Dynamic changes in host gene expression associated with H5N8 avian influenza virus infection in mice

Su Jin Park; Mukesh Kumar; Hyeok Il Kwon; Rak Kyun Seong; Kyudong Han; Jae Min Song; Chul Joong Kim; Young Ki Choi; Ok Sarah Shin

doi:10.1038/srep16512

Dynamic changes in host gene expression associated with H5N8 avian influenza virus infection in mice

Su Jin Park, Mukesh Kumar, Hyeok Il Kwon, Rak Kyun Seong, Kyudong Han, Jae Min Song, Chul Joong Kim, Young Ki Choi, Ok Sarah Shin

Research output: Contribution to journal › Article › peer-review

38 Citations (Scopus)

Abstract

Emerging outbreaks of newly found, highly pathogenic avian influenza (HPAI) A(H5N8) viruses have been reported globally. Previous studies have indicated that H5N8 pathogenicity in mice is relatively moderate compared with H5N1 pathogenicity. However, detailed mechanisms underlying avian influenza pathogenicity are still undetermined. We used a high-throughput RNA-seq method to analyse host and pathogen transcriptomes in the lungs of mice infected with A/MD/Korea/W452/2014 (H5N8) and A/EM/Korea/W149/2006 (H5N1) viruses. Sequenced numbers of viral transcripts and expression levels of host immune-related genes at 1 day post infection (dpi) were higher in H5N8-infected than H5N1-infected mice. Dual sequencing of viral transcripts revealed that in contrast to the observations at 1 dpi, higher number of H5N1 genes than H5N8 genes was sequenced at 3 and 7 dpi, which is consistent with higher viral titres and virulence observed in infected lungs in vivo. Ingenuity pathway analysis revealed a more significant upregulation of death receptor signalling, driven by H5N1 than with H5N8 infection at 3 and 7 dpi. Early induction of immune response-related genes may elicit protection in H5N8-infected mice, which correlates with moderate pathogenicity in vivo. Collectively, our data provide new insight into the underlying mechanisms of the differential pathogenicity of avian influenza viruses.

Original language	English
Article number	16512
Journal	Scientific reports
Volume	5
DOIs	https://doi.org/10.1038/srep16512
Publication status	Published - 2015 Nov 18

Bibliographical note

Funding Information:
This study was supported by a grant of the TEPIK (Transgovernmental Enterprise for Pandemic Influenza in Korea), which part of Korea Healthcare technology R&D Project by Ministry of Health & Welfare, Republic of Korea.(Grant No. : A103001).

Funding Information:
“This study was supported by a grant of the TEPIK (Transgovernmental Enterprise for Pandemic Influenza in Korea), which part of Korea Healthcare technology R&D Project by Ministry of Health & Welfare, Republic of Korea.(Grant No. A103001) and grant number P30GM114737, from the Centers of Biomedical Research Excellence program of the National Institute of General Medical Sciences, National Institutes of Health.”

Publisher Copyright:
© 2015, Nature Publishing Group. All rights reserved.

ASJC Scopus subject areas

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title = "Dynamic changes in host gene expression associated with H5N8 avian influenza virus infection in mice",

abstract = "Emerging outbreaks of newly found, highly pathogenic avian influenza (HPAI) A(H5N8) viruses have been reported globally. Previous studies have indicated that H5N8 pathogenicity in mice is relatively moderate compared with H5N1 pathogenicity. However, detailed mechanisms underlying avian influenza pathogenicity are still undetermined. We used a high-throughput RNA-seq method to analyse host and pathogen transcriptomes in the lungs of mice infected with A/MD/Korea/W452/2014 (H5N8) and A/EM/Korea/W149/2006 (H5N1) viruses. Sequenced numbers of viral transcripts and expression levels of host immune-related genes at 1 day post infection (dpi) were higher in H5N8-infected than H5N1-infected mice. Dual sequencing of viral transcripts revealed that in contrast to the observations at 1 dpi, higher number of H5N1 genes than H5N8 genes was sequenced at 3 and 7 dpi, which is consistent with higher viral titres and virulence observed in infected lungs in vivo. Ingenuity pathway analysis revealed a more significant upregulation of death receptor signalling, driven by H5N1 than with H5N8 infection at 3 and 7 dpi. Early induction of immune response-related genes may elicit protection in H5N8-infected mice, which correlates with moderate pathogenicity in vivo. Collectively, our data provide new insight into the underlying mechanisms of the differential pathogenicity of avian influenza viruses.",

author = "Park, {Su Jin} and Mukesh Kumar and Kwon, {Hyeok Il} and Seong, {Rak Kyun} and Kyudong Han and Song, {Jae Min} and Kim, {Chul Joong} and Choi, {Young Ki} and Shin, {Ok Sarah}",

note = "Funding Information: This study was supported by a grant of the TEPIK (Transgovernmental Enterprise for Pandemic Influenza in Korea), which part of Korea Healthcare technology R&D Project by Ministry of Health & Welfare, Republic of Korea.(Grant No. : A103001). Funding Information: “This study was supported by a grant of the TEPIK (Transgovernmental Enterprise for Pandemic Influenza in Korea), which part of Korea Healthcare technology R&D Project by Ministry of Health & Welfare, Republic of Korea.(Grant No. A103001) and grant number P30GM114737, from the Centers of Biomedical Research Excellence program of the National Institute of General Medical Sciences, National Institutes of Health.” Publisher Copyright: {\textcopyright} 2015, Nature Publishing Group. All rights reserved.",

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AU - Song, Jae Min

AU - Kim, Chul Joong

AU - Choi, Young Ki

AU - Shin, Ok Sarah

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Dynamic changes in host gene expression associated with H5N8 avian influenza virus infection in mice

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