Effectiveness of the RTS,S/AS01E malaria vaccine in a real-world setting over 1 year of follow-up after the three-dose primary schedule

RTS,S Epidemiology EPI-MAL-003 Study Group; Latif Ndeketa; Valérie Haine; Muriel Debois; Kwaku Poku Asante; Prince Darko Agyapong; Seyram Kaali; Raghavendra Devadiga; Samuel B.E. Harrison; Owusu Boahen; Neil French; Kingsley Kayan; Bernhards Ogutu; Elisha Adeniji; Simon Kariuki; Seth Owusu-Agyei; Fredrick Olewe; Tikhala Makhaza Jere; Kenneth Maleta; Donnie Mategula; Phylis Mzanga; Vincent Katunga Phiri; Patrick Odum Ansah; John Orimbo; Nana Akosua Ansah; Mattea Orsini; John Michael Ong'echa; Abraham Rexford Oduro; Peter M. Sifuna; Daniel K. Azongo; Walter Otieno; Oscar Bangre; Michael Bandasua Kaburise; Lucy Osei Ababio; Janet Nyawira Oyieko; Valentine Sing'oei; Stellah Kevyne Amoit; Wongani Nyangulu; Lode Schuerman; Denis Awuni; Benard Omondi Ochieng; Irene Onyango; Patricia Odera-Ojwang; Esther Achieng Oguk; Yolanda Guerra Mendoza; Reuben Yego Cherop; George Odhiambo Okoth; Cristina Cravcenco; Raphael Chipatala; François Roman; Martina Oneko

doi:10.1016/S2214-109X(25)00415-2

Effectiveness of the RTS,S/AS01_E malaria vaccine in a real-world setting over 1 year of follow-up after the three-dose primary schedule

RTS,S Epidemiology EPI-MAL-003 Study Group
, Latif Ndeketa
, Valérie Haine
, Muriel Debois
, Kwaku Poku Asante
, Prince Darko Agyapong
, Seyram Kaali
, Raghavendra Devadiga
, Samuel B.E. Harrison
, Owusu Boahen
, Neil French
, Kingsley Kayan
, Bernhards Ogutu
, Elisha Adeniji
, Simon Kariuki
, Seth Owusu-Agyei
, Fredrick Olewe
, Tikhala Makhaza Jere
, Kenneth Maleta
, Donnie Mategula

Phylis Mzanga, Vincent Katunga Phiri, Patrick Odum Ansah, John Orimbo, Nana Akosua Ansah, Mattea Orsini, John Michael Ong'echa, Abraham Rexford Oduro, Peter M. Sifuna, Daniel K. Azongo, Walter Otieno, Oscar Bangre, Michael Bandasua Kaburise, Lucy Osei Ababio, Janet Nyawira Oyieko, Valentine Sing'oei, Stellah Kevyne Amoit, Wongani Nyangulu, Lode Schuerman, Denis Awuni, Benard Omondi Ochieng, Irene Onyango, Patricia Odera-Ojwang, Esther Achieng Oguk, Yolanda Guerra Mendoza, Reuben Yego Cherop, George Odhiambo Okoth, Cristina Cravcenco, Raphael Chipatala, François Roman, Martina Oneko

Research output: Contribution to journal › Article › peer-review

Abstract

BACKGROUND: RTS,S/AS01E was first introduced within the Malaria Vaccine Implementation Programme in selected areas in Ghana, Kenya, and Malawi. A series of post-introduction observational studies were initiated in these areas to assess RTS,S/AS01E safety and effectiveness in real-world settings. Here, we report the results of the interim analysis of the EPI-MAL-003 study secondary objectives related to vaccine effectiveness.

METHODS: EPI-MAL-003 was a phase 4, disease surveillance study with prospective cohort event monitoring. The study was performed in routine medical practice settings at 12 sites (four per country) in Ghana, Kenya, and Malawi. Children younger than 18 months were enrolled in exposed clusters (sites where RTS,S/AS01E was introduced) and unexposed clusters; data were collected via active surveillance. In an interim analysis, we estimated the effect of vaccination on the incidence of malaria, all-cause hospitalisations, and malaria-related hospitalisations, the prevalence of anaemia among hospitalised children, and mortality over 1 year of follow-up after primary vaccination with three RTS,S/AS01E doses. These endpoints were analysed in the effectiveness analysis set. The primary endpoints are reported elsewhere, together with secondary safety endpoints. This study is registered with ClinicalTrials.gov, NCT03855995, and is completed.

