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Heterologous Two-Dose Vaccination with Simian Adenovirus and Poxvirus Vectors Elicits Long-Lasting Cellular Immunity to Influenza Virus A in Healthy Adults

BACKGROUND: T-cell responses against highly conserved influenza antigens have been previously associated with protection. However, these immune responses are poorly maintained following recovery from influenza infection and are not boosted by inactivated influenza vaccines. We have previously demons...

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Autores principales: Coughlan, L., Sridhar, S., Payne, R., Edmans, M., Milicic, A., Venkatraman, N., Lugonja, B., Clifton, L., Qi, C., Folegatti, P.M., Lawrie, A.M., Roberts, R., de Graaf, H., Sukhtankar, P., Faust, S.N., Lewis, D.J.M., Lambe, T., Hill, AVS, Gilbert, S.C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5926543/
https://www.ncbi.nlm.nih.gov/pubmed/29519670
http://dx.doi.org/10.1016/j.ebiom.2018.02.011
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author Coughlan, L.
Sridhar, S.
Payne, R.
Edmans, M.
Milicic, A.
Venkatraman, N.
Lugonja, B.
Clifton, L.
Qi, C.
Folegatti, P.M.
Lawrie, A.M.
Roberts, R.
de Graaf, H.
Sukhtankar, P.
Faust, S.N.
Lewis, D.J.M.
Lambe, T.
Hill, AVS
Gilbert, S.C.
author_facet Coughlan, L.
Sridhar, S.
Payne, R.
Edmans, M.
Milicic, A.
Venkatraman, N.
Lugonja, B.
Clifton, L.
Qi, C.
Folegatti, P.M.
Lawrie, A.M.
Roberts, R.
de Graaf, H.
Sukhtankar, P.
Faust, S.N.
Lewis, D.J.M.
Lambe, T.
Hill, AVS
Gilbert, S.C.
author_sort Coughlan, L.
collection PubMed
description BACKGROUND: T-cell responses against highly conserved influenza antigens have been previously associated with protection. However, these immune responses are poorly maintained following recovery from influenza infection and are not boosted by inactivated influenza vaccines. We have previously demonstrated the safety and immunogenicity of two viral vectored vaccines, modified vaccinia virus Ankara (MVA) and the chimpanzee adenovirus ChAdOx1 expressing conserved influenza virus antigens, nucleoprotein (NP) and matrix protein-1 (M1). We now report on the safety and long-term immunogenicity of multiple combination regimes of these vaccines in young and older adults. METHODS: We conducted a Phase I open-label, randomized, multi-center study in 49 subjects aged 18–46 years and 24 subjects aged 50 years or over. Following vaccination, adverse events were recorded and the kinetics of the T cell response determined at multiple time points for up to 18 months. FINDINGS: Both vaccines were well tolerated. A two dose heterologous vaccination regimen significantly increased the magnitude of pre-existing T-cell responses to NP and M1 after both doses in young and older adults. The fold-increase and peak immune responses after a single MVA-NP + M1 vaccination was significantly higher compared to ChAdOx1 NP + M1. In a mixed regression model, T-cell responses over 18 months were significantly higher following the two dose vaccination regimen of MVA/ChAdOx1 NP + M1. INTERPRETATION: A two dose heterologous vaccination regimen of MVA/ChAdOx1 NP + M1 was safe and immunogenic in young and older adults, offering a promising vaccination strategy for inducing long-term broadly cross-reactive protection against influenza A. FUNDING SOURCE: Medical Research Council UK, NIHR BMRC Oxford.
