Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.

Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.

BACKGROUND: Infectious bursal disease virus (IBDV) is a pathogen of worldwide significance to the poultry industry. IBDV has a bi-segmented double-stranded RNA genome. Segments A and B encode the capsid, ribonucleoprotein and non-structural proteins, or the virus polymerase (RdRp), respectively. Sin...

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Main Authors: Cyril Le Nouën, Didier Toquin, Hermann Müller, Rüdiger Raue, Katherine M Kean, Patrick Langlois, Martine Cherbonnel, Nicolas Eterradossi
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3258228?pdf=render
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spelling doaj-fe179aab92034c27a3604fe9a297b5f22020-11-25T01:13:35ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0171e2806410.1371/journal.pone.0028064Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.Cyril Le NouënDidier ToquinHermann MüllerRüdiger RaueKatherine M KeanPatrick LangloisMartine CherbonnelNicolas EterradossiBACKGROUND: Infectious bursal disease virus (IBDV) is a pathogen of worldwide significance to the poultry industry. IBDV has a bi-segmented double-stranded RNA genome. Segments A and B encode the capsid, ribonucleoprotein and non-structural proteins, or the virus polymerase (RdRp), respectively. Since the late eighties, very virulent (vv) IBDV strains have emerged in Europe inducing up to 60% mortality. Although some progress has been made in understanding the molecular biology of IBDV, the molecular basis for the pathogenicity of vvIBDV is still not fully understood. METHODOLOGY, PRINCIPAL FINDINGS: Strain 88180 belongs to a lineage of pathogenic IBDV phylogenetically related to vvIBDV. By reverse genetics, we rescued a molecular clone (mc88180), as pathogenic as its parent strain. To study the molecular basis for 88180 pathogenicity, we constructed and characterized in vivo reassortant or mosaic recombinant viruses derived from the 88180 and the attenuated Cu-1 IBDV strains. The reassortant virus rescued from segments A of 88180 (A88) and B of Cu-1 (BCU1) was milder than mc88180 showing that segment B is involved in 88180 pathogenicity. Next, the exchange of different regions of BCU1 with their counterparts in B88 in association with A88 did not fully restore a virulence equivalent to mc88180. This demonstrated that several regions if not the whole B88 are essential for the in vivo pathogenicity of 88180. CONCLUSION, SIGNIFICANCE: The present results show that different domains of the RdRp, are essential for the in vivo pathogenicity of IBDV, independently of the replication efficiency of the mosaic viruses.http://europepmc.org/articles/PMC3258228?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Cyril Le Nouën
Didier Toquin
Hermann Müller
Rüdiger Raue
Katherine M Kean
Patrick Langlois
Martine Cherbonnel
Nicolas Eterradossi
spellingShingle Cyril Le Nouën
Didier Toquin
Hermann Müller
Rüdiger Raue
Katherine M Kean
Patrick Langlois
Martine Cherbonnel
Nicolas Eterradossi
Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.
PLoS ONE
author_facet Cyril Le Nouën
Didier Toquin
Hermann Müller
Rüdiger Raue
Katherine M Kean
Patrick Langlois
Martine Cherbonnel
Nicolas Eterradossi
author_sort Cyril Le Nouën
title Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.
title_short Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.
title_full Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.
title_fullStr Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.
title_full_unstemmed Different domains of the RNA polymerase of infectious bursal disease virus contribute to virulence.
title_sort different domains of the rna polymerase of infectious bursal disease virus contribute to virulence.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description BACKGROUND: Infectious bursal disease virus (IBDV) is a pathogen of worldwide significance to the poultry industry. IBDV has a bi-segmented double-stranded RNA genome. Segments A and B encode the capsid, ribonucleoprotein and non-structural proteins, or the virus polymerase (RdRp), respectively. Since the late eighties, very virulent (vv) IBDV strains have emerged in Europe inducing up to 60% mortality. Although some progress has been made in understanding the molecular biology of IBDV, the molecular basis for the pathogenicity of vvIBDV is still not fully understood. METHODOLOGY, PRINCIPAL FINDINGS: Strain 88180 belongs to a lineage of pathogenic IBDV phylogenetically related to vvIBDV. By reverse genetics, we rescued a molecular clone (mc88180), as pathogenic as its parent strain. To study the molecular basis for 88180 pathogenicity, we constructed and characterized in vivo reassortant or mosaic recombinant viruses derived from the 88180 and the attenuated Cu-1 IBDV strains. The reassortant virus rescued from segments A of 88180 (A88) and B of Cu-1 (BCU1) was milder than mc88180 showing that segment B is involved in 88180 pathogenicity. Next, the exchange of different regions of BCU1 with their counterparts in B88 in association with A88 did not fully restore a virulence equivalent to mc88180. This demonstrated that several regions if not the whole B88 are essential for the in vivo pathogenicity of 88180. CONCLUSION, SIGNIFICANCE: The present results show that different domains of the RdRp, are essential for the in vivo pathogenicity of IBDV, independently of the replication efficiency of the mosaic viruses.
url http://europepmc.org/articles/PMC3258228?pdf=render
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