Safety and immunogenicity of AS03B adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study
Identifieur interne : 002523 ( Istex/Corpus ); précédent : 002522; suivant : 002524Safety and immunogenicity of AS03B adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study
Auteurs : Claire S. Waddington ; W T Walker ; C. Oeser ; A. Reiner ; T. John ; S. Wilkins ; M. Casey ; P E Eccleston ; R J Allen ; I. Okike ; S. Ladhani ; E. Sheasby ; K. Hoschler ; N. Andrews ; P. Waight ; A C Collinson ; P T Heath ; A. Finn ; S N Faust ; M D Snape ; E. Miller ; A J PollardSource :
- BMJ [ 0959-8138 ] ; 2010.
English descriptors
- Teeft :
- Adjuvant, Adjuvanted, Adjuvanted split virion, Adjuvanted split virion vaccine, Adverse events, Assay, Children research network, Clinical research, Confidence interval, Data analysis, Diary card, Diary cards, Diary cards serum sample, Dose, Engl, European medicines agency, First vaccine dose, Haemagglutination, Haemagglutination inhibition, Haemagglutination inhibition assay, Haemagglutination inhibition titres, Health protection agency, High seroconversion rates, Immune response, Immunisation, Immunogenic, Immunogenicity, Influenza, Influenza vaccine, Influenza vaccines, Microneutralisation, Microneutralisation assay, More immunogenic, More reactogenic, Nihr, Older children, Older group, Online, Paediatric, Pandemic, Pandemic influenza, Parallel group, Participant, Programme, Protocol, Protocol time lines, Randomised, Reactogenicity, Research table, Seasonal influenza vaccines, Second dose, Second vaccine dose, Seroconversion, Serum sample, Serum samples, Special interest, Systemic reactions, Titre, Vaccination, Vaccine, Vaccine group, Vaccine manufacturers, Virion, Whole virion, Whole virion vaccine, Years adjuvanted split virion, Young children, Younger group.
Abstract
Objectives To compare the safety, reactogenicity, and immunogenicity of an adjuvanted split virion H1N1 vaccine and a non-adjuvanted whole virion vaccine used in the pandemic immunisation programme in the United Kingdom. Design Open label, randomised, parallel group, phase II study. Setting Five UK centres (Oxford, Southampton, Bristol, Exeter, and London). Participants Children aged 6 months to less than 13 years for whom a parent or guardian had provided written informed consent and who were able to comply with study procedures were eligible. Those with laboratory confirmed pandemic H1N1 influenza or clinically diagnosed disease meriting antiviral treatment, allergy to egg or any other vaccine components, or coagulation defects, or who were severely immunocompromised or had recently received blood products were excluded. Children were grouped by age: 6 months-<3 years (younger group) and 3-<13 years (older group). Recruitment was by media advertising and direct mailing. Recruitment visits were attended by 949 participants, of whom 943 were enrolled and 937 included in the per protocol analysis. Interventions Participants were randomised 1:1 to receive AS03B (tocopherol based oil in water emulsion) adjuvanted split virion vaccine derived from egg culture or non-adjuvanted whole virion vaccine derived from cell culture. Both were given as two doses 21 days apart. Reactogenicity data were collected for one week after immunisation by diary card. Serum samples were collected at baseline and after the second dose. Main outcome measures Primary reactogenicity end points were frequency and severity of fever, tenderness, swelling, and erythema after vaccination. Immunogenicity was measured by microneutralisation and haemagglutination inhibition assays. The primary immunogenicity objective was a comparison between vaccines of the percentage of participants showing seroconversion by the microneutralisation assay (fourfold rise to a titre of ≥1:40 from before vaccination to three weeks after the second dose). Results Seroconversion rates were higher after the adjuvanted split virion vaccine than after the whole virion vaccine, most notably in the youngest children (163 of 166 participants with paired serum samples (98.2%, 95% confidence interval 94.8% to 99.6%) v 157 of 196 (80.1%, 73.8% to 85.5%), P<0.001) in children under 3 years and 226 of 228 (99.1%, 96.9% to 99.9%) v 95.9%, 92.4% to 98.1%, P=0.03) in those over 3 years). The adjuvanted split virion vaccine was more reactogenic than the whole virion vaccine, with more frequent systemic reactions and severe local reactions in children aged over 5 years after dose one (13 (7.2%, 3.9% to 12%) v 2 (1.1%, 0.1% to 3.9%), P<0.001) and dose two (15 (8.5%, 4.8% to 13.7%) v 2 (1.1%, 0.1% to 4.1%), P<0.002) and after dose two in those under 5 years (15 (5.9%, 3.3% to 9.6%) v 0 (0.0%, 0% to 1.4%), P<0.001). Dose two of the adjuvanted split virion vaccine was more reactogenic than dose one, especially for fever ≥38ºC in those aged under 5 (24 (8.9%, 5.8% to 12.9%) v 57 (22.4%, 17.5% to 28.1%), P<0.001). Conclusions In this first direct comparison of an AS03B adjuvanted split virion versus whole virion non-adjuvanted H1N1 vaccine, the adjuvanted vaccine, while more reactogenic, was more immunogenic and, importantly, achieved high seroconversion rates in children aged less than 3 years. This indicates the potential for improved immunogenicity of influenza vaccines in this age group. Trial registration Clinical trials.gov NCT00980850; ISRCTN89141709.
Url:
DOI: 10.1136/bmj.c2649
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Waddington</name><affiliation><mods:affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</mods:affiliation></affiliation><affiliation><mods:affiliation>E-mail: claire.waddington@paediatrics.ox.ac.uk</mods:affiliation></affiliation></author><author><name sortKey="Walker, W T" sort="Walker, W T" uniqKey="Walker W" first="W T" last="Walker">W T Walker</name><affiliation><mods:affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</mods:affiliation></affiliation></author><author><name sortKey="Oeser, C" sort="Oeser, C" uniqKey="Oeser C" first="C" last="Oeser">C. Oeser</name><affiliation><mods:affiliation>St George’s Vaccine Institute, London SW17 0QT</mods:affiliation></affiliation></author><author><name sortKey="Reiner, A" sort="Reiner, A" uniqKey="Reiner A" first="A" last="Reiner">A. 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Hoschler</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Andrews, N" sort="Andrews, N" uniqKey="Andrews N" first="N" last="Andrews">N. Andrews</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Waight, P" sort="Waight, P" uniqKey="Waight P" first="P" last="Waight">P. Waight</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Collinson, A C" sort="Collinson, A C" uniqKey="Collinson A" first="A C" last="Collinson">A C Collinson</name><affiliation><mods:affiliation>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</mods:affiliation></affiliation></author><author><name sortKey="Heath, P T" sort="Heath, P T" uniqKey="Heath P" first="P T" last="Heath">P T Heath</name><affiliation><mods:affiliation>St George’s Vaccine Institute, London SW17 0QT</mods:affiliation></affiliation></author><author><name sortKey="Finn, A" sort="Finn, A" uniqKey="Finn A" first="A" last="Finn">A. Finn</name><affiliation><mods:affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</mods:affiliation></affiliation></author><author><name sortKey="Faust, S N" sort="Faust, S N" uniqKey="Faust S" first="S N" last="Faust">S N Faust</name><affiliation><mods:affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</mods:affiliation></affiliation></author><author><name sortKey="Snape, M D" sort="Snape, M D" uniqKey="Snape M" first="M D" last="Snape">M D Snape</name><affiliation><mods:affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</mods:affiliation></affiliation></author><author><name sortKey="Miller, E" sort="Miller, E" uniqKey="Miller E" first="E" last="Miller">E. Miller</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Pollard, A J" sort="Pollard, A J" uniqKey="Pollard A" first="A J" last="Pollard">A J Pollard</name><affiliation><mods:affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</mods:affiliation></affiliation></author></titleStmt><publicationStmt><idno type="wicri:source">ISTEX</idno><idno type="RBID">ISTEX:DA78FD80666CE56A8542B3559E5D4F78DD0533E0</idno><date when="2010" year="2010">2010</date><idno type="doi">10.1136/bmj.c2649</idno><idno type="url">https://api.istex.fr/ark:/67375/NVC-MTZB16DP-T/fulltext.pdf</idno><idno type="wicri:Area/Istex/Corpus">002523</idno><idno type="wicri:explorRef" wicri:stream="Istex" wicri:step="Corpus" wicri:corpus="ISTEX">002523</idno></publicationStmt><sourceDesc><biblStruct><analytic><title level="a">Safety and immunogenicity of AS03B adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study</title><author><name sortKey="Waddington, Claire S" sort="Waddington, Claire S" uniqKey="Waddington C" first="Claire S" last="Waddington">Claire S. Waddington</name><affiliation><mods:affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</mods:affiliation></affiliation><affiliation><mods:affiliation>E-mail: claire.waddington@paediatrics.ox.ac.uk</mods:affiliation></affiliation></author><author><name