Correlates of protection against influenza infection in humans—on the path to a universal vaccine?

•Influenza infection is prevented by protective antibodies.•Flu-specific T cells can reduce viral load and disease severity.•Stem region of HA and flu internal proteins (NP and M1) are highly conserved among influenza virus.•Boosting antibody and T cell responses against conserved regions of flu pro...

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Published inCurrent opinion in immunology Vol. 25; no. 4; pp. 470 - 476
Main Authors Li, Chris Ka-fai, Rappuoli, Rino, Xu, Xiao-Ning
Format Journal Article
LanguageEnglish
Published England Elsevier Ltd 01.08.2013
Subjects
Online AccessGet full text
ISSN0952-7915
1879-0372
1879-0372
DOI10.1016/j.coi.2013.07.005

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Abstract •Influenza infection is prevented by protective antibodies.•Flu-specific T cells can reduce viral load and disease severity.•Stem region of HA and flu internal proteins (NP and M1) are highly conserved among influenza virus.•Boosting antibody and T cell responses against conserved regions of flu proteins may be critical. Influenza is an acute respiratory viral infection with high mutation rate and pandemic potential. Vaccination is an effective means of prevention and control of influenza, but the challenges of vaccine mismatches for the next influenza seasons and adequate global supply of influenza vaccines limit its effectiveness. Protective immunity in vaccination or natural infection is primarily mediated by antibody responses against surface proteins of influenza including haemagglutinin (HA) as the major neutralizing target, whereas strong T cell responses to internal viral proteins are associated with reduced disease severity. Recently, identification of broadly neutralizing antibodies against the conserved stem region of HA from influenza infected individuals has invigorated interest in development of a universal vaccine against different subtypes of influenza. Moreover, because of the cross-reactive nature of T cell recognition and more conserved internal antigens of influenza, strategies that boost memory T cell responses to these internal antigens may provide not only help for antibody-mediated protection but also limit the cell damage caused by viral infection directly. This is particularly important in acute infection with new pandemic viruses or antibody-escape variants where there are no pre-existing neutralizing antibodies. Here, we review the protective immune correlates against human influenza infection and discuss current status of universal influenza vaccine development.
AbstractList •Influenza infection is prevented by protective antibodies.•Flu-specific T cells can reduce viral load and disease severity.•Stem region of HA and flu internal proteins (NP and M1) are highly conserved among influenza virus.•Boosting antibody and T cell responses against conserved regions of flu proteins may be critical. Influenza is an acute respiratory viral infection with high mutation rate and pandemic potential. Vaccination is an effective means of prevention and control of influenza, but the challenges of vaccine mismatches for the next influenza seasons and adequate global supply of influenza vaccines limit its effectiveness. Protective immunity in vaccination or natural infection is primarily mediated by antibody responses against surface proteins of influenza including haemagglutinin (HA) as the major neutralizing target, whereas strong T cell responses to internal viral proteins are associated with reduced disease severity. Recently, identification of broadly neutralizing antibodies against the conserved stem region of HA from influenza infected individuals has invigorated interest in development of a universal vaccine against different subtypes of influenza. Moreover, because of the cross-reactive nature of T cell recognition and more conserved internal antigens of influenza, strategies that boost memory T cell responses to these internal antigens may provide not only help for antibody-mediated protection but also limit the cell damage caused by viral infection directly. This is particularly important in acute infection with new pandemic viruses or antibody-escape variants where there are no pre-existing neutralizing antibodies. Here, we review the protective immune correlates against human influenza infection and discuss current status of universal influenza vaccine development.
Influenza is an acute respiratory viral infection with high mutation rate and pandemic potential. Vaccination is an effective means of prevention and control of influenza, but the challenges of vaccine mismatches for the next influenza seasons and adequate global supply of influenza vaccines limit its effectiveness. Protective immunity in vaccination or natural infection is primarily mediated by antibody responses against surface proteins of influenza including haemagglutinin (HA) as the major neutralizing target, whereas strong T cell responses to internal viral proteins are associated with reduced disease severity. Recently, identification of broadly neutralizing antibodies against the conserved stem region of HA from influenza infected individuals has invigorated interest in development of a universal vaccine against different subtypes of influenza. Moreover, because of the cross-reactive nature of T cell recognition and more conserved internal antigens of influenza, strategies that boost memory T cell responses to these internal antigens may provide not only help for antibody-mediated protection but also limit the cell damage caused by viral infection directly. This is particularly important in acute infection with new pandemic viruses or antibody-escape variants where there are no pre-existing neutralizing antibodies. Here, we review the protective immune correlates against human influenza infection and discuss current status of universal influenza vaccine development.
