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Understanding Zika Virus stability and developing a chimeric vaccine through functional analysis

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2017
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Understanding Zika Virus stability and developing a chimeric vaccine through functional analysis.pdf (5.360xmlui.dri2xhtml.METS-1.0.size-megabytes)
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http://patua.iec.gov.br//handle/iec/2758
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Xie, Xuping
Yang, Yujiao
Muruato, Antonio E
Zou, Jing
Shan, Chao
Nunes, Bruno Tardelli Diniz
Medeiros, Daniele Barbosa de Almeida
Vasconcelos, Pedro Fernando da Costa
Weaver, Scott C
Rossi, Shannan L
Shia, Pei-Yong
xmlui.dri2xhtml.METS-1.0.item-abstract
Compared with other flaviviruses, Zika virus (ZIKV) is uniquely associated with congenital diseases in pregnant women. One recent study reported that (i) ZIKV has higher thermostability than dengue virus (DENV [a flavivirus closely related to ZIKV]), which might contribute to the disease outcome; (ii) the higher thermostability of ZIKV could arise from an extended loop structure in domain III of the viral envelope (E) protein and an extra hydrogen-bond interaction between E molecules (V. A. Kostyuchenko, E. X. Y. Lim, S. Zhang, G. Fibriansah, T.-S. Ng, J. S. G. Ooi, J. Shi, and S.-M. Lok, Nature 533:425- 428, 2016, https://doi.org/10.1038/nature17994). Here we report the functional analysis of the structural information in the context of complete ZIKV and DENV-2 virions. Swapping the prM-E genes between ZIKV and DENV-2 switched the thermostability of the chimeric viruses, identifying the prM-E proteins as the major determinants for virion thermostability. Shortening the extended loop of the E protein by 1 amino acid was lethal for ZIKV assembly/release. Mutations (Q350I and T351V) that abolished the extra hydrogen-bond interaction between the E proteins did not reduce ZIKV thermostability, indicating that the extra interaction does not increase the thermostability. Interestingly, mutant T351V was attenuated in A129 mice defective in type I interferon receptors, even though the virus retained the wild-type thermostability. Furthermore, we found that a chimeric ZIKV with the DENV-2 prM-E and a chimeric DENV-2 with the ZIKV prM-E were highly attenuated in A129 mice; these chimeric viruses were highly immunogenic and protective against DENV-2 and ZIKV challenge, respectively. These results indicate the potential of these chimeric viruses for vaccine development.
xmlui.dri2xhtml.METS-1.0.item-citation
XIE, Xuping et al. Understanding Zika Virus stability and developing a chimeric vaccine through functional analysis. MBio, v. 8, n. 1, p. 1-14, Jan.- Feb. 2017.
xmlui.dri2xhtml.METS-1.0.item-decsPrimary
Zika virus / genética
Zika virus / fisiologia
Zika virus / efeitos de radiação
Zika virus / imunologia
Vírus da Dengue / genética
Vírus da Dengue / fisiologia
Vírus da Dengue / imunologia
Vírus da Dengue / efeitos de radiação
Proteínas do Envelope Viral / genética
Replicação Viral / efeitos de radiação
Análise Mutacional de DNA
Substituição de Aminoácidos
Recombinação Genética
Vacinas Atenuadas
Virulência
Temperatura Ambiente
Reação em Cadeia da Polimerase Via Transcriptase Reversa / métodos
Microscopia de Fluorescência / métodos
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  • SAARB - Artigos Científicos

Instituto Evandro Chagas - SVS - MS - 2007-2018 Rodovia BR316 km 7 sn - Levilandia - 67030-000 - Ananindeua - Para - Brasil.
Licença Creative CommonsEste trabalho está licenciado com uma Licença Creative Commons - Atribuição-NãoComercial 4.0 Internacional
Tel: (55 91) 3214-2191
Email: biblioteca@iec.gov.br / clariceneta@iec.gov.br
 

 

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Instituto Evandro Chagas - SVS - MS - 2007-2018 Rodovia BR316 km 7 sn - Levilandia - 67030-000 - Ananindeua - Para - Brasil.
Licença Creative CommonsEste trabalho está licenciado com uma Licença Creative Commons - Atribuição-NãoComercial 4.0 Internacional
Tel: (55 91) 3214-2191
Email: biblioteca@iec.gov.br / clariceneta@iec.gov.br