A Study Assessing the Safety, Efficacy, and Impact of GlaxoSmithKline Biologicals' RTS, S/AS01E Malaria Vaccine in Young Children Across Sub-Saharan Africa

Recruiting

• Conditions: Malaria; Malaria Vaccines
• Interventions: Procedure: Whole blood sample

• Registration Number: NCT03855995
• Lead Sponsor: GlaxoSmithKline

Brief Summary

The RTS, S/AS01E vaccine was developed to protect children in sub-Saharan Africa from malaria as part of routine immunization programs. This study aims to check the vaccine's safety after it has been introduced. Along with safety, researchers will also assess how well the vaccine works and its overall impact on children's health.

Detailed Description

This is a disease surveillance study with prospective cohort event monitoring including both temporal and concurrent comparisons of the occurrence of adverse and malaria events between vaccinated and unvaccinated subjects living in exposed or unexposed clusters located in sub-Saharan Africa (SSA) countries, and eligible for RTS,S/AS01E vaccination for those living in the exposed clusters. The design includes active surveillance and enhanced hospitalization surveillance in both exposed and unexposed clusters.

The study targeted enrolling at least 45,000 children in active surveillance, including 22,500 in the exposed clusters and 22,500 in the unexposed clusters for evaluation of the vaccine safety, effectiveness, and impact.

All data analyses will be computed in a descriptive manner. Data regarding the hospitalization will be uniformly collected whether the child is enrolled in active surveillance or in enhanced hospitalization surveillance.

Study Timeline

• Study First Submitted: 2019-02-25
• Study First Submitted QC: 2019-02-25
• Study First Posted: 2019-02-27
• Study Start: 2019-03-21
• Status Verified: 2025-02
• Last Update Submitted: 2025-02-14
• Last Update Posted: 2025-02-18
• Primary Completion: 2025-05-26
• Study Completion: 2025-05-26

Recruitment & Eligibility

• Status: RECRUITING
• Sex: All
• Target Recruitment: 78000

Inclusion Criteria

Not provided

Exclusion Criteria

• Child in care = A child who has been placed under the control or protection of an agency, organization, institution or entity by the courts, the government, or a government body, acting in accordance with powers conferred on them by law or regulation. The definition of a child in care can include a child cared for by foster parents or living in a care home or institution, provided that the arrangement falls within the definition above. The definition of a child in care does not include a child who is adopted or has an appointed legal guardian.

Study & Design

• Study Type: OBSERVATIONAL
• Study Design: Not specified

Arm && Interventions

Group	Intervention	Description
Active surveillance (DTP sub-Group)	Whole blood sample	Children enrolled in the active surveillance (AS), \<18 months of age who were identified at any administration of DTP/HepB/Hib (usually given at 6, 10 and 14 weeks of age) or at hospitalisation before administration of 3rd dose of DTP/HepB/Hib and vaccinated with at least one dose of DTP/HepB/Hib; including both RTS,S/AS01E vaccinated and unvaccinated children (from exposed or unexposed clusters), living in the HDSS area are eligible for enrolment in the DTP sub-group of active surveillance.
Enhanced Hospitalisation Surveillance Group	Whole blood sample	Children at least 6 weeks and \<5 years of age, within the study areas in both exposed and unexposed clusters, not already enrolled in the active surveillance (because parents/ Legally Acceptable Representative (LARs) declined enrolment in active surveillance or because recruitment had been completed) or not eligible for active surveillance at the time of hospitalisation, living in the HDSS area are eligible for enrolment in the Enhanced Hospital Surveillance (EHS) group.
Active surveillance (Catch-up sub-Group)	Whole blood sample	Children enrolled in the active surveillance (AS), \<18 months of age who were identified at 1st RTS,S/AS01E dose administration and who either received all DTP/HepB/Hib doses before study start or received at least one dose of DTP/HepB/Hib and are older than the age corresponding to the 3rd DTP/HepB/Hib dose at study start; including only RTS,S/AS01E vaccinated children from exposed clusters who could not be recruited at the time of DTP/HepB/Hib administration because the study had not yet started, living in the HDSS area are eligible for enrolment in the Catch-up sub-group of active surveillance.

Primary Outcome Measures

Name	Time	Method
Incidence rates of aetiology-confirmed meningitis	During the entire study period (From Day 0 up to Month 62)	Incidence rate of aetiology confirmed meningitis is analyzed with an at-risk period of 12 months. At the site level, a suspected meningitis case based on clinical symptoms and/or signs is defined as: * A child with sudden onset of fever (\> 38.0°C rectal or 37.5°C axillary) and one or more of the following signs: neck stiffness, altered consciousness with no other alternative diagnosis, or other meningeal sign such as bulging fontanelle in children under one year of age.; If a Cerebrospinal fluid (CSF) sample is available and any known aetiologic agent (bacterial or not) has been identified, it is defined as an aetiology confirmed meningitis.; The incidence rate will be calculated by dividing the number of study participants reporting at least one event over the follow-up period by the total person-time.
Incidence rates of adverse events of special interest (AESI)	During the entire study period (From Day 0 up to Month 62)	AESI are predefined list of adverse events that have historically been associated with vaccines other than RTS,S/AS01E, or may hypothetically be associated with RTS,S/AS01E due to the fact that this vaccine has components which are new compared to current widely used vaccines.; The incidence rate will be calculated by dividing the number of study participants reporting at least one event over the follow-up period by the total person-time. The person-time for an event of interest will be calculated as the time between the reference date (date of first RTS,S/AS01E vaccination for the vaccinated study participants and virtual vaccination corresponding to the week before first visit for the unvaccinated study participants) and the end of the at-risk period or the earliest of the followings: Date of first diagnosis of event of interest, Date of end of study period, Date when child reaches 5 years, Date of last contact or Date of death.

