Safety and immunogenicity of inactivated poliovirus vaccine when given with measles–rubella combined vaccine and yellow fever vaccine and when given via different administration routes: a phase 4, randomised, non-inferiority trial in The Gambia
Autor: | Ed Clarke, Matthias Niedrig, Ralf Clemens, Panchali Roy Chowdhury, David Jeffries, Ananda S Bandyopadhyay, Michael Okoye, Mariama Badjie Hydara, Ama Umesi, Beate Kampmann, Kevin E. Brown, Ikechukwu Adigweme, Elishia Roberts, Pa Modou Cham, Jenny Mueller, Jane U. Adetifa, Adedapo O Bashorun, Ngozi Moneke-Anyanwoke, Yauba Saidu |
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Jazyk: | angličtina |
Rok vydání: | 2016 |
Předmět: |
Male
030231 tropical medicine Yellow fever vaccine medicine.disease_cause Rubella Measles Injections 03 medical and health sciences 0302 clinical medicine Blood serum Seroepidemiologic Studies medicine Humans 030212 general & internal medicine Vaccines Combined Seroconversion Immunization Schedule business.industry lcsh:Public aspects of medicine Poliovirus Vaccination Yellow Fever Vaccine Infant lcsh:RA1-1270 General Medicine medicine.disease Virology Poliovirus Vaccine Inactivated Inactivated Poliovirus Vaccine Female Gambia business medicine.drug Poliomyelitis |
Zdroj: | e547 e534 The Lancet Global Health, Vol 4, Iss 8, Pp e534-e547 (2016) |
ISSN: | 0184-7872 2214-109X |
Popis: | Summary Background The introduction of the inactivated poliovirus vaccine (IPV) represents a crucial step in the polio eradication endgame. This trial examined the safety and immunogenicity of IPV given alongside the measles–rubella and yellow fever vaccines at 9 months and when given as a full or fractional dose using needle and syringe or disposable-syringe jet injector. Methods We did a phase 4, randomised, non-inferiority trial at three periurban government clinics in west Gambia. Infants aged 9–10 months who had already received oral poliovirus vaccine were randomly assigned to receive the IPV, measles–rubella, and yellow fever vaccines, singularly or in combination. Separately, IPV was given as a full intramuscular or fractional intradermal dose by needle and syringe or disposable-syringe jet injector at a second visit. The primary outcomes were seroprevalence rates for poliovirus 4–6 weeks post-vaccination and the rate of seroconversion between baseline and post-vaccination serum samples for measles, rubella, and yellow fever; and the post-vaccination antibody titres generated against each component of the vaccines. We did a per-protocol analysis with a non-inferiority margin of 10% for poliovirus seroprevalence and measles, rubella, and yellow fever seroconversion, and (1/3) log 2 for log 2 -transformed antibody titres. This trial is registered with ClinicalTrials.gov, number NCT01847872. Findings Between July 10, 2013, and May 8, 2014, we assessed 1662 infants for eligibility, of whom 1504 were enrolled into one of seven groups for vaccine interference and one of four groups for fractional dosing and alternative route of administration. The rubella and yellow fever antibody titres were reduced by co-administration but the seroconversion rates achieved non-inferiority in both cases (rubella, −4·5% [95% CI −9·5 to −0·1]; yellow fever, 1·2% [–2·9 to 5·5]). Measles and poliovirus responses were unaffected (measles, 6·8% [95% CI −1·4 to 14·9]; poliovirus serotype 1, 1·6% [–6·7 to 4·7]; serotype 2, 0·0% [–2·1 to 2·1]; serotype 3, 0·0% [–3·8 to 3·9]). Poliovirus seroprevalence was universally high (>97%) after vaccination, but the antibody titres generated by fractional intradermal doses of IPV did not achieve non-inferiority compared with full dose. The number of infants who seroconverted or had a four-fold rise in titres was also lower by the intradermal route. There were no safety concerns. Interpretation The data support the future co-administration of IPV, measles–rubella, and yellow fever vaccines within the Expanded Programme on Immunization schedule at 9 months. The administration of single fractional intradermal doses of IPV by needle and syringe or disposable-syringe jet injector compromises the immunity generated, although it results in a high post-vaccination poliovirus seroprevalence. Funding Bill & Melinda Gates Foundation. |
Databáze: | OpenAIRE |
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