sortKey="Walker, W T" sort="Walker, W T" uniqKey="Walker W" first="W T" last="Walker">W T Walker</name><affiliation><mods:affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</mods:affiliation></affiliation></author><author><name sortKey="Oeser, C" sort="Oeser, C" uniqKey="Oeser C" first="C" last="Oeser">C. Oeser</name><affiliation><mods:affiliation>St George’s Vaccine Institute, London SW17 0QT</mods:affiliation></affiliation></author><author><name sortKey="Reiner, A" sort="Reiner, A" uniqKey="Reiner A" first="A" last="Reiner">A. Reiner</name><affiliation><mods:affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</mods:affiliation></affiliation></author><author><name sortKey="John, T" sort="John, T" uniqKey="John T" first="T" last="John">T. John</name><affiliation><mods:affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</mods:affiliation></affiliation></author><author><name sortKey="Wilkins, S" sort="Wilkins, S" uniqKey="Wilkins S" first="S" last="Wilkins">S. Wilkins</name><affiliation><mods:affiliation>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</mods:affiliation></affiliation></author><author><name sortKey="Casey, M" sort="Casey, M" uniqKey="Casey M" first="M" last="Casey">M. Casey</name><affiliation><mods:affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</mods:affiliation></affiliation></author><author><name sortKey="Eccleston, P E" sort="Eccleston, P E" uniqKey="Eccleston P" first="P E" last="Eccleston">P E Eccleston</name><affiliation><mods:affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</mods:affiliation></affiliation></author><author><name sortKey="Allen, R J" sort="Allen, R J" uniqKey="Allen R" first="R J" last="Allen">R J Allen</name><affiliation><mods:affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</mods:affiliation></affiliation></author><author><name sortKey="Okike, I" sort="Okike, I" uniqKey="Okike I" first="I" last="Okike">I. Okike</name><affiliation><mods:affiliation>St George’s Vaccine Institute, London SW17 0QT</mods:affiliation></affiliation></author><author><name sortKey="Ladhani, S" sort="Ladhani, S" uniqKey="Ladhani S" first="S" last="Ladhani">S. Ladhani</name><affiliation><mods:affiliation>St George’s Vaccine Institute, London SW17 0QT</mods:affiliation></affiliation><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Sheasby, E" sort="Sheasby, E" uniqKey="Sheasby E" first="E" last="Sheasby">E. Sheasby</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Hoschler, K" sort="Hoschler, K" uniqKey="Hoschler K" first="K" last="Hoschler">K. Hoschler</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Andrews, N" sort="Andrews, N" uniqKey="Andrews N" first="N" last="Andrews">N. Andrews</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Waight, P" sort="Waight, P" uniqKey="Waight P" first="P" last="Waight">P. Waight</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Collinson, A C" sort="Collinson, A C" uniqKey="Collinson A" first="A C" last="Collinson">A C Collinson</name><affiliation><mods:affiliation>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</mods:affiliation></affiliation></author><author><name sortKey="Heath, P T" sort="Heath, P T" uniqKey="Heath P" first="P T" last="Heath">P T Heath</name><affiliation><mods:affiliation>St George’s Vaccine Institute, London SW17 0QT</mods:affiliation></affiliation></author><author><name sortKey="Finn, A" sort="Finn, A" uniqKey="Finn A" first="A" last="Finn">A. Finn</name><affiliation><mods:affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</mods:affiliation></affiliation></author><author><name sortKey="Faust, S N" sort="Faust, S N" uniqKey="Faust S" first="S N" last="Faust">S N Faust</name><affiliation><mods:affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</mods:affiliation></affiliation></author><author><name sortKey="Snape, M D" sort="Snape, M D" uniqKey="Snape M" first="M D" last="Snape">M D Snape</name><affiliation><mods:affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</mods:affiliation></affiliation></author><author><name sortKey="Miller, E" sort="Miller, E" uniqKey="Miller E" first="E" last="Miller">E. Miller</name><affiliation><mods:affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</mods:affiliation></affiliation></author><author><name sortKey="Pollard, A J" sort="Pollard, A J" uniqKey="Pollard A" first="A J" last="Pollard">A J Pollard</name><affiliation><mods:affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</mods:affiliation></affiliation></author></analytic><monogr></monogr><series><title level="j">BMJ</title><title level="j" type="abbrev">BMJ</title><idno type="ISSN">0959-8138</idno><idno type="eISSN">1468-5833</idno><imprint><publisher>British Medical Journal Publishing Group</publisher><date type="published" when="2010">2010</date><biblScope unit="volume">340</biblScope></imprint><idno type="ISSN">0959-8138</idno></series></biblStruct></sourceDesc><seriesStmt><idno type="ISSN">0959-8138</idno></seriesStmt></fileDesc><profileDesc><textClass><keywords scheme="Teeft" xml:lang="en"><term>Adjuvant</term><term>Adjuvanted</term><term>Adjuvanted split virion</term><term>Adjuvanted split virion vaccine</term><term>Adverse events</term><term>Assay</term><term>Children research network</term><term>Clinical research</term><term>Confidence interval</term><term>Data analysis</term><term>Diary card</term><term>Diary cards</term><term>Diary cards serum sample</term><term>Dose</term><term>Engl</term><term>European medicines agency</term><term>First vaccine dose</term><term>Haemagglutination</term><term>Haemagglutination inhibition</term><term>Haemagglutination inhibition assay</term><term>Haemagglutination inhibition titres</term><term>Health protection agency</term><term>High seroconversion rates</term><term>Immune response</term><term>Immunisation</term><term>Immunogenic</term><term>Immunogenicity</term><term>Influenza</term><term>Influenza vaccine</term><term>Influenza vaccines</term><term>Microneutralisation</term><term>Microneutralisation assay</term><term>More immunogenic</term><term>More reactogenic</term><term>Nihr</term><term>Older children</term><term>Older group</term><term>Online</term><term>Paediatric</term><term>Pandemic</term><term>Pandemic influenza</term><term>Parallel group</term><term>Participant</term><term>Programme</term><term>Protocol</term><term>Protocol time lines</term><term>Randomised</term><term>Reactogenicity</term><term>Research table</term><term>Seasonal influenza vaccines</term><term>Second dose</term><term>Second vaccine dose</term><term>Seroconversion</term><term>Serum sample</term><term>Serum samples</term><term>Special interest</term><term>Systemic reactions</term><term>Titre</term><term>Vaccination</term><term>Vaccine</term><term>Vaccine group</term><term>Vaccine manufacturers</term><term>Virion</term><term>Whole virion</term><term>Whole virion vaccine</term><term>Years adjuvanted split virion</term><term>Young children</term><term>Younger group</term></keywords></textClass><langUsage><language ident="en">en</language></langUsage></profileDesc></teiHeader><front><div type="abstract">Objectives To compare the safety, reactogenicity, and immunogenicity of an adjuvanted split virion H1N1 vaccine and a non-adjuvanted whole virion vaccine used in the pandemic immunisation programme in the United Kingdom. Design Open label, randomised, parallel group, phase II study. Setting Five UK centres (Oxford, Southampton, Bristol, Exeter, and London). Participants Children aged 6 months to less than 13 years for whom a parent or guardian had provided written informed consent and who were able to comply with study procedures were eligible. Those with laboratory confirmed pandemic H1N1 influenza or clinically diagnosed disease meriting antiviral treatment, allergy to egg or any other vaccine components, or coagulation defects, or who were severely immunocompromised or had recently received blood products were excluded. Children were grouped by age: 6 months-<3 years (younger group) and 3-<13 years (older group). Recruitment was by media advertising and direct mailing. Recruitment visits were attended by 949 participants, of whom 943 were enrolled and 937 included in the per protocol analysis. Interventions Participants were randomised 1:1 to receive AS03B (tocopherol based oil in water emulsion) adjuvanted split virion vaccine derived from egg culture or non-adjuvanted whole virion vaccine derived from cell culture. Both were given as two doses 21 days apart. Reactogenicity data were collected for one week after immunisation by diary card. Serum samples were collected at baseline and after the second dose. Main outcome measures Primary reactogenicity end points were frequency and severity of fever, tenderness, swelling, and erythema after vaccination. Immunogenicity was measured by microneutralisation and haemagglutination inhibition assays. The primary immunogenicity objective was a comparison between vaccines of the percentage of participants showing seroconversion by the microneutralisation assay (fourfold rise to a titre of ≥1:40 from before vaccination to three weeks after the second dose). Results Seroconversion rates were