FINDINGS: The first child was enrolled on March 21, 2019, and the cutoff date for the current analysis was Nov 2, 2023. 45 000 children were enrolled (22 426 [49·8%] were female and 22 574 [50·25%] were male). 39 463 children were included in the analyses. When comparing vaccinated children from exposed clusters with unvaccinated children from unexposed clusters, country-adjusted incidence rate ratios were 0·70 (95% CI 0·67-0·73; p<0·001) for any malaria, 0·42 (0·30-0·60; p<0·001) for severe malaria, 0·64 (0·56-0·72; p<0·001) for malaria-related hospitalisations, 0·79 (0·74-0·84; p<0·001) for all-cause hospitalisations, and 0·83 (0·64-1·09; p=0·18) for all-cause mortality. The adjusted odds ratio for the prevalence of anaemia among children who were hospitalised (vaccinated children from exposed clusters vs unvaccinated children from unexposed clusters) was 0·81 (95% CI 0·73-0·90; p<0·001). Similar trends were observed in a before-after comparison with unvaccinated children enrolled in the EPI-MAL-002 study conducted before the RTS,S/AS01E introduction.

INTERPRETATION: Over 1 year of follow-up after the third vaccine dose, vaccination with RTS,S/AS01E in real-world settings showed significant reductions in malaria burden. These findings reinforce the continued use of RTS,S/AS01E vaccination in children as an effective public health measure to reduce malaria-related illness and mortality in endemic regions, and highlight its relevance for future malaria control strategies.GSK.

Original language	English
Pages (from-to)	e61-e69
Journal	The Lancet. Global health
Volume	14
Issue number	1
Early online date	6 Nov 2025
DOIs	https://doi.org/10.1016/S2214-109X(25)00415-2
Publication status	E-pub ahead of print - 6 Nov 2025
Externally published	Yes

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Cite this

RTS,S Epidemiology EPI-MAL-003 Study Group, Ndeketa, L., Haine, V., Debois, M., Asante, K. P., Agyapong, P. D., Kaali, S., Devadiga, R., Harrison, S. B. E., Boahen, O., French, N., Kayan, K., Ogutu, B., Adeniji, E., Kariuki, S., Owusu-Agyei, S., Olewe, F., Jere, T. M., Maleta, K., ... Oneko, M. (2025). Effectiveness of the RTS,S/AS01_E malaria vaccine in a real-world setting over 1 year of follow-up after the three-dose primary schedule. The Lancet. Global health, 14(1), e61-e69. Advance online publication. https://doi.org/10.1016/S2214-109X(25)00415-2

@article{f62bf895fb7241b491250598c48419ab,

title = "Effectiveness of the RTS,S/AS01E malaria vaccine in a real-world setting over 1 year of follow-up after the three-dose primary schedule",

