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Vaccination with Consensus H7 Elicits Broadly Reactive and Protective Antibodies against Eurasian and North American Lineage H7 Viruses

H7 subtype avian influenza viruses have caused outbreaks in poultry, and even human infection, for decades in both Eurasia and North America. Although effective vaccines offer the best protection against avian influenza viruses, antigenically distinct Eurasian and North American lineage subtype H7 v...

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Autores principales: Fadlallah, Gendeal M., Ma, Fuying, Zhang, Zherui, Hao, Mengchan, Hu, Juefu, Li, Mingxin, Liu, Haizhou, Liang, Biling, Yao, Yanfeng, Gong, Rui, Zhang, Bo, Liu, Di, Chen, Jianjun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7157604/
https://www.ncbi.nlm.nih.gov/pubmed/32210092
http://dx.doi.org/10.3390/vaccines8010143
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author Fadlallah, Gendeal M.
Ma, Fuying
Zhang, Zherui
Hao, Mengchan
Hu, Juefu
Li, Mingxin
Liu, Haizhou
Liang, Biling
Yao, Yanfeng
Gong, Rui
Zhang, Bo
Liu, Di
Chen, Jianjun
author_facet Fadlallah, Gendeal M.
Ma, Fuying
Zhang, Zherui
Hao, Mengchan
Hu, Juefu
Li, Mingxin
Liu, Haizhou
Liang, Biling
Yao, Yanfeng
Gong, Rui
Zhang, Bo
Liu, Di
Chen, Jianjun
author_sort Fadlallah, Gendeal M.
collection PubMed
description H7 subtype avian influenza viruses have caused outbreaks in poultry, and even human infection, for decades in both Eurasia and North America. Although effective vaccines offer the best protection against avian influenza viruses, antigenically distinct Eurasian and North American lineage subtype H7 viruses require the development of cross-protective vaccine candidates. In this study, a methodology called computationally optimized broadly reactive antigen (COBRA) was used to develop four consensus H7 antigens (CH7-22, CH7-24, CH7-26, and CH7-28). In vitro experiments confirmed the binding of monoclonal antibodies to the head and stem domains of cell surface-expressed consensus HAs, indicating display of their antigenicity. Immunization with DNA vaccines encoding the four antigens was evaluated in a mouse model. Broadly reactive antibodies against H7 viruses from Eurasian and North American lineages were elicited and detected by binding, inhibition, and neutralizing analyses. Further infection with Eurasian H7N9 and North American H7N3 virus strains confirmed that CH7-22 and CH7-24 conferred the most effective protection against hetero-lethal challenge. Our data showed that the consensus H7 vaccines elicit a broadly reactive, protective response against Eurasian and North American lineage H7 viruses, which are suitable for development against other zoonotic influenza viruses.
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spelling pubmed-71576042020-05-01 Vaccination with Consensus H7 Elicits Broadly Reactive and Protective Antibodies against Eurasian and North American Lineage H7 Viruses Fadlallah, Gendeal M. Ma, Fuying Zhang, Zherui Hao, Mengchan Hu, Juefu Li, Mingxin Liu, Haizhou Liang, Biling Yao, Yanfeng Gong, Rui Zhang, Bo Liu, Di Chen, Jianjun Vaccines (Basel) Article H7 subtype avian influenza viruses have caused outbreaks in poultry, and even human infection, for decades in both Eurasia and North America. Although effective vaccines offer the best protection against avian influenza viruses, antigenically distinct Eurasian and North American lineage subtype H7 viruses require the development of cross-protective vaccine candidates. In this study, a methodology called computationally optimized broadly reactive antigen (COBRA) was used to develop four consensus H7 antigens (CH7-22, CH7-24, CH7-26, and CH7-28). In vitro experiments confirmed the binding of monoclonal antibodies to the head and stem domains of cell surface-expressed consensus HAs, indicating display of their antigenicity. Immunization with DNA vaccines encoding the four antigens was evaluated in a mouse model. Broadly reactive antibodies against H7 viruses from Eurasian and North American lineages were elicited and detected by binding, inhibition, and neutralizing analyses. Further infection with Eurasian H7N9 and North American H7N3 virus strains confirmed that CH7-22 and CH7-24 conferred the most effective protection against hetero-lethal challenge. Our data showed that the consensus H7 vaccines elicit a broadly reactive, protective response against Eurasian and North American lineage H7 viruses, which are suitable for development against other zoonotic influenza viruses. MDPI 2020-03-23 /pmc/articles/PMC7157604/ /pubmed/32210092 http://dx.doi.org/10.3390/vaccines8010143 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Fadlallah, Gendeal M.
Ma, Fuying
Zhang, Zherui
Hao, Mengchan
Hu, Juefu
Li, Mingxin
Liu, Haizhou
Liang, Biling
Yao, Yanfeng
Gong, Rui
Zhang, Bo
Liu, Di
Chen, Jianjun
Vaccination with Consensus H7 Elicits Broadly Reactive and Protective Antibodies against Eurasian and North American Lineage H7 Viruses
title Vaccination with Consensus H7 Elicits Broadly Reactive and Protective Antibodies against Eurasian and North American Lineage H7 Viruses
title_full Vaccination with Consensus H7 Elicits Broadly Reactive and Protective Antibodies against Eurasian and North American Lineage H7 Viruses
title_fullStr Vaccination with Consensus H7 Elicits Broadly Reactive and Protective Antibodies against Eurasian and North American Lineage H7 Viruses
title_full_unstemmed Vaccination with Consensus H7 Elicits Broadly Reactive and Protective Antibodies against Eurasian and North American Lineage H7 Viruses
title_short Vaccination with Consensus H7 Elicits Broadly Reactive and Protective Antibodies against Eurasian and North American Lineage H7 Viruses
title_sort vaccination with consensus h7 elicits broadly reactive and protective antibodies against eurasian and north american lineage h7 viruses
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7157604/
https://www.ncbi.nlm.nih.gov/pubmed/32210092
http://dx.doi.org/10.3390/vaccines8010143
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