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spelling pubmed-59265432018-05-01 Heterologous Two-Dose Vaccination with Simian Adenovirus and Poxvirus Vectors Elicits Long-Lasting Cellular Immunity to Influenza Virus A in Healthy Adults Coughlan, L. Sridhar, S. Payne, R. Edmans, M. Milicic, A. Venkatraman, N. Lugonja, B. Clifton, L. Qi, C. Folegatti, P.M. Lawrie, A.M. Roberts, R. de Graaf, H. Sukhtankar, P. Faust, S.N. Lewis, D.J.M. Lambe, T. Hill, AVS Gilbert, S.C. EBioMedicine Research Paper BACKGROUND: T-cell responses against highly conserved influenza antigens have been previously associated with protection. However, these immune responses are poorly maintained following recovery from influenza infection and are not boosted by inactivated influenza vaccines. We have previously demonstrated the safety and immunogenicity of two viral vectored vaccines, modified vaccinia virus Ankara (MVA) and the chimpanzee adenovirus ChAdOx1 expressing conserved influenza virus antigens, nucleoprotein (NP) and matrix protein-1 (M1). We now report on the safety and long-term immunogenicity of multiple combination regimes of these vaccines in young and older adults. METHODS: We conducted a Phase I open-label, randomized, multi-center study in 49 subjects aged 18–46 years and 24 subjects aged 50 years or over. Following vaccination, adverse events were recorded and the kinetics of the T cell response determined at multiple time points for up to 18 months. FINDINGS: Both vaccines were well tolerated. A two dose heterologous vaccination regimen significantly increased the magnitude of pre-existing T-cell responses to NP and M1 after both doses in young and older adults. The fold-increase and peak immune responses after a single MVA-NP + M1 vaccination was significantly higher compared to ChAdOx1 NP + M1. In a mixed regression model, T-cell responses over 18 months were significantly higher following the two dose vaccination regimen of MVA/ChAdOx1 NP + M1. INTERPRETATION: A two dose heterologous vaccination regimen of MVA/ChAdOx1 NP + M1 was safe and immunogenic in young and older adults, offering a promising vaccination strategy for inducing long-term broadly cross-reactive protection against influenza A. FUNDING SOURCE: Medical Research Council UK, NIHR BMRC Oxford. Elsevier 2018-02-15 /pmc/articles/PMC5926543/ /pubmed/29519670 http://dx.doi.org/10.1016/j.ebiom.2018.02.011 Text en © 2018 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Paper
Coughlan, L.
Sridhar, S.
Payne, R.
Edmans, M.
Milicic, A.
Venkatraman, N.
Lugonja, B.
Clifton, L.
Qi, C.
Folegatti, P.M.
Lawrie, A.M.
Roberts, R.
de Graaf, H.
Sukhtankar, P.
Faust, S.N.
Lewis, D.J.M.
Lambe, T.
Hill, AVS
Gilbert, S.C.
Heterologous Two-Dose Vaccination with Simian Adenovirus and Poxvirus Vectors Elicits Long-Lasting Cellular Immunity to Influenza Virus A in Healthy Adults
title Heterologous Two-Dose Vaccination with Simian Adenovirus and Poxvirus Vectors Elicits Long-Lasting Cellular Immunity to Influenza Virus A in Healthy Adults
title_full Heterologous Two-Dose Vaccination with Simian Adenovirus and Poxvirus Vectors Elicits Long-Lasting Cellular Immunity to Influenza Virus A in Healthy Adults
title_fullStr Heterologous Two-Dose Vaccination with Simian Adenovirus and Poxvirus Vectors Elicits Long-Lasting Cellular Immunity to Influenza Virus A in Healthy Adults
title_full_unstemmed Heterologous Two-Dose Vaccination with Simian Adenovirus and Poxvirus Vectors Elicits Long-Lasting Cellular Immunity to Influenza Virus A in Healthy Adults
title_short Heterologous Two-Dose Vaccination with Simian Adenovirus and Poxvirus Vectors Elicits Long-Lasting Cellular Immunity to Influenza Virus A in Healthy Adults
title_sort heterologous two-dose vaccination with simian adenovirus and poxvirus vectors elicits long-lasting cellular immunity to influenza virus a in healthy adults
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5926543/
https://www.ncbi.nlm.nih.gov/pubmed/29519670
http://dx.doi.org/10.1016/j.ebiom.2018.02.011
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