higher after the adjuvanted split virion vaccine than after the whole virion vaccine, most notably in the youngest children (163 of 166 participants with paired serum samples (98.2%, 95% confidence interval 94.8% to 99.6%) v 157 of 196 (80.1%, 73.8% to 85.5%), P<0.001) in children under 3 years and 226 of 228 (99.1%, 96.9% to 99.9%) v 95.9%, 92.4% to 98.1%, P=0.03) in those over 3 years). The adjuvanted split virion vaccine was more reactogenic than the whole virion vaccine, with more frequent systemic reactions and severe local reactions in children aged over 5 years after dose one (13 (7.2%, 3.9% to 12%) v 2 (1.1%, 0.1% to 3.9%), P<0.001) and dose two (15 (8.5%, 4.8% to 13.7%) v 2 (1.1%, 0.1% to 4.1%), P<0.002) and after dose two in those under 5 years (15 (5.9%, 3.3% to 9.6%) v 0 (0.0%, 0% to 1.4%), P<0.001). Dose two of the adjuvanted split virion vaccine was more reactogenic than dose one, especially for fever ≥38ºC in those aged under 5 (24 (8.9%, 5.8% to 12.9%) v 57 (22.4%, 17.5% to 28.1%), P<0.001). Conclusions In this first direct comparison of an AS03B adjuvanted split virion versus whole virion non-adjuvanted H1N1 vaccine, the adjuvanted vaccine, while more reactogenic, was more immunogenic and, importantly, achieved high seroconversion rates in children aged less than 3 years. This indicates the potential for improved immunogenicity of influenza vaccines in this age group. 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manufacturers</json:string><json:string>participant</json:string><json:string>protocol</json:string></teeft></keywords><author><json:item><name>Claire S Waddington</name><affiliations><json:string>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</json:string><json:string>E-mail: claire.waddington@paediatrics.ox.ac.uk</json:string></affiliations></json:item><json:item><name>W T Walker</name><affiliations><json:string>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</json:string></affiliations></json:item><json:item><name>C Oeser</name><affiliations><json:string>St George’s Vaccine Institute, London SW17 0QT</json:string></affiliations></json:item><json:item><name>A Reiner</name><affiliations><json:string>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</json:string></affiliations></json:item><json:item><name>T John</name><affiliations><json:string>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</json:string></affiliations></json:item><json:item><name>S Wilkins</name><affiliations><json:string>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</json:string></affiliations></json:item><json:item><name>M Casey</name><affiliations><json:string>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</json:string></affiliations></json:item><json:item><name>P E Eccleston</name><affiliations><json:string>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</json:string></affiliations></json:item><json:item><name>R J Allen</name><affiliations><json:string>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</json:string></affiliations></json:item><json:item><name>I Okike</name><affiliations><json:string>St George’s Vaccine Institute, London SW17 0QT</json:string></affiliations></json:item><json:item><name>S Ladhani</name><affiliations><json:string>St George’s Vaccine Institute, London SW17 0QT</json:string><json:string>Centre for Infections, Health Protection Agency, London NW9 5EQ</json:string></affiliations></json:item><json:item><name>E Sheasby</name><affiliations><json:string>Centre for Infections, Health Protection Agency, London NW9 5EQ</json:string></affiliations></json:item><json:item><name>K Hoschler</name><affiliations><json:string>Centre for Infections, Health Protection Agency, London NW9 5EQ</json:string></affiliations></json:item><json:item><name>N Andrews</name><affiliations><json:string>Centre for Infections, Health Protection Agency, London NW9 5EQ</json:string></affiliations></json:item><json:item><name>P Waight</name><affiliations><json:string>Centre for Infections, Health Protection Agency, London NW9 5EQ</json:string></affiliations></json:item><json:item><name>A C Collinson</name><affiliations><json:string>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</json:string></affiliations></json:item><json:item><name>P T Heath</name><affiliations><json:string>St George’s Vaccine Institute, London SW17 0QT</json:string></affiliations></json:item><json:item><name>A Finn</name><affiliations><json:string>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</json:string></affiliations></json:item><json:item><name>S N Faust</name><affiliations><json:string>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</json:string></affiliations></json:item><json:item><name>M D Snape</name><affiliations><json:string>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</json:string></affiliations></json:item><json:item><name>E Miller</name><affiliations><json:string>Centre for Infections, Health Protection Agency, London NW9 5EQ</json:string></affiliations></json:item><json:item><name>A J Pollard</name><affiliations><json:string>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</json:string></affiliations></json:item></author><articleId><json:string>wadc777714</json:string></articleId><arkIstex>ark:/67375/NVC-MTZB16DP-T</arkIstex><language><json:string>eng</json:string></language><originalGenre><json:string>research-article</json:string></originalGenre><abstract>Objectives To compare the safety, reactogenicity, and immunogenicity of an adjuvanted split virion H1N1 vaccine and a non-adjuvanted whole virion vaccine used in the pandemic immunisation programme in the United Kingdom. Design Open label, randomised, parallel group, phase II study. Setting Five UK centres (Oxford, Southampton, Bristol, Exeter, and London). Participants Children aged 6 months to less than 13 years for whom a parent or guardian had provided written informed consent and who were able to comply with study procedures were eligible. Those with laboratory confirmed pandemic H1N1 influenza or clinically diagnosed disease meriting antiviral treatment, allergy to egg or any other vaccine components, or coagulation defects, or who were severely immunocompromised or had recently received blood products were excluded. Children were grouped by age: 6 months->3 years (younger group) and 3->13 years (older group). Recruitment was by media advertising and direct mailing. Recruitment visits were attended by 949 participants, of whom 943 were enrolled and 937 included in the per protocol analysis. Interventions Participants were randomised 1:1 to receive AS03B (tocopherol based oil in water emulsion) adjuvanted split virion vaccine derived from egg culture or non-adjuvanted whole virion vaccine derived from cell culture. Both were given as two doses 21 days apart. Reactogenicity data were collected for one week after immunisation by diary card. Serum samples were collected at baseline and after the second dose. Main outcome measures Primary reactogenicity end points were frequency and severity of fever, tenderness, swelling, and erythema after vaccination. Immunogenicity was measured by microneutralisation and haemagglutination inhibition assays. The primary immunogenicity objective was a comparison between vaccines of the percentage of participants showing seroconversion by the microneutralisation assay (fourfold rise to a titre of ≥1:40 from before vaccination to three weeks after the second dose). Results Seroconversion rates were higher after the adjuvanted split virion vaccine than after the whole virion vaccine, most notably in the youngest children (163 of 166 participants with paired serum samples (98.2%, 95% confidence interval 94.8% to 99.6%) v 157 of 196 (80.1%, 73.8% to 85.5%), P>0.001) in children under 3 years and 226 of 228 (99.1%, 96.9% to 99.9%) v 95.9%, 92.4% to 98.1%, P=0.03) in those over 3 years). The adjuvanted split virion vaccine was more reactogenic than the whole virion vaccine, with more frequent systemic reactions and severe local reactions in children aged over 5 years after dose one (13 (7.2%, 3.9% to 12%) v 2 (1.1%, 0.1% to 3.9%), P>0.001) and dose two (15 (8.5%, 4.8% to 13.7%) v 2 (1.1%, 0.1% to 4.1%), P>0.002) and after dose two in those under 5 years (15 (5.9%, 3.3% to 9.6%) v 0 (0.0%, 0% to 1.4%), P>0.001). Dose two of the adjuvanted split virion vaccine was more reactogenic than dose one, especially for fever ≥38ºC in those aged under 5 (24 (8.9%, 5.8% to 12.9%) v 57 (22.4%, 17.5% to 28.1%), P>0.001). Conclusions In this first direct comparison of an AS03B adjuvanted split virion versus whole virion non-adjuvanted H1N1 vaccine, the adjuvanted vaccine, while more reactogenic, was more immunogenic and, importantly, achieved high seroconversion rates in children aged less than 3 years. This indicates the potential for improved immunogenicity of influenza vaccines in this age group. Trial registration Clinical trials.gov NCT00980850; ISRCTN89141709.