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Clinical Trial Details — Status: Active, not recruiting

Administrative data

NCT number NCT05471544
Other study ID # SMCSSPHASE1
Secondary ID
Status Active, not recruiting
Phase Phase 3
First received
Last updated
Start date July 18, 2022
Est. completion date December 31, 2024

Study information

Verified date October 2023
Source Malaria Consortium
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This study aims to explore whether SMC is an effective intervention in the context of Northen Bahr el Gazal state, South Sudan. It also aims to assess the protective efficacy of the antimalarials used in SMC in the target population and investigate levels of parasite resistance in the study counties. If successful, this trial should provide the evidence for SMC to be included in malaria programming and policy in South Sudan. A Type II hybrid effectiveness-implementation study design will be used to evaluate the effects of a clinical intervention on relevant outcomes whilst collecting information on implementation. It is designed to determine feasibility and effectiveness of an innovative intervention, as well as the protective efficacy of the antimalarial drugs used. The study consists of five components: 1) A series of cross-sectional surveys establishing confirmed malaria cases in children; 2) A prospective cohort study to determine the protective efficacy of SPAQ (if SPAQ provides 28 days of protection from infection) and whether drug concentrations and/or resistance influence the duration of protection; 3) A resistance markers study in children 3-59 months in the research county; 4) Modelling the protective effect of SPAQ in South Sudan to determine where SMC could be a suitable malaria prevention strategy in other areas of the country, and 5) A process evaluation to understand feasibility and acceptability of the SMC intervention in South Sudan.


Description:

This is an implementation research study, using a Type II hybrid effectiveness-implementation study design, to evaluate the effects of a clinical intervention on relevant outcomes whilst collecting information on implementation. The study uses pragmatic implementation research with the objective of contributing to the development of practical recommendations for health policy, practice and potential scale up. It is designed as an implementation study to determine effectiveness and protective efficacy to gather evidence of its potential impact on health outcomes. Five monthly cycles of SMC will be implemented between June and October 2022 in one county, Aweil South, in Northern Bahr el Gazal state. The study will comprise the following six components : 1. Two cross-sectional surveys at the height of the malaria season to explore impact on malaria incidence 2. End-of-round survey 3. Prospective protective efficacy cohort study to determine if SPAQ provides 28 days of protection from infection and whether drug concentrations and/or resistance influence the duration of protection 4. Resistance markers study in children 3-59 months in the two research counties plus the two standard intervention counties to measure changes in resistance marker prevalence over time (pre and post within the same year and between years)


Recruitment information / eligibility

Status Active, not recruiting
Enrollment 3575
Est. completion date December 31, 2024
Est. primary completion date December 15, 2024
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 3 Months to 59 Months
Eligibility Inclusion Criteria: - Being resident in the project area - Afebrile with no other malaria associated symptoms in the past 48 hours or at time of recruitment - Consent to participate in the study obtained - Can comply with 3 day DOT of standard SPAQ regimen (day 0-2) - Willingness and ability of the childs guardians to comply with the study protocol for the duration of the study including all dry blood spot and slide collections Exclusion Criteria: - Symptoms of malaria (tympanic fever = 37.5 °C or history of fever in past 48 hours) - Known allergy to medicine provided - Receiving a sulfa-based medication for treatment or prophylaxis, including co-trimoxazole (trimethoprim-sulfamethoxazole). - Individuals receiving azithromycin due to the antimalarial activity of azithromycin. - Severe malnutrition according to WHO guidelines - Recruited in cross sectional surveys or any other SMC studies. - Children with HIV - Previous treatment with Amodiaquine in the past 28 days (treatment with ASAQ or SPAQ)

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Sulfadoxine pyrimethamine
Sulphadoxine is a slowly eliminated sulphonamide. It is used in a fixed dose combination of 20 parts sulphadoxine with 1 part pyrimethamine given orally or intramuscularly. The medicine is no longer recommended for the treatment of malaria. However, it is being used for Intermittent Preventive Treatment during pregnancy (IPTp) and as a co-packaged combination with amodiaquine for seasonal malaria chemoprevention. Sulphadoxine is readily absorbed from the GIT. It is widely distributed in body tissues and fluids and crosses the placenta into foetal circulation. It is also readily detectable in breast milk. It is excreted predominantly as the unchanged drug.
Amodiaquine
Amodiaquine is a Mannich base 4 amino-quinoline that interferes with parasite haem detoxification. It is more effective than chloroquine in both chloroquine sensitive and resistant P. falciparum infections. However, there is cross-resistance between chloroquine and amodiaquine. It is readily absorbed in the GIT and rapidly converted in the liver to the active metabolite, desethylamodiaquine. Desethylamodiaquine is responsible for all the antimalarial effect.

Locations

Country Name City State
South Sudan Aweil South Aweil Northern Bahr El Gazal

Sponsors (1)

Lead Sponsor Collaborator
Malaria Consortium

Country where clinical trial is conducted

South Sudan, 

Outcome

Type Measure Description Time frame Safety issue
Primary Malaria incidence in study population in intervention county and eligible children in one control county Number of malaria cases in the intervention population and eligible children in one control county over the study period as reported through care givers in cross-sectional surveys at baseline, mid-intervention and endline Five months
Primary Chemoprevention failure as defined by positive parasites in malaria slides after day 7 or positive qPCR in dried blood spot (DBS) on day 28 Malaria slides and dry blood spots (DBS) taken at days 0,7, 28 will be analysed with qPCR methodology to detect low level submicroscopic parasitemia in children treated with SPAQ One month
Primary Prevalence of antimalarial resistance markers (dhfr, dhps, Pfcrt, pfmdr1) among chemoprevention failures as defined in outcome 2 All Dried blood spots (DBS) will be analysed for malaria mutation genotypes (dhfr, dhps, Pfcrt, pfmdr1) on baseline and endline and additionally on day 7, day 28, or if participant slide is positive for parasites on day 7 or an infection is reported through care givers in cross-sectional survey. One month
Primary Drug concentrations of Sulfadoxine-pyrimethamine and amodiaquine among chemoprevention failures (as defined in outcome 1) Drug concentrations will be analyzed for all samples on baseline, day 7 and day 28 and will be linked to chemoprevention failure cases as defined in outcome 2 or a malaria infection is reported through care givers in cross sectional survey. One month
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