abstract = "BACKGROUND: RTS,S/AS01E was first introduced within the Malaria Vaccine Implementation Programme in selected areas in Ghana, Kenya, and Malawi. A series of post-introduction observational studies were initiated in these areas to assess RTS,S/AS01E safety and effectiveness in real-world settings. Here, we report the results of the interim analysis of the EPI-MAL-003 study secondary objectives related to vaccine effectiveness. METHODS: EPI-MAL-003 was a phase 4, disease surveillance study with prospective cohort event monitoring. The study was performed in routine medical practice settings at 12 sites (four per country) in Ghana, Kenya, and Malawi. Children younger than 18 months were enrolled in exposed clusters (sites where RTS,S/AS01E was introduced) and unexposed clusters; data were collected via active surveillance. In an interim analysis, we estimated the effect of vaccination on the incidence of malaria, all-cause hospitalisations, and malaria-related hospitalisations, the prevalence of anaemia among hospitalised children, and mortality over 1 year of follow-up after primary vaccination with three RTS,S/AS01E doses. These endpoints were analysed in the effectiveness analysis set. The primary endpoints are reported elsewhere, together with secondary safety endpoints. This study is registered with ClinicalTrials.gov, NCT03855995, and is completed. FINDINGS: The first child was enrolled on March 21, 2019, and the cutoff date for the current analysis was Nov 2, 2023. 45 000 children were enrolled (22 426 [49·8\%] were female and 22 574 [50·25\%] were male). 39 463 children were included in the analyses. When comparing vaccinated children from exposed clusters with unvaccinated children from unexposed clusters, country-adjusted incidence rate ratios were 0·70 (95\% CI 0·67-0·73; p<0·001) for any malaria, 0·42 (0·30-0·60; p<0·001) for severe malaria, 0·64 (0·56-0·72; p<0·001) for malaria-related hospitalisations, 0·79 (0·74-0·84; p<0·001) for all-cause hospitalisations, and 0·83 (0·64-1·09; p=0·18) for all-cause mortality. The adjusted odds ratio for the prevalence of anaemia among children who were hospitalised (vaccinated children from exposed clusters vs unvaccinated children from unexposed clusters) was 0·81 (95\% CI 0·73-0·90; p<0·001). Similar trends were observed in a before-after comparison with unvaccinated children enrolled in the EPI-MAL-002 study conducted before the RTS,S/AS01E introduction. INTERPRETATION: Over 1 year of follow-up after the third vaccine dose, vaccination with RTS,S/AS01E in real-world settings showed significant reductions in malaria burden. These findings reinforce the continued use of RTS,S/AS01E vaccination in children as an effective public health measure to reduce malaria-related illness and mortality in endemic regions, and highlight its relevance for future malaria control strategies.GSK.",

author = "\{RTS,S Epidemiology EPI-MAL-003 Study Group\} and Latif Ndeketa and Val{\'e}rie Haine and Muriel Debois and Asante, \{Kwaku Poku\} and Agyapong, \{Prince Darko\} and Seyram Kaali and Raghavendra Devadiga and Harrison, \{Samuel B.E.\} and Owusu Boahen and Neil French and Kingsley Kayan and Bernhards Ogutu and Elisha Adeniji and Simon Kariuki and Seth Owusu-Agyei and Fredrick Olewe and Jere, \{Tikhala Makhaza\} and Kenneth Maleta and Donnie Mategula and Phylis Mzanga and Phiri, \{Vincent Katunga\} and Ansah, \{Patrick Odum\} and John Orimbo and Ansah, \{Nana Akosua\} and Mattea Orsini and Ong'echa, \{John Michael\} and Oduro, \{Abraham Rexford\} and Sifuna, \{Peter M.\} and Azongo, \{Daniel K.\} and Walter Otieno and Oscar Bangre and Kaburise, \{Michael Bandasua\} and Ababio, \{Lucy Osei\} and Oyieko, \{Janet Nyawira\} and Valentine Sing'oei and Amoit, \{Stellah Kevyne\} and Wongani Nyangulu and Lode Schuerman and Denis Awuni and Ochieng, \{Benard Omondi\} and Irene Onyango and Patricia Odera-Ojwang and Oguk, \{Esther Achieng\} and Mendoza, \{Yolanda Guerra\} and Cherop, \{Reuben Yego\} and Okoth, \{George Odhiambo\} and Cristina Cravcenco and Raphael Chipatala and Fran{\c c}ois Roman and Martina Oneko",

note = "Publisher Copyright: Copyright {\textcopyright} 2025 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Published by Elsevier Ltd.. All rights reserved.",

year = "2025",

month = nov,

day = "6",

doi = "10.1016/S2214-109X(25)00415-2",

language = "English",

volume = "14",

pages = "e61--e69",

journal = "The Lancet. Global health",

issn = "2572-116X",

publisher = "Elsevier Ltd",

number = "1",

}

RTS,S Epidemiology EPI-MAL-003 Study Group, Ndeketa, L, Haine, V, Debois, M, Asante, KP, Agyapong, PD, Kaali, S, Devadiga, R, Harrison, SBE, Boahen, O, French, N, Kayan, K, Ogutu, B, Adeniji, E, Kariuki, S, Owusu-Agyei, S, Olewe, F, Jere, TM, Maleta, K, Mategula, D, Mzanga, P, Phiri, VK, Ansah, PO, Orimbo, J, Ansah, NA, Orsini, M, Ong'echa, JM, Oduro, AR, Sifuna, PM, Azongo, DK, Otieno, W, Bangre, O, Kaburise, MB, Ababio, LO, Oyieko, JN, Sing'oei, V, Amoit, SK, Nyangulu, W, Schuerman, L, Awuni, D, Ochieng, BO, Onyango, I, Odera-Ojwang, P, Oguk, EA, Mendoza, YG, Cherop, RY, Okoth, GO, Cravcenco, C, Chipatala, R, Roman, F & Oneko, M 2025, 'Effectiveness of the RTS,S/AS01_E malaria vaccine in a real-world setting over 1 year of follow-up after the three-dose primary schedule', The Lancet. Global health, vol. 14, no. 1, pp. e61-e69. https://doi.org/10.1016/S2214-109X(25)00415-2