</abstract><qualityIndicators><score>10</score><pdfWordCount>7459</pdfWordCount><pdfCharCount>46037</pdfCharCount><pdfVersion>1.6</pdfVersion><pdfPageCount>11</pdfPageCount><pdfPageSize>595 x 794 pts</pdfPageSize><refBibsNative>true</refBibsNative><abstractWordCount>536</abstractWordCount><abstractCharCount>3544</abstractCharCount><keywordCount>0</keywordCount></qualityIndicators><title>Safety and immunogenicity of AS03B adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study</title><pmid><json:string>20508026</json:string></pmid><genre><json:string>research-article</json:string></genre><host><title>BMJ</title><language><json:string>unknown</json:string></language><issn><json:string>0959-8138</json:string></issn><eissn><json:string>1468-5833</json:string></eissn><publisherId><json:string>bmj</json:string></publisherId><volume>340</volume><genre><json:string>journal</json:string></genre><subject><json:item><value>Infectious diseases</value></json:item><json:item><value>Immunology (including allergy)</value></json:item><json:item><value>Child health</value></json:item><json:item><value>Dermatology</value></json:item><json:item><value>Informed consent</value></json:item><json:item><value>Legal and forensic medicine</value></json:item></subject></host><namedEntities><unitex><date><json:string>2009</json:string><json:string>2010-05-27</json:string><json:string>April-June 2009</json:string></date><geogName></geogName><orgName><json:string>WTW, CO</json:string><json:string>ACIP</json:string><json:string>National Institute of Health Research</json:string><json:string>BRC</json:string><json:string>NIHR</json:string><json:string>Children Research Network</json:string><json:string>NHS</json:string><json:string>Oxfordshire Research Ethics Committee A</json:string><json:string>Advisory Committee on Immunization Practices</json:string><json:string>Clinical Trials Research Governance, University of Oxford</json:string><json:string>Vaccine Institute, London SW</json:string><json:string>University of Southampton Wellcome Trust Clinical Research Facility and Division</json:string><json:string>National Institute BMJ</json:string><json:string>UK Department of Health</json:string><json:string>European Commission</json:string><json:string>NRES</json:string><json:string>Products Regulatory Agency</json:string><json:string>Department of Paediatrics, University of Oxford, Oxford OX</json:string><json:string>Trust Research and Development Office, Child Health Computer Departments of Primary Care Trusts</json:string><json:string>NHS Foundation Trust and University</json:string><json:string>Biomedical Research Unit</json:string><json:string>Health Protection Agency, London</json:string><json:string>NHS Foundation Trust, Exeter EX</json:string><json:string>MCRN</json:string><json:string>RESEARCH Table</json:string><json:string>US Food and Drug</json:string><json:string>Local Research Networks</json:string><json:string>National Research Ethics Service</json:string><json:string>Oxford Biomedical Research Centre</json:string><json:string>Comprehensive Local Research Networks</json:string><json:string>MHRA</json:string><json:string>Healthcare Products Regulatory Agency</json:string><json:string>European Medicines Agency</json:string><json:string>Health Protection Agency</json:string><json:string>Southampton University</json:string><json:string>Oxford Comprehensive Biomedical Research Centre</json:string><json:string>UK Medicines and Healthcare</json:string><json:string>Jenner Institute Investigator</json:string><json:string>Health Protection Agency Centre for Infections</json:string><json:string>National Health Service</json:string><json:string>NIHR Health Technology Assessment Programme</json:string></orgName><orgName_funder><json:string>NIHR Health Technology Assessment Programme</json:string></orgName_funder><orgName_provider></orgName_provider><persName><json:string>Simon Bevan</json:string><json:string>Our</json:string><json:string>Any Diarrhoea</json:string><json:string>M. Incidence</json:string><json:string>K. Responses</json:string><json:string>Elizabeth Miller</json:string><json:string>Philip Monk</json:string><json:string>Stephen Evans</json:string><json:string>Paula Williamson</json:string><json:string>Any Headache</json:string><json:string>Any Redness</json:string><json:string>Any Nausea</json:string><json:string>Delane Shingadia</json:string><json:string>Heather House</json:string><json:string>Rev</json:string><json:string>Andrew Pollard</json:string><json:string>Simon Knoll</json:string><json:string>Stephen Welch</json:string><json:string>Chris Verit</json:string></persName><placeName><json:string>Stanford</json:string><json:string>Bristol</json:string><json:string>Southampton</json:string><json:string>Reactogenicity</json:string><json:string>United States</json:string><json:string>UK</json:string><json:string>Richmond</json:string><json:string>Markendorf</json:string><json:string>Houston</json:string><json:string>Immunogenicity</json:string><json:string>St 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infectieuse</json:string></inist></categories><publicationDate>2010</publicationDate><copyrightDate>2010</copyrightDate><doi><json:string>10.1136/bmj.c2649</json:string></doi><id>DA78FD80666CE56A8542B3559E5D4F78DD0533E0</id><score>1</score><fulltext><json:item><extension>pdf</extension><original>true</original><mimetype>application/pdf</mimetype><uri>https://api.istex.fr/ark:/67375/NVC-MTZB16DP-T/fulltext.pdf</uri></json:item><json:item><extension>zip</extension><original>false</original><mimetype>application/zip</mimetype><uri>https://api.istex.fr/ark:/67375/NVC-MTZB16DP-T/bundle.zip</uri></json:item><istex:fulltextTEI uri="https://api.istex.fr/ark:/67375/NVC-MTZB16DP-T/fulltext.tei"><teiHeader><fileDesc><titleStmt><title level="a">Safety and immunogenicity of AS03B adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study</title></titleStmt><publicationStmt><authority>ISTEX</authority><publisher scheme="https://publisher-list.data.istex.fr">British Medical Journal Publishing Group</publisher><availability status="free"><p>Open Access</p></availability><date>2010-05-27</date></publicationStmt><notesStmt><note type="research-article" scheme="https://content-type.data.istex.fr/ark:/67375/XTP-1JC4F85T-7">research-article</note><note type="journal" scheme="https://publication-type.data.istex.fr/ark:/67375/JMC-0GLKJH51-B">journal</note></notesStmt><sourceDesc><biblStruct type="inbook"><analytic><title level="a">Safety and immunogenicity of AS03B adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study</title><author xml:id="author-0000" corresp="yes"><persName><forename type="first">Claire S</forename><surname>Waddington</surname></persName><email>claire.waddington@paediatrics.ox.ac.uk</email><note type="biography">clinical research fellow</note><affiliation>clinical research fellow</affiliation><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation></author><author xml:id="author-0001"><persName><forename type="first">W T</forename><surname>Walker</surname></persName><note type="biography">Wellcome Trust clinical research facility fellow</note><affiliation>Wellcome Trust clinical research facility fellow</affiliation><affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</affiliation></author><author xml:id="author-0002"><persName><forename type="first">C</forename><surname>Oeser</surname></persName><note type="biography">clinical research fellow</note><affiliation>clinical research fellow</affiliation><affiliation>St George’s Vaccine Institute, London SW17 0QT</affiliation></author><author xml:id="author-0003"><persName><forename type="first">A</forename><surname>Reiner</surname></persName><note type="biography">project manager</note><affiliation>project manager</affiliation><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation></author><author xml:id="author-0004"><persName><forename type="first">T</forename><surname>John</surname></persName><note type="biography">clinical team lead</note><affiliation>clinical team lead</affiliation><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation></author><author xml:id="author-0005"><persName><forename type="first">S</forename><surname>Wilkins</surname></persName><note type="biography">research nurse</note><affiliation>research nurse</affiliation><affiliation>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</affiliation></author><author xml:id="author-0006"><persName><forename type="first">M</forename><surname>Casey</surname></persName><note type="biography">children’s senior research sister</note><affiliation>children’s senior research sister</affiliation><affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</affiliation></author><author xml:id="author-0007"><persName><forename type="first">P E</forename><surname>Eccleston</surname></persName><note type="biography">data manager</note><affiliation>data manager</affiliation><affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</affiliation></author><author xml:id="author-0008"><persName><forename type="first">R J</forename><surname>Allen</surname></persName><note type="biography">research network manager</note><affiliation>research network manager</affiliation><affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</affiliation></author><author xml:id="author-0009"><persName><forename