Evaluation of two formulations of adjuvanted RTS, S malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of Mozambique: a Phase I/IIb randomized double-blind bridging trial

BACKGROUND: Previous trials of the RTS, S malaria candidate vaccine have shown that this vaccine is safe, tolerated and immunogenic. The development plan for this vaccine aims at administering it in the first year of life through the Expanded Program on Immunization (EPI). The objective was to evalu...

Descripción completa

Detalles Bibliográficos
Autores principales: Macete, Eusebio V, Sacarlal, Jahit, Aponte, John J, Leach, Amanda, Navia, Margarita M, Milman, Jessica, Guinovart, Caterina, Mandomando, Inacio, López-Púa, Yolanda, Lievens, Marc, Owusu-Ofori, Alex, Dubois, Marie-Claude, Cahill, Conor P, Koutsoukos, Marguerite, Sillman, Marla, Thompson, Ricardo, Dubovsky, Filip, Ballou, W Ripley, Cohen, Joe, Alonso, Pedro L
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2007
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1847838/
https://www.ncbi.nlm.nih.gov/pubmed/17386091
http://dx.doi.org/10.1186/1745-6215-8-11
_version_ 1782132926745411584
author Macete, Eusebio V
Sacarlal, Jahit
Aponte, John J
Leach, Amanda
Navia, Margarita M
Milman, Jessica
Guinovart, Caterina
Mandomando, Inacio
López-Púa, Yolanda
Lievens, Marc
Owusu-Ofori, Alex
Dubois, Marie-Claude
Cahill, Conor P
Koutsoukos, Marguerite
Sillman, Marla
Thompson, Ricardo
Dubovsky, Filip
Ballou, W Ripley
Cohen, Joe
Alonso, Pedro L
author_facet Macete, Eusebio V
Sacarlal, Jahit
Aponte, John J
Leach, Amanda
Navia, Margarita M
Milman, Jessica
Guinovart, Caterina
Mandomando, Inacio
López-Púa, Yolanda
Lievens, Marc
Owusu-Ofori, Alex
Dubois, Marie-Claude
Cahill, Conor P
Koutsoukos, Marguerite
Sillman, Marla
Thompson, Ricardo
Dubovsky, Filip
Ballou, W Ripley
Cohen, Joe
Alonso, Pedro L
author_sort Macete, Eusebio V
collection PubMed
description BACKGROUND: Previous trials of the RTS, S malaria candidate vaccine have shown that this vaccine is safe, tolerated and immunogenic. The development plan for this vaccine aims at administering it in the first year of life through the Expanded Program on Immunization (EPI). The objective was to evaluate the safety and reactogenicity of RTS, S/AS02D (0.5 ml dose), a pediatric formulation of GlaxoSmithKline Biologicals' current malaria candidate vaccine RTS, S/AS02A (0.25 ml dose). A 0.5 ml dose of AS02D is composed of the same active ingredients in the same quantities as in a 0.25 ml dose of AS02A and has been developed to be easily introduced into routine EPI practices. METHODS: We performed a phase I/IIb randomized double-blind bridging study in a malaria-endemic region of Mozambique, to compare the safety and immunogenicity of both candidate vaccines with the aim of replacing RTS, S/AS02A with RTS, S/AS02D as the candidate pediatric vaccine. 200 Mozambican children aged 3 to 5 years were randomized 1:1 to receive one of the 2 vaccines according to a 0, 1, 2 month schedule. RESULTS: Both vaccines were safe and had similar reactogenicity profiles. All subjects with paired pre and post-vaccination samples showed a vaccine response with respect to anti-circumsporozoite (CS) antibodies irrespective of initial anti-CS serostatus. Geometric mean titers (GMTs) were 191 EU/ml (95% CI 150–242) in recipients of RTS, S/AS02D compared to 180 EU/ml (95% CI 146–221) in recipients of RTS, S/AS02A. For the anti-hepatitis B surface antigen (HBsAg), all subjects were seroprotected at day 90, and the GMTs were 23978 mIU/ml (95% CI 17896–32127) in RTS, S/AS02D recipients and 17410 mIU/ml (95% CI 13322–22752) in RTS, S/AS02A recipients. There was a decrease in anti-CS GMTs between months 3 and 14 in both groups (191 vs 22 EU/mL in RTS, S/AS02D group and 180 vs 29 EU/mL in RTS, S/AS02A group). CONCLUSION: Our data show that the RTS, S/AS02D is safe, well tolerated, and demonstrates non-inferiority (defined as upper limit of the 95% confidence interval of the anti-CS GMT ratio of RTS, S/AS02A to RTS, S/AS02D below 3.0) of the antibody responses to circumsporozoite and HBsAg induced by the RTS, S/AS02D as compared to the RTS, S/AS02A.
format Text
id pubmed-1847838
institution National Center for Biotechnology Information
language English
publishDate 2007
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-18478382007-04-06 Evaluation of two formulations of adjuvanted RTS, S malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of Mozambique: a Phase I/IIb randomized double-blind bridging trial Macete, Eusebio V Sacarlal, Jahit Aponte, John J Leach, Amanda Navia, Margarita M Milman, Jessica Guinovart, Caterina Mandomando, Inacio López-Púa, Yolanda Lievens, Marc Owusu-Ofori, Alex Dubois, Marie-Claude Cahill, Conor P Koutsoukos, Marguerite Sillman, Marla Thompson, Ricardo Dubovsky, Filip Ballou, W Ripley Cohen, Joe Alonso, Pedro L Trials Research BACKGROUND: Previous trials of the RTS, S malaria candidate vaccine have shown that this vaccine is safe, tolerated and immunogenic. The development plan for this vaccine aims at administering it in the first year of life through the Expanded Program on Immunization (EPI). The objective was to evaluate the safety and reactogenicity of RTS, S/AS02D (0.5 ml dose), a pediatric formulation of GlaxoSmithKline Biologicals' current malaria candidate vaccine RTS, S/AS02A (0.25 ml dose). A 0.5 ml dose of AS02D is composed of the same active ingredients in the same quantities as in a 0.25 ml dose of AS02A and has been developed to be easily introduced into routine EPI practices. METHODS: We performed a phase I/IIb randomized double-blind bridging study in a malaria-endemic region of Mozambique, to compare the safety and immunogenicity of both candidate vaccines with the aim of replacing RTS, S/AS02A with RTS, S/AS02D as the candidate pediatric vaccine. 