Influenza A virus NS1 gene mutations F103L and M106I increase replication and virulence

BACKGROUND: To understand the evolutionary steps required for a virus to become virulent in a new host, a human influenza A virus (IAV), A/Hong Kong/1/68(H3N2) (HK-wt), was adapted to increased virulence in the mouse. Among eleven mutations selected in the NS1 gene, two mutations F103L and M106I had...

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Autores principales: Dankar, Samar K, Wang, Shuai, Ping, Jihui, Forbes, Nicole E, Keleta, Liya, Li, Yishan, Brown, Earl G
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3032709/
https://www.ncbi.nlm.nih.gov/pubmed/21226922
http://dx.doi.org/10.1186/1743-422X-8-13
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author Dankar, Samar K
Wang, Shuai
Ping, Jihui
Forbes, Nicole E
Keleta, Liya
Li, Yishan
Brown, Earl G
author_facet Dankar, Samar K
Wang, Shuai
Ping, Jihui
Forbes, Nicole E
Keleta, Liya
Li, Yishan
Brown, Earl G
author_sort Dankar, Samar K
collection PubMed
description BACKGROUND: To understand the evolutionary steps required for a virus to become virulent in a new host, a human influenza A virus (IAV), A/Hong Kong/1/68(H3N2) (HK-wt), was adapted to increased virulence in the mouse. Among eleven mutations selected in the NS1 gene, two mutations F103L and M106I had been previously detected in the highly virulent human H5N1 isolate, A/HK/156/97, suggesting a role for these mutations in virulence in mice and humans. RESULTS: To determine the selective advantage of these mutations, reverse genetics was used to rescue viruses containing each of the NS1 mouse adapted mutations into viruses possessing the HK-wt NS1 gene on the A/PR/8/34 genetic backbone. Both F103L and M106I NS1 mutations significantly enhanced growth in vitro (mouse and canine cells) and in vivo (BALB/c mouse lungs) as well as enhanced virulence in the mouse. Only the M106I NS1 mutation enhanced growth in human cells. Furthermore, these NS1 mutations enhanced early viral protein synthesis in MDCK cells and showed an increased ability to replicate in mouse interferon β (IFN-β) pre-treated mouse cells relative to rPR8-HK-NS-wt NS1. The double mutant, rPR8-HK-NS-F103L + M106I, demonstrated growth attenuation late in infection due to increased IFN-β induction in mouse cells. We then generated a rPR8 virus possessing the A/HK/156/97 NS gene that possesses 103L + 106I, and then rescued the L103F + I106M mutant. The 103L + 106I mutations increased virulence by >10 fold in BALB/c mice. We also inserted the avian A/Ck/Beijing/1/95 NS1 gene (the source lineage of the A/HK/156/97 NS1 gene) that possesses 103L + 106I, onto the A/WSN/33 backbone and then generated the L103F + I106M mutant. None of the H5N1 and H9N2 NS containing viruses resulted in increased IFN-β induction. The rWSN-A/Ck/Beijing/1/95-NS1 gene possessing 103L and 106I demonstrated 100 fold enhanced growth and >10 fold enhanced virulence that was associated with increased tropism for lung alveolar and bronchiolar tissues relative to the corresponding L103F and I106M mutant. CONCLUSIONS: The F103L and M106I NS1 mutations were adaptive genetic determinants of growth and virulence in both human and avian NS1 genes in the mouse model.
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spelling pubmed-30327092011-02-03 Influenza A virus NS1 gene mutations F103L and M106I increase replication and virulence Dankar, Samar K Wang, Shuai Ping, Jihui Forbes, Nicole E Keleta, Liya Li, Yishan Brown, Earl G Virol J Research BACKGROUND: To understand the evolutionary steps required for a virus to become virulent in a new host, a human influenza A virus (IAV), A/Hong Kong/1/68(H3N2) (HK-wt), was adapted to increased virulence in the mouse. Among eleven mutations selected in the NS1 gene, two mutations F103L and M106I had been previously detected in the highly virulent human H5N1 isolate, A/HK/156/97, suggesting a role for these mutations in virulence in mice and humans. RESULTS: To determine the selective advantage of these mutations, reverse genetics was used to rescue viruses containing each of the NS1 mouse adapted mutations into viruses possessing the HK-wt NS1 gene on the A/PR/8/34 genetic backbone. Both F103L and M106I NS1 mutations significantly enhanced growth in vitro (mouse and canine cells) and in vivo (BALB/c mouse lungs) as well as enhanced virulence in the mouse. Only the M106I NS1 mutation enhanced growth in human cells. Furthermore, these NS1 mutations enhanced early viral protein synthesis in MDCK cells and showed an increased ability to replicate in mouse interferon β (IFN-β) pre-treated mouse cells relative to rPR8-HK-NS-wt NS1. The double mutant, rPR8-HK-NS-F103L + M106I, demonstrated growth attenuation late in infection due to increased IFN-β induction in mouse cells. We then generated a rPR8 virus possessing the A/HK/156/97 NS gene that possesses 103L + 106I, and then rescued the L103F + I106M mutant. The 103L + 106I mutations increased virulence by >10 fold in BALB/c mice. We also inserted the avian A/Ck/Beijing/1/95 NS1 gene (the source lineage of the A/HK/156/97 NS1 gene) that possesses 103L + 106I, onto the A/WSN/33 backbone and then generated the L103F + I106M mutant. None of the H5N1 and H9N2 NS containing viruses resulted in increased IFN-β induction. The rWSN-A/Ck/Beijing/1/95-NS1 gene possessing 103L and 106I demonstrated 100 fold enhanced growth and >10 fold enhanced virulence that was associated with increased tropism for lung alveolar and bronchiolar tissues relative to the corresponding L103F and I106M mutant. CONCLUSIONS: The F103L and M106I NS1 mutations were adaptive genetic determinants of growth and virulence in both human and avian NS1 genes in the mouse model. BioMed Central 2011-01-12 /pmc/articles/PMC3032709/ /pubmed/21226922 http://dx.doi.org/10.1186/1743-422X-8-13 Text en Copyright ©2011 Dankar et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Dankar, Samar K
Wang, Shuai
Ping, Jihui
Forbes, Nicole E
Keleta, Liya
Li, Yishan
Brown, Earl G
Influenza A virus NS1 gene mutations F103L and M106I increase replication and virulence
title Influenza A virus NS1 gene mutations F103L and M106I increase replication and virulence
title_full Influenza A virus NS1 gene mutations F103L and M106I increase replication and virulence
title_fullStr Influenza A virus NS1 gene mutations F103L and M106I increase replication and virulence
title_full_unstemmed Influenza A virus NS1 gene mutations F103L and M106I increase replication and virulence
title_short Influenza A virus NS1 gene mutations F103L and M106I increase replication and virulence
title_sort influenza a virus ns1 gene mutations f103l and m106i increase replication and virulence
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3032709/
https://www.ncbi.nlm.nih.gov/pubmed/21226922
http://dx.doi.org/10.1186/1743-422X-8-13
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