type="first">I</forename><surname>Okike</surname></persName><note type="biography">clinical research fellow</note><affiliation>clinical research fellow</affiliation><affiliation>St George’s Vaccine Institute, London SW17 0QT</affiliation></author><author xml:id="author-0010"><persName><forename type="first">S</forename><surname>Ladhani</surname></persName><note type="biography">consultant in paediatric infectious diseases</note><affiliation>consultant in paediatric infectious diseases</affiliation><affiliation>St George’s Vaccine Institute, London SW17 0QT</affiliation><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation></author><author xml:id="author-0011"><persName><forename type="first">E</forename><surname>Sheasby</surname></persName><note type="biography">quality manager</note><affiliation>quality manager</affiliation><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation></author><author xml:id="author-0012"><persName><forename type="first">K</forename><surname>Hoschler</surname></persName><note type="biography">advanced healthcare scientist and clinical scientist</note><affiliation>advanced healthcare scientist and clinical scientist</affiliation><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation></author><author xml:id="author-0013"><persName><forename type="first">N</forename><surname>Andrews</surname></persName><note type="biography">senior statistician</note><affiliation>senior statistician</affiliation><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation></author><author xml:id="author-0014"><persName><forename type="first">P</forename><surname>Waight</surname></persName><note type="biography">senior scientific data analyst</note><affiliation>senior scientific data analyst</affiliation><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation></author><author xml:id="author-0015"><persName><forename type="first">A C</forename><surname>Collinson</surname></persName><note type="biography">consultant paediatrician, co-director of Medicines for Children Research Network, south west</note><affiliation>consultant paediatrician, co-director of Medicines for Children Research Network, south west</affiliation><affiliation>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</affiliation></author><author xml:id="author-0016"><persName><forename type="first">P T</forename><surname>Heath</surname></persName><note type="biography">reader, honorary consultant in paediatric infectious diseases, executive officer paediatric studies</note><affiliation>reader, honorary consultant in paediatric infectious diseases, executive officer paediatric studies</affiliation><affiliation>St George’s Vaccine Institute, London SW17 0QT</affiliation></author><author xml:id="author-0017"><persName><forename type="first">A</forename><surname>Finn</surname></persName><note type="biography">David Baum professor of paediatrics, director of Medicines for Children Research Network, south west</note><affiliation>David Baum professor of paediatrics, director of Medicines for Children Research Network, south west</affiliation><affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</affiliation></author><author xml:id="author-0018"><persName><forename type="first">S N</forename><surname>Faust</surname></persName><note type="biography">senior lecturer in paediatric immunology and infectious diseases, director Wellcome Trust clinical research facility</note><affiliation>senior lecturer in paediatric immunology and infectious diseases, director Wellcome Trust clinical research facility</affiliation><affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</affiliation></author><author xml:id="author-0019"><persName><forename type="first">M D</forename><surname>Snape</surname></persName><note type="biography">consultant paediatrician and vaccinologist</note><affiliation>consultant paediatrician and vaccinologist</affiliation><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation></author><author xml:id="author-0020"><persName><forename type="first">E</forename><surname>Miller</surname></persName><note type="biography">professor, consultant epidemiologist</note><affiliation>professor, consultant epidemiologist</affiliation><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation></author><author xml:id="author-0021"><persName><forename type="first">A J</forename><surname>Pollard</surname></persName><note type="biography">professor of paediatric infection and immunity, director of the Oxford Vaccine Group, honorary consultant paediatrician</note><affiliation>professor of paediatric infection and immunity, director of the Oxford Vaccine Group, honorary consultant paediatrician</affiliation><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation></author><idno type="istex">DA78FD80666CE56A8542B3559E5D4F78DD0533E0</idno><idno type="ark">ark:/67375/NVC-MTZB16DP-T</idno><idno type="DOI">10.1136/bmj.c2649</idno><idno type="href">bmj-340-bmj-c2649.pdf</idno><idno type="article-id">wadc777714</idno><idno type="PMID">20508026</idno><idno type="local">bmj;340/may27_1/c2649</idno></analytic><monogr><title level="j">BMJ</title><title level="j" type="abbrev">BMJ</title><idno type="pISSN">0959-8138</idno><idno type="eISSN">1468-5833</idno><idno type="publisher-id">bmj</idno><idno type="PublisherID-hwp">bmj</idno><idno type="PublisherID-nlm-ta">BMJ</idno><imprint><publisher>British Medical Journal Publishing Group</publisher><date type="published" when="2010"></date><biblScope unit="volume">340</biblScope></imprint></monogr></biblStruct></sourceDesc></fileDesc><profileDesc><creation><date>2010-05-27</date></creation><langUsage><language ident="en">en</language></langUsage><abstract><p>Objectives To compare the safety, reactogenicity, and immunogenicity of an adjuvanted split virion H1N1 vaccine and a non-adjuvanted whole virion vaccine used in the pandemic immunisation programme in the United Kingdom. Design Open label, randomised, parallel group, phase II study. Setting Five UK centres (Oxford, Southampton, Bristol, Exeter, and London). Participants Children aged 6 months to less than 13 years for whom a parent or guardian had provided written informed consent and who were able to comply with study procedures were eligible. Those with laboratory confirmed pandemic H1N1 influenza or clinically diagnosed disease meriting antiviral treatment, allergy to egg or any other vaccine components, or coagulation defects, or who were severely immunocompromised or had recently received blood products were excluded. Children were grouped by age: 6 months-<3 years (younger group) and 3-<13 years (older group). Recruitment was by media advertising and direct mailing. Recruitment visits were attended by 949 participants, of whom 943 were enrolled and 937 included in the per protocol analysis. Interventions Participants were randomised 1:1 to receive AS03B (tocopherol based oil in water emulsion) adjuvanted split virion vaccine derived from egg culture or non-adjuvanted whole virion vaccine derived from cell culture. Both were given as two doses 21 days apart. Reactogenicity data were collected for one week after immunisation by diary card. Serum samples were collected at baseline and after the second dose. Main outcome measures Primary reactogenicity end points were frequency and severity of fever, tenderness, swelling, and erythema after vaccination. Immunogenicity was measured by microneutralisation and haemagglutination inhibition assays. The primary immunogenicity objective was a comparison between vaccines of the percentage of participants showing seroconversion by the microneutralisation assay (fourfold rise to a titre of ≥1:40 from before vaccination to three weeks after the second dose). Results Seroconversion rates were higher after the adjuvanted split virion vaccine than after the whole virion vaccine, most notably in the youngest children (163 of 166 participants with paired serum samples (98.2%, 95% confidence interval 94.8% to 99.6%) v 157 of 196 (80.1%, 73.8% to 85.5%), P<0.001) in children under 3 years and 226 of 228 (99.1%, 96.9% to 99.9%) v 95.9%, 92.4% to 98.1%, P=0.03) in those over 3 years). The adjuvanted split virion vaccine was more reactogenic than the whole virion vaccine, with more frequent systemic reactions and severe local reactions in children aged over 5 years after dose one (13 (7.2%, 3.9% to 12%) v 2 (1.1%, 0.1% to 3.9%), P<0.001) and dose two (15 (8.5%, 4.8% to 13.7%) v 2 (1.1%, 0.1% to 4.1%), P<0.002) and after dose two in those under 5 years (15 (5.9%, 3.3% to 9.6%) v 0 (0.0%, 0% to 1.4%), P<0.001). Dose two of the adjuvanted split virion vaccine was more reactogenic than dose one, especially for fever ≥38ºC in those aged under 5 (24 (8.9%, 5.8% to 12.9%) v 57 (22.4%, 17.5% to 28.1%), P<0.001). Conclusions In this first direct comparison of an AS03B adjuvanted split virion versus whole virion non-adjuvanted H1N1 vaccine, the adjuvanted vaccine, while more reactogenic, was more immunogenic and, importantly, achieved high seroconversion rates in children aged less than 3 years. This indicates the potential for improved immunogenicity of influenza vaccines in this age group. Trial registration Clinical trials.gov NCT00980850; ISRCTN89141709.