Antibodies directed toward neuraminidase N1 control disease in a mouse model of influenza
- Author
- Emma Job (UGent) , Michael Schotsaert (UGent) , Lorena Ibanez (UGent) , Anouk Smet (UGent) , Tine Ysenbaert (UGent) , Kenny Roose (UGent) , M. Dai, C. A. M. de Haan, H. Kleanthous, T. U. Vogel and Xavier Saelens (UGent)
- Organization
- Abstract
- There is increasing evidence to suggest that antibodies directed toward influenza A virus (IAV) neuraminidase (NA) are an important correlate of protection against influenza in humans. Moreover, the potential of NA-specific antibodies to provide broader protection than conventional hemagglutinin (HA) antibodies has been recognized. Here, we describe the isolation of two monoclonal antibodies, N1-7D3 and N1-C4, directed toward the N1 NA. N1-7D3 binds to a conserved linear epitope in the membrane- distal, carboxy-terminal part of the NA and reacted with the NA of seasonal H1N1 isolates ranging from 1977 to 2007 and the 2009 H1N1pdm virus, as well as A/Vietnam/ 1194/04 (H5N1). However, N1-7D3 lacked NA inhibition (NI) activity and the ability to protect BALB/c mice against a lethal challenge with a range of H1N1 viruses. Conversely, N1-C4 bound to a conformational epitope that is conserved between two influenza virus subtypes, 2009 H1N1pdm and H5N1 IAV, and displayed potent in vitro antiviral activity mediating both NI and plaque size reduction. Moreover, N1-C4 could provide heterosubtypic protection in BALB/c mice against a lethal challenge with 2009 H1N1pdm or H5N1 virus. Glutamic acid residue 311 in the NA was found to be critical for the NA binding and antiviral activity of monoclonal antibody N1-C4. Our data provide further evidence for cross-protective epitopes within the N1 subtype and highlight the potential of NA as an important target for vaccine and therapeutic approaches. IMPORTANCE Influenza remains a worldwide burden on public health. As such, the development of novel vaccines and therapeutics against influenza virus is crucial. Human challenge studies have recently highlighted the importance of antibodies directed toward the viral neuraminidase (NA) as an important correlate of reduced influenza-associated disease severity. Furthermore, there is evidence that anti-NA antibodies can provide broader protection than antibodies toward the viral hemagglutinin. Here, we describe the isolation and detailed characterization of two N1 NA-specific monoclonal antibodies. One of these monoclonal antibodies broadly binds N1-type NAs, and the second displays NA inhibition and in vitro and in vivo antiviral activity against 2009 H1N1pdm and H5N1 influenza viruses. These two new anti-NA antibodies contribute to our understanding of the antigenic properties and protective potential of the influenza virus NA antigen.
- Keywords
- MONOCLONAL-ANTIBODIES, VIRUS NEURAMINIDASE, VIRAL NEURAMINIDASE, CROSS-PROTECTION, PANDEMIC H1N1, VACCINE, HEMAGGLUTININ, INFECTION, IMMUNITY, GENERATION, influenza A virus, neuraminidase, monoclonal antibody, therapeutic
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Citation
Please use this url to cite or link to this publication: http://hdl.handle.net/1854/LU-8719293
- MLA
- Job, Emma, et al. “Antibodies Directed toward Neuraminidase N1 Control Disease in a Mouse Model of Influenza.” JOURNAL OF VIROLOGY, vol. 92, no. 4, 2018, doi:10.1128/JVI.01584-17.
- APA
- Job, E., Schotsaert, M., Ibanez, L., Smet, A., Ysenbaert, T., Roose, K., … Saelens, X. (2018). Antibodies directed toward neuraminidase N1 control disease in a mouse model of influenza. JOURNAL OF VIROLOGY, 92(4). https://doi.org/10.1128/JVI.01584-17
- Chicago author-date
- Job, Emma, Michael Schotsaert, Lorena Ibanez, Anouk Smet, Tine Ysenbaert, Kenny Roose, M. Dai, et al. 2018. “Antibodies Directed toward Neuraminidase N1 Control Disease in a Mouse Model of Influenza.” JOURNAL OF VIROLOGY 92 (4). https://doi.org/10.1128/JVI.01584-17.