Influenza is an acute respiratory viral infection with high mutation rate and pandemic potential. Vaccination is an effective means of prevention and control of influenza, but the challenges of vaccine mismatches for the next influenza seasons and adequate global supply of influenza vaccines limit its effectiveness. Protective immunity in vaccination or natural infection is primarily mediated by antibody responses against surface proteins of influenza including haemagglutinin (HA) as the major neutralizing target, whereas strong T cell responses to internal viral proteins are associated with reduced disease severity. Recently, identification of broadly neutralizing antibodies against the conserved stem region of HA from influenza infected individuals has invigorated interest in development of a universal vaccine against different subtypes of influenza. Moreover, because of the cross-reactive nature of T cell recognition and more conserved internal antigens of influenza, strategies that boost memory T cell responses to these internal antigens may provide not only help for antibody-mediated protection but also limit the cell damage caused by viral infection directly. This is particularly important in acute infection with new pandemic viruses or antibody-escape variants where there are no pre-existing neutralizing antibodies. Here, we review the protective immune correlates against human influenza infection and discuss current status of universal influenza vaccine development.Influenza is an acute respiratory viral infection with high mutation rate and pandemic potential. Vaccination is an effective means of prevention and control of influenza, but the challenges of vaccine mismatches for the next influenza seasons and adequate global supply of influenza vaccines limit its effectiveness. Protective immunity in vaccination or natural infection is primarily mediated by antibody responses against surface proteins of influenza including haemagglutinin (HA) as the major neutralizing target, whereas strong T cell responses to internal viral proteins are associated with reduced disease severity. Recently, identification of broadly neutralizing antibodies against the conserved stem region of HA from influenza infected individuals has invigorated interest in development of a universal vaccine against different subtypes of influenza. Moreover, because of the cross-reactive nature of T cell recognition and more conserved internal antigens of influenza, strategies that boost memory T cell responses to these internal antigens may provide not only help for antibody-mediated protection but also limit the cell damage caused by viral infection directly. This is particularly important in acute infection with new pandemic viruses or antibody-escape variants where there are no pre-existing neutralizing antibodies. Here, we review the protective immune correlates against human influenza infection and discuss current status of universal influenza vaccine development.
Highlights • Influenza infection is prevented by protective antibodies. • Flu-specific T cells can reduce viral load and disease severity. • Stem region of HA and flu internal proteins (NP and M1) are highly conserved among influenza virus. • Boosting antibody and T cell responses against conserved regions of flu proteins may be critical.
Author Rappuoli, Rino
Li, Chris Ka-fai
Xu, Xiao-Ning
Author_xml – sequence: 1
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  email: xiaoning.xu@imm.ox.ac.uk
  organization: Novartis Vaccines and Diagnostics, 1 via Fiorentina, Siena, Italy
BackLink https://www.ncbi.nlm.nih.gov/pubmed/23948572$$D View this record in MEDLINE/PubMed
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Snippet •Influenza infection is prevented by protective antibodies.•Flu-specific T cells can reduce viral load and disease severity.•Stem region of HA and flu internal...
Highlights • Influenza infection is prevented by protective antibodies. • Flu-specific T cells can reduce viral load and disease severity. • Stem region of HA...
Influenza is an acute respiratory viral infection with high mutation rate and pandemic potential. Vaccination is an effective means of prevention and control...
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SubjectTerms Allergy and Immunology
Animals
antigens
B-Lymphocytes - immunology
disease severity
Drug Design
hemagglutinins
human influenza
Humans
humoral immunity
Influenza Vaccines - immunology
Influenza, Human - immunology
Influenza, Human - prevention & control
mutation
neutralization
neutralizing antibodies
pandemic
surface proteins
T-lymphocytes
T-Lymphocytes - immunology
vaccination
vaccine development
vaccines
viral proteins
viruses
Title Correlates of protection against influenza infection in humans—on the path to a universal vaccine?
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https://dx.doi.org/10.1016/j.coi.2013.07.005
https://www.ncbi.nlm.nih.gov/pubmed/23948572
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Volume 25
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