection have highlighted the need for a better understanding of ZIKV-specific immune responses. The ZIKV envelope glycoprotein (E<sub>ZIKV</sub>) is the most abundant protein on the virus surface and it is the main target of the protective immune response. E<sub>ZIKV</sub> protein contains the central domain (EDI), a dimerization domain containing the fusion peptide (EDII), and a domain that binds to the cell surface receptor (EDIII). In this study, we performed a systematic comparison of the specific immune response induced by different E<sub>ZIKV</sub> recombinant proteins (E<sub>ZIKV</sub>, EDI/II<sub>ZIKV</sub> or EDIII<sub>ZIKV</sub>) in two mice strains. Immunization induced high titers of E-specific antibodies which recognized ZIKV-infected cells and neutralized the virus. Furthermore, immunization with E<sub>ZIKV</sub>, EDI/II<sub>ZIKV</sub> and EDIII<sub>ZIKV</sub> proteins induced specific IFNγ-producing cells and polyfunctional CD4<sup>+</sup> and CD8<sup>+</sup> T cells. Finally, we identified 4 peptides present in the envelope protein (E<sub>1-20</sub>, E<sub>51-70</sub>, E<sub>351-370</sub> and E<sub>361-380</sub>), capable of inducing a cellular immune response to the H-2K<sup>d</sup> and H-2K<sup>b</sup> haplotypes. In summary, our work provides a detailed assessment of the immune responses induced after immunization with different regions of the ZIKV envelope protein.