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Specificity, cross-reactivity, and function of antibodies elicited by Zika virus infection

Authors :
Stettler, K
Beltramello, M
Espinosa, DA
Graham, V
Cassotta, A
Bianchi, S
Vanzetta, F
Minola, A
Jaconi, S
Mele, F
Foglierini, M
Pedotti, M
Simonelli, L
Dowall, S
Atkinson, B
Percivalle, E
Simmons, CP
Varani, L
Blum, J
Baldanti, F
Cameroni, E
Hewson, R
Harris, E
Lanzavecchia, A
Sallusto, F
Corti, D
Stettler, K
Beltramello, M
Espinosa, DA
Graham, V
Cassotta, A
Bianchi, S
Vanzetta, F
Minola, A
Jaconi, S
Mele, F
Foglierini, M
Pedotti, M
Simonelli, L
Dowall, S
Atkinson, B
Percivalle, E
Simmons, CP
Varani, L
Blum, J
Baldanti, F
Cameroni, E
Hewson, R
Harris, E
Lanzavecchia, A
Sallusto, F
Corti, D
Publication Year :
2016

Abstract

Zika virus (ZIKV), a mosquito-borne flavivirus with homology to Dengue virus (DENV), has become a public health emergency. By characterizing memory lymphocytes from ZIKV-infected patients, we dissected ZIKV-specific and DENV-cross-reactive immune responses. Antibodies to nonstructural protein 1 (NS1) were largely ZIKV-specific and were used to develop a serological diagnostic tool. In contrast, antibodies against E protein domain I/II (EDI/II) were cross-reactive and, although poorly neutralizing, potently enhanced ZIKV and DENV infection in vitro and lethally enhanced DENV disease in mice. Memory T cells against NS1 or E proteins were poorly cross-reactive, even in donors preexposed to DENV. The most potent neutralizing antibodies were ZIKV-specific and targeted EDIII or quaternary epitopes on infectious virus. An EDIII-specific antibody protected mice from lethal ZIKV infection, illustrating the potential for antibody-based therapy.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1315663669
Document Type :
Electronic Resource

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