TY - JOUR

T1 - Effectiveness of the RTS,S/AS01E malaria vaccine in a real-world setting over 1 year of follow-up after the three-dose primary schedule

AU - RTS,S Epidemiology EPI-MAL-003 Study Group

AU - Ndeketa, Latif

AU - Haine, Valérie

AU - Debois, Muriel

AU - Asante, Kwaku Poku

AU - Agyapong, Prince Darko

AU - Kaali, Seyram

AU - Devadiga, Raghavendra

AU - Harrison, Samuel B.E.

AU - Boahen, Owusu

AU - French, Neil

AU - Kayan, Kingsley

AU - Ogutu, Bernhards

AU - Adeniji, Elisha

AU - Kariuki, Simon

AU - Owusu-Agyei, Seth

AU - Olewe, Fredrick

AU - Jere, Tikhala Makhaza

AU - Maleta, Kenneth

AU - Mategula, Donnie

AU - Mzanga, Phylis

AU - Phiri, Vincent Katunga

AU - Ansah, Patrick Odum

AU - Orimbo, John

AU - Ansah, Nana Akosua

AU - Orsini, Mattea

AU - Ong'echa, John Michael

AU - Oduro, Abraham Rexford

AU - Sifuna, Peter M.

AU - Azongo, Daniel K.

AU - Otieno, Walter

AU - Bangre, Oscar

AU - Kaburise, Michael Bandasua

AU - Ababio, Lucy Osei

AU - Oyieko, Janet Nyawira

AU - Sing'oei, Valentine

AU - Amoit, Stellah Kevyne

AU - Nyangulu, Wongani

AU - Schuerman, Lode

AU - Awuni, Denis

AU - Ochieng, Benard Omondi

AU - Onyango, Irene

AU - Odera-Ojwang, Patricia

AU - Oguk, Esther Achieng

AU - Mendoza, Yolanda Guerra

AU - Cherop, Reuben Yego

AU - Okoth, George Odhiambo

AU - Cravcenco, Cristina

AU - Chipatala, Raphael

AU - Roman, François

AU - Oneko, Martina

PY - 2025/11/6

Y1 - 2025/11/6

N2 - BACKGROUND: RTS,S/AS01E was first introduced within the Malaria Vaccine Implementation Programme in selected areas in Ghana, Kenya, and Malawi. A series of post-introduction observational studies were initiated in these areas to assess RTS,S/AS01E safety and effectiveness in real-world settings. Here, we report the results of the interim analysis of the EPI-MAL-003 study secondary objectives related to vaccine effectiveness. METHODS: EPI-MAL-003 was a phase 4, disease surveillance study with prospective cohort event monitoring. The study was performed in routine medical practice settings at 12 sites (four per country) in Ghana, Kenya, and Malawi. Children younger than 18 months were enrolled in exposed clusters (sites where RTS,S/AS01E was introduced) and unexposed clusters; data were collected via active surveillance. In an interim analysis, we estimated the effect of vaccination on the incidence of malaria, all-cause hospitalisations, and malaria-related hospitalisations, the prevalence of anaemia among hospitalised children, and mortality over 1 year of follow-up after primary vaccination with three RTS,S/AS01E doses. These endpoints were analysed in the effectiveness analysis set. The primary endpoints are reported elsewhere, together with secondary safety endpoints. This study is registered with ClinicalTrials.gov, NCT03855995, and is completed. FINDINGS: The first child was enrolled on March 21, 2019, and the cutoff date for the current analysis was Nov 2, 2023. 45 000 children were enrolled (22 426 [49·8%] were female and 22 574 [50·25%] were male). 39 463 children were included in the analyses. When comparing vaccinated children from exposed clusters with unvaccinated children from unexposed clusters, country-adjusted incidence rate ratios were 0·70 (95% CI 0·67-0·73; p<0·001) for any malaria, 0·42 (0·30-0·60; p<0·001) for severe malaria, 0·64 (0·56-0·72; p<0·001) for malaria-related hospitalisations, 0·79 (0·74-0·84; p<0·001) for all-cause hospitalisations, and 0·83 (0·64-1·09; p=0·18) for all-cause mortality. The adjusted odds ratio for the prevalence of anaemia among children who were hospitalised (vaccinated children from exposed clusters vs unvaccinated children from unexposed clusters) was 0·81 (95% CI 0·73-0·90; p<0·001). Similar trends were observed in a before-after comparison with unvaccinated children enrolled in the EPI-MAL-002 study conducted before the RTS,S/AS01E introduction. INTERPRETATION: Over 1 year of follow-up after the third vaccine dose, vaccination with RTS,S/AS01E in real-world settings showed significant reductions in malaria burden. These findings reinforce the continued use of RTS,S/AS01E vaccination in children as an effective public health measure to reduce malaria-related illness and mortality in endemic regions, and highlight its relevance for future malaria control strategies.GSK.