</p></abstract><textClass><keywords scheme="Journal Subject"><list><head>hwp-journal-coll</head><item><term>Infectious diseases</term></item></list></keywords></textClass><textClass><keywords scheme="Journal Subject"><list><head>hwp-journal-coll</head><item><term>Immunology (including allergy)</term></item></list></keywords></textClass><textClass><keywords scheme="Journal Subject"><list><head>hwp-journal-coll</head><item><term>Child health</term></item></list></keywords></textClass><textClass><keywords scheme="Journal Subject"><list><head>hwp-journal-coll</head><item><term>Dermatology</term></item></list></keywords></textClass><textClass><keywords scheme="Journal Subject"><list><head>hwp-journal-coll</head><item><term>Informed consent</term></item></list></keywords></textClass><textClass><keywords scheme="Journal Subject"><list><head>hwp-journal-coll</head><item><term>Legal and forensic medicine</term></item></list></keywords></textClass></profileDesc><revisionDesc><change when="2010-05-27">Created</change><change when="2010">Published</change></revisionDesc></teiHeader></istex:fulltextTEI><json:item><extension>txt</extension><original>false</original><mimetype>text/plain</mimetype><uri>https://api.istex.fr/ark:/67375/NVC-MTZB16DP-T/fulltext.txt</uri></json:item></fulltext><metadata><istex:metadataXml wicri:clean="corpus bmj" wicri:toSee="no header"><istex:xmlDeclaration>version="1.0" encoding="UTF-8" standalone="no"</istex:xmlDeclaration><istex:docType PUBLIC="-//NLM//DTD Journal Archiving and Interchange DTD v2.3 20070202//EN" URI="archivearticle.dtd" name="istex:docType"></istex:docType><istex:document><article article-type="research-article"><front><journal-meta><journal-id journal-id-type="hwp">bmj</journal-id><journal-id journal-id-type="nlm-ta">BMJ</journal-id><journal-id journal-id-type="publisher-id">bmj</journal-id><journal-title>BMJ</journal-title><abbrev-journal-title abbrev-type="publisher">BMJ</abbrev-journal-title><issn pub-type="ppub">0959-8138</issn><issn pub-type="epub">1468-5833</issn><publisher><publisher-name>British Medical Journal Publishing Group</publisher-name></publisher></journal-meta><article-meta><article-id pub-id-type="publisher-id">wadc777714</article-id><article-id pub-id-type="doi">10.1136/bmj.c2649</article-id><article-id pub-id-type="other">bmj;340/may27_1/c2649</article-id><article-id pub-id-type="other">bmj;bmj.c2649</article-id><article-id pub-id-type="other">may27_1</article-id><article-id pub-id-type="pmid">20508026</article-id><article-id pub-id-type="other">bmj.c2649</article-id><article-id pub-id-type="other">bmj.c2649</article-id><article-categories><subj-group subj-group-type="heading"><subject>Research</subject></subj-group><subj-group subj-group-type="hwp-journal-coll"><subject>Infectious diseases</subject></subj-group><subj-group subj-group-type="hwp-journal-coll"><subject>Immunology (including allergy)</subject></subj-group><subj-group subj-group-type="hwp-journal-coll"><subject>Child health</subject></subj-group><subj-group subj-group-type="hwp-journal-coll"><subject>Dermatology</subject></subj-group><subj-group subj-group-type="hwp-journal-coll"><subject>Informed consent</subject></subj-group><subj-group subj-group-type="hwp-journal-coll"><subject>Legal and forensic medicine</subject></subj-group></article-categories><title-group><article-title>Safety and immunogenicity of AS03<sub>B</sub> adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study</article-title></title-group><contrib-group><contrib contrib-type="author" corresp="yes"><name><surname>Waddington</surname><given-names>Claire S</given-names></name><role>clinical research fellow</role><xref ref-type="aff" rid="aff1">1</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Walker</surname><given-names>W T</given-names></name><role>Wellcome Trust clinical research facility fellow</role><xref ref-type="aff" rid="aff2">2</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Oeser</surname><given-names>C</given-names></name><role>clinical research fellow</role><xref ref-type="aff" rid="aff3">3</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Reiner</surname><given-names>A</given-names></name><role>project manager</role><xref ref-type="aff" rid="aff1">1</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>John</surname><given-names>T</given-names></name><role>clinical team lead</role><xref ref-type="aff" rid="aff1">1</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Wilkins</surname><given-names>S</given-names></name><role>research nurse</role><xref ref-type="aff" rid="aff4">4</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Casey</surname><given-names>M</given-names></name><role>children’s senior research sister</role><xref ref-type="aff" rid="aff2">2</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Eccleston</surname><given-names>P E</given-names></name><role>data manager</role><xref ref-type="aff" rid="aff5">5</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Allen</surname><given-names>R J</given-names></name><role>research network manager</role><xref ref-type="aff" rid="aff5">5</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Okike</surname><given-names>I</given-names></name><role>clinical research fellow</role><xref ref-type="aff" rid="aff3">3</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Ladhani</surname><given-names>S</given-names></name><role>consultant in paediatric infectious diseases</role><xref ref-type="aff" rid="aff3">3</xref><xref ref-type="aff" rid="aff6">6</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Sheasby</surname><given-names>E</given-names></name><role>quality manager</role><xref ref-type="aff" rid="aff6">6</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Hoschler</surname><given-names>K</given-names></name><role>advanced healthcare scientist and clinical scientist</role><xref ref-type="aff" rid="aff6">6</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Andrews</surname><given-names>N</given-names></name><role>senior statistician</role><xref ref-type="aff" rid="aff6">6</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Waight</surname><given-names>P</given-names></name><role>senior scientific data analyst</role><xref ref-type="aff" rid="aff6">6</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Collinson</surname><given-names>A C</given-names></name><role>consultant paediatrician, co-director of Medicines for Children Research Network, south west</role><xref ref-type="aff" rid="aff4">4</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Heath</surname><given-names>P T</given-names></name><role>reader, honorary consultant in paediatric infectious diseases, executive officer paediatric studies</role><xref ref-type="aff" rid="aff3">3</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Finn</surname><given-names>A</given-names></name><role>David Baum professor of paediatrics, director of Medicines for Children Research Network, south west</role><xref ref-type="aff" rid="aff5">5</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Faust</surname><given-names>S N</given-names></name><role>senior lecturer in paediatric immunology and infectious diseases, director Wellcome Trust clinical research facility</role><xref ref-type="aff" rid="aff2">2</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Snape</surname><given-names>M D</given-names></name><role>consultant paediatrician and vaccinologist</role><xref ref-type="aff" rid="aff1">1</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Miller</surname><given-names>E</given-names></name><role>professor, consultant epidemiologist</role><xref ref-type="aff" rid="aff6">6</xref></contrib><contrib contrib-type="author" corresp="no"><name><surname>Pollard</surname><given-names>A J</given-names></name><role>professor of paediatric infection and immunity, director of the Oxford Vaccine Group, honorary consultant paediatrician</role><xref ref-type="aff" rid="aff1">1</xref></contrib><aff id="aff1"><label>1</label>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ </aff><aff id="aff2"><label>2</label>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</aff><aff id="aff3"><label>3</label>St George’s Vaccine Institute, London SW17 0QT </aff><aff id="aff4"><label>4</label>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW </aff><aff id="aff5"><label>5</label>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE </aff><aff id="aff6"><label>6</label>Centre for Infections, Health Protection Agency, London NW9 5EQ</aff></contrib-group><author-notes><corresp>Correspondence to: C S Waddington <email>claire.waddington@paediatrics.ox.ac.uk</email></corresp></author-notes><pub-date pub-type="collection"><year>2010</year></pub-date><pub-date pub-type="ppub"><year>2010</year></pub-date><pub-date pub-type="epub-original"><year>2010</year></pub-date><pub-date pub-type="epub"><day>27</day><month>5</month><year>2010</year></pub-date><volume>340</volume><volume-id pub-id-type="other">340</volume-id><volume-id pub-id-type="other">340</volume-id><elocation-id>c2649</elocation-id><history><date date-type="accepted"><day>12</day><month>May</month><year>2010</year></date></history><permissions><copyright-statement>© Waddington et al 2010</copyright-statement><copyright-year>2010</copyright-year><copyright-holder>Waddington et al</copyright-holder><license license-type="open-access"><p>This is an open-access article distributed under the terms of the Creative Commons Attribution Non-commercial License, which permits use, distribution, and reproduction in any medium, provided the original work is properly cited, the use is non commercial and is otherwise in compliance with the license. See: <ext-link xlink:href="http://creativecommons.org/licenses/by-nc/2.0/" ext-link-type="uri">http://creativecommons.org/licenses/by-nc/2.0/</ext-link> and <ext-link xlink:href="http://creativecommons.org/licenses/by-nc/2.0/legalcode" ext-link-type="uri">http://creativecommons.org/licenses/by-nc/2.0/legalcode</ext-link>.