200 Mozambican children aged 3 to 5 years were randomized 1:1 to receive one of the 2 vaccines according to a 0, 1, 2 month schedule. RESULTS: Both vaccines were safe and had similar reactogenicity profiles. All subjects with paired pre and post-vaccination samples showed a vaccine response with respect to anti-circumsporozoite (CS) antibodies irrespective of initial anti-CS serostatus. Geometric mean titers (GMTs) were 191 EU/ml (95% CI 150–242) in recipients of RTS, S/AS02D compared to 180 EU/ml (95% CI 146–221) in recipients of RTS, S/AS02A. For the anti-hepatitis B surface antigen (HBsAg), all subjects were seroprotected at day 90, and the GMTs were 23978 mIU/ml (95% CI 17896–32127) in RTS, S/AS02D recipients and 17410 mIU/ml (95% CI 13322–22752) in RTS, S/AS02A recipients. There was a decrease in anti-CS GMTs between months 3 and 14 in both groups (191 vs 22 EU/mL in RTS, S/AS02D group and 180 vs 29 EU/mL in RTS, S/AS02A group). CONCLUSION: Our data show that the RTS, S/AS02D is safe, well tolerated, and demonstrates non-inferiority (defined as upper limit of the 95% confidence interval of the anti-CS GMT ratio of RTS, S/AS02A to RTS, S/AS02D below 3.0) of the antibody responses to circumsporozoite and HBsAg induced by the RTS, S/AS02D as compared to the RTS, S/AS02A. BioMed Central 2007-03-26 /pmc/articles/PMC1847838/ /pubmed/17386091 http://dx.doi.org/10.1186/1745-6215-8-11 Text en Copyright © 2007 Macete et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Macete, Eusebio V
Sacarlal, Jahit
Aponte, John J
Leach, Amanda
Navia, Margarita M
Milman, Jessica
Guinovart, Caterina
Mandomando, Inacio
López-Púa, Yolanda
Lievens, Marc
Owusu-Ofori, Alex
Dubois, Marie-Claude
Cahill, Conor P
Koutsoukos, Marguerite
Sillman, Marla
Thompson, Ricardo
Dubovsky, Filip
Ballou, W Ripley
Cohen, Joe
Alonso, Pedro L
Evaluation of two formulations of adjuvanted RTS, S malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of Mozambique: a Phase I/IIb randomized double-blind bridging trial
title Evaluation of two formulations of adjuvanted RTS, S malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of Mozambique: a Phase I/IIb randomized double-blind bridging trial
title_full Evaluation of two formulations of adjuvanted RTS, S malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of Mozambique: a Phase I/IIb randomized double-blind bridging trial
title_fullStr Evaluation of two formulations of adjuvanted RTS, S malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of Mozambique: a Phase I/IIb randomized double-blind bridging trial
title_full_unstemmed Evaluation of two formulations of adjuvanted RTS, S malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of Mozambique: a Phase I/IIb randomized double-blind bridging trial
title_short Evaluation of two formulations of adjuvanted RTS, S malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of Mozambique: a Phase I/IIb randomized double-blind bridging trial
title_sort evaluation of two formulations of adjuvanted rts, s malaria vaccine in children aged 3 to 5 years living in a malaria-endemic region of mozambique: a phase i/iib randomized double-blind bridging trial
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1847838/
https://www.ncbi.nlm.nih.gov/pubmed/17386091
http://dx.doi.org/10.1186/1745-6215-8-11
work_keys_str_mv AT maceteeusebiov evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT sacarlaljahit evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT apontejohnj evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT leachamanda evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT naviamargaritam evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT milmanjessica evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT guinovartcaterina evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT mandomandoinacio evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT lopezpuayolanda evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT lievensmarc evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT owusuoforialex evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT duboismarieclaude evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT cahillconorp evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT koutsoukosmarguerite evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT sillmanmarla evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT thompsonricardo evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT dubovskyfilip evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT ballouwripley evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT cohenjoe evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial
AT alonsopedrol evaluationoftwoformulationsofadjuvantedrtssmalariavaccineinchildrenaged3to5yearslivinginamalariaendemicregionofmozambiqueaphaseiiibrandomizeddoubleblindbridgingtrial

Ejemplares similares