A recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.

We have shown previously that replacement of the spike (S) gene of the apathogenic IBV strain Beau-R with that from the pathogenic strain of the same serotype, M41, resulted in an apathogenic virus, BeauR-M41(S), that conferred protection against challenge with M41. We have constructed a recombinant...

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Main Authors: Maria Armesto, Sharon Evans, David Cavanagh, Abu-Bakr Abu-Median, Sarah Keep, Paul Britton
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3166170?pdf=render
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spelling doaj-8c7f16473dc14ba8a69c228f3a79a50f2020-11-25T01:14:48ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-01-0168e2435210.1371/journal.pone.0024352A recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.Maria ArmestoSharon EvansDavid CavanaghAbu-Bakr Abu-MedianSarah KeepPaul BrittonWe have shown previously that replacement of the spike (S) gene of the apathogenic IBV strain Beau-R with that from the pathogenic strain of the same serotype, M41, resulted in an apathogenic virus, BeauR-M41(S), that conferred protection against challenge with M41. We have constructed a recombinant IBV, BeauR-4/91(S), with the genetic backbone of Beau-R but expressing the spike protein of the pathogenic IBV strain 4/91(UK), which belongs to a different serogroup as Beaudette or M41. Similar to our previous findings with BeauR-M41(S), clinical signs observations showed that the S gene of the pathogenic 4/91 virus did not confer pathogenicity to the rIBV BeauR-4/91(S). Furthermore, protection studies showed there was homologous protection; BeauR-4/91(S) conferred protection against challenge with wild type 4/91 virus as shown by the absence of clinical signs, IBV RNA assessed by qRT-PCR and the fact that no virus was isolated from tracheas removed from birds primarily infected with BeauR-4/91(S) and challenged with IBV 4/91(UK). A degree of heterologous protection against M41 challenge was observed, albeit at a lower level.Our results confirm and extend our previous findings and conclusions that swapping of the ectodomain of the S protein is a precise and effective way of generating genetically defined candidate IBV vaccines.http://europepmc.org/articles/PMC3166170?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Maria Armesto
Sharon Evans
David Cavanagh
Abu-Bakr Abu-Median
Sarah Keep
Paul Britton
spellingShingle Maria Armesto
Sharon Evans
David Cavanagh
Abu-Bakr Abu-Median
Sarah Keep
Paul Britton
A recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.
PLoS ONE
author_facet Maria Armesto
Sharon Evans
David Cavanagh
Abu-Bakr Abu-Median
Sarah Keep
Paul Britton
author_sort Maria Armesto
title A recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.
title_short A recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.
title_full A recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.
title_fullStr A recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.
title_full_unstemmed A recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.
title_sort recombinant avian infectious bronchitis virus expressing a heterologous spike gene belonging to the 4/91 serotype.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2011-01-01
description We have shown previously that replacement of the spike (S) gene of the apathogenic IBV strain Beau-R with that from the pathogenic strain of the same serotype, M41, resulted in an apathogenic virus, BeauR-M41(S), that conferred protection against challenge with M41. We have constructed a recombinant IBV, BeauR-4/91(S), with the genetic backbone of Beau-R but expressing the spike protein of the pathogenic IBV strain 4/91(UK), which belongs to a different serogroup as Beaudette or M41. Similar to our previous findings with BeauR-M41(S), clinical signs observations showed that the S gene of the pathogenic 4/91 virus did not confer pathogenicity to the rIBV BeauR-4/91(S). Furthermore, protection studies showed there was homologous protection; BeauR-4/91(S) conferred protection against challenge with wild type 4/91 virus as shown by the absence of clinical signs, IBV RNA assessed by qRT-PCR and the fact that no virus was isolated from tracheas removed from birds primarily infected with BeauR-4/91(S) and challenged with IBV 4/91(UK). A degree of heterologous protection against M41 challenge was observed, albeit at a lower level.Our results confirm and extend our previous findings and conclusions that swapping of the ectodomain of the S protein is a precise and effective way of generating genetically defined candidate IBV vaccines.
url http://europepmc.org/articles/PMC3166170?pdf=render
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