</p></license></permissions><self-uri content-type="pdf" xlink:role="full-text" xlink:href="bmj-340-bmj-c2649.pdf"></self-uri><abstract><p><bold>Objectives</bold> To compare the safety, reactogenicity, and immunogenicity of an adjuvanted split virion H1N1 vaccine and a non-adjuvanted whole virion vaccine used in the pandemic immunisation programme in the United Kingdom.</p><p><bold>Design</bold> Open label, randomised, parallel group, phase II study.</p><p><bold>Setting</bold> Five UK centres (Oxford, Southampton, Bristol, Exeter, and London).</p><p><bold>Participants</bold> Children aged 6 months to less than 13 years for whom a parent or guardian had provided written informed consent and who were able to comply with study procedures were eligible. Those with laboratory confirmed pandemic H1N1 influenza or clinically diagnosed disease meriting antiviral treatment, allergy to egg or any other vaccine components, or coagulation defects, or who were severely immunocompromised or had recently received blood products were excluded. Children were grouped by age: 6 months-<3 years (younger group) and 3-<13 years (older group). Recruitment was by media advertising and direct mailing. Recruitment visits were attended by 949 participants, of whom 943 were enrolled and 937 included in the per protocol analysis.</p><p><bold>Interventions</bold> Participants were randomised 1:1 to receive AS03<sub>B</sub> (tocopherol based oil in water emulsion) adjuvanted split virion vaccine derived from egg culture or non-adjuvanted whole virion vaccine derived from cell culture. Both were given as two doses 21 days apart. Reactogenicity data were collected for one week after immunisation by diary card. Serum samples were collected at baseline and after the second dose.</p><p><bold>Main outcome measures</bold> Primary reactogenicity end points were frequency and severity of fever, tenderness, swelling, and erythema after vaccination. Immunogenicity was measured by microneutralisation and haemagglutination inhibition assays. The primary immunogenicity objective was a comparison between vaccines of the percentage of participants showing seroconversion by the microneutralisation assay (fourfold rise to a titre of ≥1:40 from before vaccination to three weeks after the second dose).</p><p><bold>Results</bold> Seroconversion rates were higher after the adjuvanted split virion vaccine than after the whole virion vaccine, most notably in the youngest children (163 of 166 participants with paired serum samples (98.2%, 95% confidence interval 94.8% to 99.6%) <italic>v</italic> 157 of 196 (80.1%, 73.8% to 85.5%), P<0.001) in children under 3 years and 226 of 228 (99.1%, 96.9% to 99.9%) <italic>v</italic> 95.9%, 92.4% to 98.1%, P=0.03) in those over 3 years). The adjuvanted split virion vaccine was more reactogenic than the whole virion vaccine, with more frequent systemic reactions and severe local reactions in children aged over 5 years after dose one (13 (7.2%, 3.9% to 12%) <italic>v</italic> 2 (1.1%, 0.1% to 3.9%), P<0.001) and dose two (15 (8.5%, 4.8% to 13.7%) <italic>v</italic> 2 (1.1%, 0.1% to 4.1%), P<0.002) and after dose two in those under 5 years (15 (5.9%, 3.3% to 9.6%) <italic>v</italic> 0 (0.0%, 0% to 1.4%), P<0.001). Dose two of the adjuvanted split virion vaccine was more reactogenic than dose one, especially for fever ≥38ºC in those aged under 5 (24 (8.9%, 5.8% to 12.9%) <italic>v</italic> 57 (22.4%, 17.5% to 28.1%), P<0.001).</p><p><bold>Conclusions</bold> In this first direct comparison of an AS03<sub>B</sub> adjuvanted split virion versus whole virion non-adjuvanted H1N1 vaccine, the adjuvanted vaccine, while more reactogenic, was more immunogenic and, importantly, achieved high seroconversion rates in children aged less than 3 years. This indicates the potential for improved immunogenicity of influenza vaccines in this age group.</p><p><bold>Trial registration</bold> Clinical trials.gov <ext-link ext-link-type="clintrialgov" xlink:href="NCT00980850">NCT00980850</ext-link>; <ext-link ext-link-type="isrctn" xlink:href="ISRCTN89141709">ISRCTN89141709</ext-link>.</p></abstract></article-meta></front></article></istex:document></istex:metadataXml><mods version="3.6"><titleInfo><title>Safety and immunogenicity of AS03B adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study</title></titleInfo><titleInfo type="alternative" contentType="CDATA"><title>Safety and immunogenicity of AS03B adjuvanted split virion versus non-adjuvanted whole virion H1N1 influenza vaccine in UK children aged 6 months-12 years: open label, randomised, parallel group, multicentre study</title></titleInfo><name type="personal" displayLabel="corresp"><namePart type="given">Claire S</namePart><namePart type="family">Waddington</namePart><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation><affiliation>E-mail: claire.waddington@paediatrics.ox.ac.uk</affiliation><description>clinical research fellow</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">W T</namePart><namePart type="family">Walker</namePart><affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</affiliation><description>Wellcome Trust clinical research facility fellow</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">C</namePart><namePart type="family">Oeser</namePart><affiliation>St George’s Vaccine Institute, London SW17 0QT</affiliation><description>clinical research fellow</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">A</namePart><namePart type="family">Reiner</namePart><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation><description>project manager</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">T</namePart><namePart type="family">John</namePart><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation><description>clinical team lead</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">S</namePart><namePart type="family">Wilkins</namePart><affiliation>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</affiliation><description>research nurse</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">M</namePart><namePart type="family">Casey</namePart><affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</affiliation><description>children’s senior research sister</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">P E</namePart><namePart type="family">Eccleston</namePart><affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</affiliation><description>data manager</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">R J</namePart><namePart type="family">Allen</namePart><affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</affiliation><description>research network manager</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">I</namePart><namePart type="family">Okike</namePart><affiliation>St George’s Vaccine Institute, London SW17 0QT</affiliation><description>clinical research fellow</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">S</namePart><namePart type="family">Ladhani</namePart><affiliation>St George’s Vaccine Institute, London SW17 0QT</affiliation><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation><description>consultant in paediatric infectious diseases</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">E</namePart><namePart type="family">Sheasby</namePart><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation><description>quality manager</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">K</namePart><namePart type="family">Hoschler</namePart><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation><description>advanced healthcare scientist and clinical scientist</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">N</namePart><namePart type="family">Andrews</namePart><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation><description>senior statistician</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">P</namePart><namePart type="family">Waight</namePart><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation><description>senior scientific data analyst</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">A C</namePart><namePart type="family">Collinson</namePart><affiliation>Royal Devon and Exeter NHS Foundation Trust, Exeter EX2 5DW</affiliation><description>consultant paediatrician, co-director of Medicines for