Secondary Outcome Measures

Name	Time	Method
Incidence rate of probable meningitis (final classification)	During the entire study period (From Day 0 up to Month 62)	At the site level, a suspected probable meningitis case based on clinical symptoms and/or signs is defined by the below characteristics: CSF sample is available, no bacterial agent has been identified in the CSF, but some abnormalities in the CSF have been detected (such as turbid macroscopic aspect, positive Gram, positive antigen test, pleiocytosis, abnormal glucose or protein levels) or positive blood culture to a bacterial agent.; The incidence rate will be calculated by dividing the number of study participants reporting at least one event over the follow-up period by the total person-time.
Incidence rates of clinically suspected meningitis (final classification)	During the entire study period (From Day 0 up to Month 62)	At the site level, a clinically suspected meningitis case based on clinical symptoms and/or signs is defined by the below characteristics: * If a CSF sample is available and all examinations are normal at first line laboratory level, or if no CSF sample is available and no alternative diagnosis.; The incidence rate will be calculated by dividing the number of study participants reporting at least one event over the follow-up period by the total person-time.
Number of meningitis cases identified at site level (first line laboratory)	During the entire study period (From Day 0 up to Month 62)	At the site level, a suspected meningitis case based on clinical symptoms and/or signs is defined as: * A child with sudden onset of fever (\> 38.0°C rectal or 37.5°C axillary) and one or more of the following signs: neck stiffness, altered consciousness with no other alternative diagnosis, or other meningeal sign such as bulging fontanelle in children under one year of age.
Incidence rates of cerebral malaria (diagnosed by Rapid Diagnostic Test [RDT] and/or microscopy)	During the entire study period (From Day 0 up to Month 62)	Cerebral malaria is defined as: * Severe Plasmodium falciparum malaria with impaired consciousness (Glasgow coma score \< 11 in children ≥ 2 years of age or Blantyre coma score \< 3 in children \< 2 years of age); And,; * If malaria with seizure: coma persisting for \> 30 min after the seizure.; * Other treatable causes of coma should be excluded before diagnosing cerebral malaria (e.g. hypoglycaemia, bacterial meningitis).; Suspected malaria cases routinely tested using RDT will have a blood smear for reading by microscopy in parallel, in order to measure sensitivity and specificity. This is done for all suspected cases presenting at primary health care facilities one day per month during the first year of the study.; The incidence rate will be calculated by dividing the number of study participants reporting at least one event over the follow-up period by the total person-time.
Incidence rates of malaria episodes diagnosed by RDT and/or microscopy	During the entire study period (From Day 0 up to Month 62)	Any malaria is uncomplicated malaria (i.e. Plasmodium parasitaemia \>0 detected by microscopy and/or RDT, presence of fever (≥37.5°C) reported by parent(s)/LARs or recorded at time of presentation and without severity signs or vital organ dysfunction) and severe malaria (SM) (i.e. P. falciparum parasitaemia \>0 detected by microscopy and/or RDT, one/more of the following: impaired consciousness, prostration, multiple convulsions, acidosis, hypoglycemia, severe malarial anemia, renal impairment, jaundice, pulmonary oedema, significant bleeding, shock, hyperparasitemia). Severe vivax malaria is SM but with no parasite density thresholds. Cerebral malaria is SM with impaired consciousness with the exclusion of other treatable causes of coma. The incidence rate will be calculated by dividing the number of subjects reporting at least one event over the follow-up period by the total person-time.
Incidence rates of anaemia cases at hospital entry among hospitalised children	During the entire study period (From Day 0 up to Month 62)	This outcome measure is assessed for children included only in active surveillance.; Anaemia is defined as: * All anaemia: haemoglobin \<11 (grams per decilitre) g/dL.; * Severe anaemia: haemoglobin \<7g/dL. The incidence rate will be calculated by dividing the number of study participants reporting at least one event over the follow-up period by the total person-time.
Incidence rates of hospitalisation cases	During the entire study period (From Day 0 up to month 62)	Hospitalisation is defined as: All causes and hospitalisations for any malaria (including P. falciparum malaria), severe malaria (including P. falciparum malaria) and cerebral malaria.; A hospitalised study participant with malaria (including P. falciparum malaria) and for whom malaria is the primary cause of hospitalisation.; This outcome measure is assessed for children included only in active surveillance.; The incidence rate will be calculated by dividing the number of study participants reporting at least one event over the follow-up period by the total person-time.
Number of deaths	During the entire study period (From Day 0 up to month 62)	Death is defined as: * Malaria attributed death (including P. falciparum malaria) defined as a fatality for which malaria (including P. falciparum malaria) is listed as a contributing cause of death, based on either verbal autopsy using the INDEPTH Standard Verbal Autopsy Questionnaire for children, who died at home or medical judgment/medical records for children who died at a primary health care facility or hospital.; * Deaths attributed to an AE defined as a fatality for which an AE is listed as a contributing cause of death, based on either verbal autopsy using the INDEPTH Standard Verbal Autopsy Questionnaire for children, who died at home or medical judgment/medical records for children who died at a primary health care facility or hospital.; The incidence rate (mortality rate) will be calculated by dividing the number of study participants reporting at least one event over the follow-up period by the total person-time.

Trial Locations

Locations (1)

GSK Investigational Site; 🇲🇼 Mangochi, Malawi