- Chicago author-date (all authors)
- Job, Emma, Michael Schotsaert, Lorena Ibanez, Anouk Smet, Tine Ysenbaert, Kenny Roose, M. Dai, C. A. M. de Haan, H. Kleanthous, T. U. Vogel, and Xavier Saelens. 2018. “Antibodies Directed toward Neuraminidase N1 Control Disease in a Mouse Model of Influenza.” JOURNAL OF VIROLOGY 92 (4). doi:10.1128/JVI.01584-17.
- Vancouver
- 1.Job E, Schotsaert M, Ibanez L, Smet A, Ysenbaert T, Roose K, et al. Antibodies directed toward neuraminidase N1 control disease in a mouse model of influenza. JOURNAL OF VIROLOGY. 2018;92(4).
- IEEE
- [1]E. Job et al., “Antibodies directed toward neuraminidase N1 control disease in a mouse model of influenza,” JOURNAL OF VIROLOGY, vol. 92, no. 4, 2018.
@article{8719293, abstract = {{There is increasing evidence to suggest that antibodies directed toward influenza A virus (IAV) neuraminidase (NA) are an important correlate of protection against influenza in humans. Moreover, the potential of NA-specific antibodies to provide broader protection than conventional hemagglutinin (HA) antibodies has been recognized. Here, we describe the isolation of two monoclonal antibodies, N1-7D3 and N1-C4, directed toward the N1 NA. N1-7D3 binds to a conserved linear epitope in the membrane- distal, carboxy-terminal part of the NA and reacted with the NA of seasonal H1N1 isolates ranging from 1977 to 2007 and the 2009 H1N1pdm virus, as well as A/Vietnam/ 1194/04 (H5N1). However, N1-7D3 lacked NA inhibition (NI) activity and the ability to protect BALB/c mice against a lethal challenge with a range of H1N1 viruses. Conversely, N1-C4 bound to a conformational epitope that is conserved between two influenza virus subtypes, 2009 H1N1pdm and H5N1 IAV, and displayed potent in vitro antiviral activity mediating both NI and plaque size reduction. Moreover, N1-C4 could provide heterosubtypic protection in BALB/c mice against a lethal challenge with 2009 H1N1pdm or H5N1 virus. Glutamic acid residue 311 in the NA was found to be critical for the NA binding and antiviral activity of monoclonal antibody N1-C4. Our data provide further evidence for cross-protective epitopes within the N1 subtype and highlight the potential of NA as an important target for vaccine and therapeutic approaches. IMPORTANCE Influenza remains a worldwide burden on public health. As such, the development of novel vaccines and therapeutics against influenza virus is crucial. Human challenge studies have recently highlighted the importance of antibodies directed toward the viral neuraminidase (NA) as an important correlate of reduced influenza-associated disease severity. Furthermore, there is evidence that anti-NA antibodies can provide broader protection than antibodies toward the viral hemagglutinin. Here, we describe the isolation and detailed characterization of two N1 NA-specific monoclonal antibodies. One of these monoclonal antibodies broadly binds N1-type NAs, and the second displays NA inhibition and in vitro and in vivo antiviral activity against 2009 H1N1pdm and H5N1 influenza viruses. These two new anti-NA antibodies contribute to our understanding of the antigenic properties and protective potential of the influenza virus NA antigen.}}, articleno = {{e01584-17}}, author = {{Job, Emma and Schotsaert, Michael and Ibanez, Lorena and Smet, Anouk and Ysenbaert, Tine and Roose, Kenny and Dai, M. and de Haan, C. A. M. and Kleanthous, H. and Vogel, T. U. and Saelens, Xavier}}, issn = {{0022-538X}}, journal = {{JOURNAL OF VIROLOGY}}, keywords = {{MONOCLONAL-ANTIBODIES,VIRUS NEURAMINIDASE,VIRAL NEURAMINIDASE,CROSS-PROTECTION,PANDEMIC H1N1,VACCINE,HEMAGGLUTININ,INFECTION,IMMUNITY,GENERATION,influenza A virus,neuraminidase,monoclonal antibody,therapeutic}}, language = {{eng}}, number = {{4}}, pages = {{17}}, title = {{Antibodies directed toward neuraminidase N1 control disease in a mouse model of influenza}}, url = {{http://doi.org/10.1128/JVI.01584-17}}, volume = {{92}}, year = {{2018}}, }
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