The PB2, PA, HA, NP, and NS genes of a highly pathogenic avian influenza virus A/whooper swan/Mongolia/3/2005 (H5N1) are responsible for pathogenicity in ducks

Kajihara Masahiro; Sakoda Yoshihiro; Soda Kosuke; Minari Kenji; Okamatsu Masatoshi; Takada Ayato; Kida Hiroshi

Title	en The PB2, PA, HA, NP, and NS genes of a highly pathogenic avian influenza virus A/whooper swan/Mongolia/3/2005 (H5N1) are responsible for pathogenicity in ducks
Creator	en Kajihara, Masahiro NRID 1000070711894 en Sakoda, Yoshihiro NRID 1000040333637 en Soda, Kosuke en Minari, Kenji en Okamatsu, Masatoshi NRID 1000000507163 en Takada, Ayato NRID 1000010292062 en Kida, Hiroshi NRID 1000010109506
Accessrights	open access
Rights	http://creativecommons.org/licenses/by-nc-sa/2.1/jp/ en Creative Commons Attribution-NonCommercial-ShareAlike 2.1 Japan
Subject	Other en H5N1 influenza virus Other en Duck Other en Natural host Other en Pathogenicity NDC 491
Description	Abstract en Background: Wild ducks are the natural hosts of influenza A viruses. Duck influenza, therefore, has been believed inapparent infection with influenza A viruses, including highly pathogenic avian influenza viruses (HPAIVs) in chickens. In fact, ducks experimentally infected with an HPAIV strain, A/Hong Kong/483/1997 (H5N1) (HK483), did not show any clinical signs. Another HPAIV strain, A/whooper swan/Mongolia/3/2005 (H5N1) (MON3) isolated from a dead swan, however, caused neurological dysfunction and death in ducks. Method: To understand the mechanism whereby MON3 shows high pathogenicity in ducks, HK483, MON3, and twenty-four reassortants generated between these two H5N1 viruses were compared for their pathogenicity in domestic ducks. Results: None of the ducks infected with MON3-based single-gene reassortants bearing the PB2, NP, or NS gene segment of HK483 died, and HK483-based single-gene reassortants bearing PB2, NP, or NS genes of MON3 were not pathogenic in ducks, suggesting that multiple gene segments contribute to the pathogenicity of MON3 in ducks. All the ducks infected with the reassortant bearing PB2, PA, HA, NP, and NS gene segments of MON3 died within five days post-inoculation, as did those infected with MON3. Each of the viruses was assessed for replication in ducks three days post-inoculation. MON3 and multi-gene reassortants pathogenic in ducks were recovered from all of the tissues examined and replicated with high titers in the brains and lungs. Conclusion: The present results indicate that multigenic factors are responsible for efficient replication of MON3 in ducks. In particular, virus growth in the brain might correlate with neurological dysfunction and the disease severity.
Publisher	en BioMed Central
Date	Issued2013-02-02
Language	eng
Resource Type	journal article
Version Type	VoR
Identifier	HDL http://hdl.handle.net/2115/53253
Relation	isIdenticalTo DOI https://doi.org/10.1186/1743-422X-10-45
Journal	PISSN 1743-422X en Virology Journal Volume Number10 Page Start45
File	fulltext 1743-422X-10-45.pdf 355.14 KB (application/pdf) Issued2013-02-02
Oaidate	2023-07-26