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Large-scale analysis of B-cell epitopes of envelope: Implications for Zika vaccine and immunotherapeutic development

Background: Cases of the re-emergence of Zika virus in 2015 were associated with severe neurologic complications, including Gillien-Barre syndrome in adults and congenital Zika syndrome in newborns. The major structural determinant of immunity to the Zika virus is the E protein. Although B-cell epit...

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Autores principales: Almansour, Iman, Alfares, Rahaf, Aljofi, Halah
Formato: Online Artículo Texto
Lenguaje:English
Publicado: F1000 Research Limited 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6611143/
https://www.ncbi.nlm.nih.gov/pubmed/31316749
http://dx.doi.org/10.12688/f1000research.16454.2
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author Almansour, Iman
Alfares, Rahaf
Aljofi, Halah
author_facet Almansour, Iman
Alfares, Rahaf
Aljofi, Halah
author_sort Almansour, Iman
collection PubMed
description Background: Cases of the re-emergence of Zika virus in 2015 were associated with severe neurologic complications, including Gillien-Barre syndrome in adults and congenital Zika syndrome in newborns. The major structural determinant of immunity to the Zika virus is the E protein. Although B-cell epitopes of Zika E protein were recently identified, data regarding epitope variations among Zika strains in pre-epidemic and epidemic periods are lacking. Methods: Here, we conducted systematic bioinformatics analyses of Zika strains isolated between 1968 and 2017. Multiple sequence alignment of E protein as well as B-cell epitopes annotations were performed. In addition, homology-based approach was utilized to construct three-dimensional structures of monomeric E glycoproteins to annotate epitope variations. Lastly, prediction of of N-glycosylation patterns and prediction of protein stability upon mutations were also investigated. Results: Our analyses indicates that epitopes recognized by human mAbs ZIKV-117, ZIKV-15, and ZIKV-19 were highly conserved, suggesting as attractive targets for the development of vaccines and immunotherapeutics directed against diverse Zika strains. In addition, the epitope recognized by ZIKV-E-2A10G6 mAb derived from immunized mice was mostly conserved across Zika strains. Conclusions: Our data provide new insights regarding antigenic similarities between Zika strains circulating worldwide. These data are essential for understanding the impact of evolution on antigenic cross-reactivity between Zika lineages and strains. Further in-vitro analyses are needed to determine how mutationsat predefined epitopes could impact the development of vaccines that can effectively neutralize Zika viruses.
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spelling pubmed-66111432019-07-16 Large-scale analysis of B-cell epitopes of envelope: Implications for Zika vaccine and immunotherapeutic development Almansour, Iman Alfares, Rahaf Aljofi, Halah F1000Res Research Article Background: Cases of the re-emergence of Zika virus in 2015 were associated with severe neurologic complications, including Gillien-Barre syndrome in adults and congenital Zika syndrome in newborns. The major structural determinant of immunity to the Zika virus is the E protein. Although B-cell epitopes of Zika E protein were recently identified, data regarding epitope variations among Zika strains in pre-epidemic and epidemic periods are lacking. Methods: Here, we conducted systematic bioinformatics analyses of Zika strains isolated between 1968 and 2017. Multiple sequence alignment of E protein as well as B-cell epitopes annotations were performed. In addition, homology-based approach was utilized to construct three-dimensional structures of monomeric E glycoproteins to annotate epitope variations. Lastly, prediction of of N-glycosylation patterns and prediction of protein stability upon mutations were also investigated. Results: Our analyses indicates that epitopes recognized by human mAbs ZIKV-117, ZIKV-15, and ZIKV-19 were highly conserved, suggesting as attractive targets for the development of vaccines and immunotherapeutics directed against diverse Zika strains. In addition, the epitope recognized by ZIKV-E-2A10G6 mAb derived from immunized mice was mostly conserved across Zika strains. Conclusions: Our data provide new insights regarding antigenic similarities between Zika strains circulating worldwide. These data are essential for understanding the impact of evolution on antigenic cross-reactivity between Zika lineages and strains. Further in-vitro analyses are needed to determine how mutationsat predefined epitopes could impact the development of vaccines that can effectively neutralize Zika viruses. F1000 Research Limited 2019-06-27 /pmc/articles/PMC6611143/ /pubmed/31316749 http://dx.doi.org/10.12688/f1000research.16454.2 Text en Copyright: © 2019 Almansour I et al. http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution Licence, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Almansour, Iman
Alfares, Rahaf
Aljofi, Halah
Large-scale analysis of B-cell epitopes of envelope: Implications for Zika vaccine and immunotherapeutic development
title Large-scale analysis of B-cell epitopes of envelope: Implications for Zika vaccine and immunotherapeutic development
title_full Large-scale analysis of B-cell epitopes of envelope: Implications for Zika vaccine and immunotherapeutic development
title_fullStr Large-scale analysis of B-cell epitopes of envelope: Implications for Zika vaccine and immunotherapeutic development
title_full_unstemmed Large-scale analysis of B-cell epitopes of envelope: Implications for Zika vaccine and immunotherapeutic development
title_short Large-scale analysis of B-cell epitopes of envelope: Implications for Zika vaccine and immunotherapeutic development
title_sort large-scale analysis of b-cell epitopes of envelope: implications for zika vaccine and immunotherapeutic development
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6611143/
https://www.ncbi.nlm.nih.gov/pubmed/31316749
http://dx.doi.org/10.12688/f1000research.16454.2
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