Children Research Network, south west</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">P T</namePart><namePart type="family">Heath</namePart><affiliation>St George’s Vaccine Institute, London SW17 0QT</affiliation><description>reader, honorary consultant in paediatric infectious diseases, executive officer paediatric studies</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">A</namePart><namePart type="family">Finn</namePart><affiliation>Bristol Children’s Vaccine Centre, University Hospitals Bristol NHS Foundation Trust and University of Bristol, Bristol BS2 8AE</affiliation><description>David Baum professor of paediatrics, director of Medicines for Children Research Network, south west</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">S N</namePart><namePart type="family">Faust</namePart><affiliation>University of Southampton Wellcome Trust Clinical Research Facility and Division of Infection, Inflammation and Immunity, Southampton SO16 6YD</affiliation><description>senior lecturer in paediatric immunology and infectious diseases, director Wellcome Trust clinical research facility</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">M D</namePart><namePart type="family">Snape</namePart><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation><description>consultant paediatrician and vaccinologist</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">E</namePart><namePart type="family">Miller</namePart><affiliation>Centre for Infections, Health Protection Agency, London NW9 5EQ</affiliation><description>professor, consultant epidemiologist</description><role><roleTerm type="text">author</roleTerm></role></name><name type="personal"><namePart type="given">A J</namePart><namePart type="family">Pollard</namePart><affiliation>Oxford Vaccine Group, Department of Paediatrics, University of Oxford, Oxford OX3 7LJ</affiliation><description>professor of paediatric infection and immunity, director of the Oxford Vaccine Group, honorary consultant paediatrician</description><role><roleTerm type="text">author</roleTerm></role></name><typeOfResource>text</typeOfResource><genre type="research-article" displayLabel="research-article" authority="ISTEX" authorityURI="https://content-type.data.istex.fr" valueURI="https://content-type.data.istex.fr/ark:/67375/XTP-1JC4F85T-7">research-article</genre><originInfo><publisher>British Medical Journal Publishing Group</publisher><dateIssued encoding="w3cdtf">2010</dateIssued><dateCreated encoding="w3cdtf">2010-05-27</dateCreated><copyrightDate encoding="w3cdtf">2010</copyrightDate></originInfo><language><languageTerm type="code" authority="iso639-2b">eng</languageTerm><languageTerm type="code" authority="rfc3066">en</languageTerm></language><abstract>Objectives To compare the safety, reactogenicity, and immunogenicity of an adjuvanted split virion H1N1 vaccine and a non-adjuvanted whole virion vaccine used in the pandemic immunisation programme in the United Kingdom. Design Open label, randomised, parallel group, phase II study. Setting Five UK centres (Oxford, Southampton, Bristol, Exeter, and London). Participants Children aged 6 months to less than 13 years for whom a parent or guardian had provided written informed consent and who were able to comply with study procedures were eligible. Those with laboratory confirmed pandemic H1N1 influenza or clinically diagnosed disease meriting antiviral treatment, allergy to egg or any other vaccine components, or coagulation defects, or who were severely immunocompromised or had recently received blood products were excluded. Children were grouped by age: 6 months-<3 years (younger group) and 3-<13 years (older group). Recruitment was by media advertising and direct mailing. Recruitment visits were attended by 949 participants, of whom 943 were enrolled and 937 included in the per protocol analysis. Interventions Participants were randomised 1:1 to receive AS03B (tocopherol based oil in water emulsion) adjuvanted split virion vaccine derived from egg culture or non-adjuvanted whole virion vaccine derived from cell culture. Both were given as two doses 21 days apart. Reactogenicity data were collected for one week after immunisation by diary card. Serum samples were collected at baseline and after the second dose. Main outcome measures Primary reactogenicity end points were frequency and severity of fever, tenderness, swelling, and erythema after vaccination. Immunogenicity was measured by microneutralisation and haemagglutination inhibition assays. The primary immunogenicity objective was a comparison between vaccines of the percentage of participants showing seroconversion by the microneutralisation assay (fourfold rise to a titre of ≥1:40 from before vaccination to three weeks after the second dose). Results Seroconversion rates were higher after the adjuvanted split virion vaccine than after the whole virion vaccine, most notably in the youngest children (163 of 166 participants with paired serum samples (98.2%, 95% confidence interval 94.8% to 99.6%) v 157 of 196 (80.1%, 73.8% to 85.5%), P<0.001) in children under 3 years and 226 of 228 (99.1%, 96.9% to 99.9%) v 95.9%, 92.4% to 98.1%, P=0.03) in those over 3 years). The adjuvanted split virion vaccine was more reactogenic than the whole virion vaccine, with more frequent systemic reactions and severe local reactions in children aged over 5 years after dose one (13 (7.2%, 3.9% to 12%) v 2 (1.1%, 0.1% to 3.9%), P<0.001) and dose two (15 (8.5%, 4.8% to 13.7%) v 2 (1.1%, 0.1% to 4.1%), P<0.002) and after dose two in those under 5 years (15 (5.9%, 3.3% to 9.6%) v 0 (0.0%, 0% to 1.4%), P<0.001). Dose two of the adjuvanted split virion vaccine was more reactogenic than dose one, especially for fever ≥38ºC in those aged under 5 (24 (8.9%, 5.8% to 12.9%) v 57 (22.4%, 17.5% to 28.1%), P<0.001). Conclusions In this first direct comparison of an AS03B adjuvanted split virion versus whole virion non-adjuvanted H1N1 vaccine, the adjuvanted vaccine, while more reactogenic, was more immunogenic and, importantly, achieved high seroconversion rates in children aged less than 3 years. This indicates the potential for improved immunogenicity of influenza vaccines in this age group. Trial registration Clinical trials.gov NCT00980850; ISRCTN89141709.</abstract><relatedItem type="host"><titleInfo><title>BMJ</title></titleInfo><titleInfo type="abbreviated"><title>BMJ</title></titleInfo><genre type="journal" authority="ISTEX" authorityURI="https://publication-type.data.istex.fr" valueURI="https://publication-type.data.istex.fr/ark:/67375/JMC-0GLKJH51-B">journal</genre><subject><genre>hwp-journal-coll</genre><topic>Infectious diseases</topic></subject><subject><genre>hwp-journal-coll</genre><topic>Immunology (including allergy)</topic></subject><subject><genre>hwp-journal-coll</genre><topic>Child health</topic></subject><subject><genre>hwp-journal-coll</genre><topic>Dermatology</topic></subject><subject><genre>hwp-journal-coll</genre><topic>Informed consent</topic></subject><subject><genre>hwp-journal-coll</genre><topic>Legal and forensic medicine</topic></subject><identifier type="ISSN">0959-8138</identifier><identifier type="eISSN">1468-5833</identifier><identifier type="PublisherID">bmj</identifier><identifier type="PublisherID-hwp">bmj</identifier><identifier type="PublisherID-nlm-ta">BMJ</identifier><part><date>2010</date><detail type="volume"><caption>vol.</caption><number>340</number></detail></part></relatedItem><identifier type="istex">DA78FD80666CE56A8542B3559E5D4F78DD0533E0</identifier><identifier type="ark">ark:/67375/NVC-MTZB16DP-T</identifier><identifier type="DOI">10.1136/bmj.c2649</identifier><identifier type="href">bmj-340-bmj-c2649.pdf</identifier><identifier type="ArticleID">wadc777714</identifier><identifier type="PMID">20508026</identifier><identifier type="local">bmj;340/may27_1/c2649</identifier><accessCondition type="use and reproduction" contentType="open-access">This is an open-access article distributed under the terms of the Creative Commons Attribution Non-commercial License, which permits use, distribution, and reproduction in any medium, provided the original work is properly cited, the use is non commercial and is otherwise in compliance with the license. See: http://creativecommons.org/licenses/by-nc/2.0/ and http://creativecommons.org/licenses/by-nc/2.0/legalcode.</accessCondition><recordInfo><recordContentSource authority="ISTEX" authorityURI="https://loaded-corpus.data.istex.fr" valueURI="https://loaded-corpus.data.istex.fr/ark:/67375/XBH-7M42M2QJ-2">bmj</recordContentSource><recordOrigin>© Waddington et al 2010</recordOrigin></recordInfo></mods><json:item><extension>json</extension><original>false</original><mimetype>application/json</mimetype><uri>https://api.istex.fr/ark:/67375/NVC-MTZB16DP-T/record.json</uri></json:item></metadata><annexes><json:item><extension>jpeg</extension><original>true</original><mimetype>image/jpeg</mimetype><uri>https://api.istex.fr/ark:/67375/NVC-MTZB16DP-T/annexes.jpeg</uri></json:item></annexes><serie></serie></istex></record>Pour manipuler ce document sous Unix (Dilib)
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