AB - BACKGROUND: RTS,S/AS01E was first introduced within the Malaria Vaccine Implementation Programme in selected areas in Ghana, Kenya, and Malawi. A series of post-introduction observational studies were initiated in these areas to assess RTS,S/AS01E safety and effectiveness in real-world settings. Here, we report the results of the interim analysis of the EPI-MAL-003 study secondary objectives related to vaccine effectiveness. METHODS: EPI-MAL-003 was a phase 4, disease surveillance study with prospective cohort event monitoring. The study was performed in routine medical practice settings at 12 sites (four per country) in Ghana, Kenya, and Malawi. Children younger than 18 months were enrolled in exposed clusters (sites where RTS,S/AS01E was introduced) and unexposed clusters; data were collected via active surveillance. In an interim analysis, we estimated the effect of vaccination on the incidence of malaria, all-cause hospitalisations, and malaria-related hospitalisations, the prevalence of anaemia among hospitalised children, and mortality over 1 year of follow-up after primary vaccination with three RTS,S/AS01E doses. These endpoints were analysed in the effectiveness analysis set. The primary endpoints are reported elsewhere, together with secondary safety endpoints. This study is registered with ClinicalTrials.gov, NCT03855995, and is completed. FINDINGS: The first child was enrolled on March 21, 2019, and the cutoff date for the current analysis was Nov 2, 2023. 45 000 children were enrolled (22 426 [49·8%] were female and 22 574 [50·25%] were male). 39 463 children were included in the analyses. When comparing vaccinated children from exposed clusters with unvaccinated children from unexposed clusters, country-adjusted incidence rate ratios were 0·70 (95% CI 0·67-0·73; p<0·001) for any malaria, 0·42 (0·30-0·60; p<0·001) for severe malaria, 0·64 (0·56-0·72; p<0·001) for malaria-related hospitalisations, 0·79 (0·74-0·84; p<0·001) for all-cause hospitalisations, and 0·83 (0·64-1·09; p=0·18) for all-cause mortality. The adjusted odds ratio for the prevalence of anaemia among children who were hospitalised (vaccinated children from exposed clusters vs unvaccinated children from unexposed clusters) was 0·81 (95% CI 0·73-0·90; p<0·001). Similar trends were observed in a before-after comparison with unvaccinated children enrolled in the EPI-MAL-002 study conducted before the RTS,S/AS01E introduction. INTERPRETATION: Over 1 year of follow-up after the third vaccine dose, vaccination with RTS,S/AS01E in real-world settings showed significant reductions in malaria burden. These findings reinforce the continued use of RTS,S/AS01E vaccination in children as an effective public health measure to reduce malaria-related illness and mortality in endemic regions, and highlight its relevance for future malaria control strategies.GSK.

U2 - 10.1016/S2214-109X(25)00415-2

DO - 10.1016/S2214-109X(25)00415-2

M3 - Article

C2 - 41207319

AN - SCOPUS:105024877089

SN - 2572-116X

VL - 14

SP - e61-e69

JO - The Lancet. Global health

JF - The Lancet. Global health

IS - 1

ER -