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Clinical Trial Summary

This is a cluster randomised controlled trial comparing the impact of two community based malaria interventions: reactive case detection (RACD) vs reactive targeted presumptive treatment (focal mass drug administration, fMDA) on the incidence of malaria in Swaziland.


Clinical Trial Description

Title Evaluating the effectiveness and feasibility of reactive focal mass drug administration (fMDA) vs. reactive case detection (RACD) as a community level intervention in response to a passively identified index malaria case in Swaziland Study design Cluster randomised controlled trial Aims Primary aim: To compare the impact of fMDA versus RACD on malaria incidence. Secondary aims Effectiveness: 1. To compare the impact of fMDA versus RACD on seroprevalence. 2. To compare the impact of fMDA versus RACD on prevalence of infection. Feasibility: 1. To evaluate the safety of fMDA. 2. To measure the adherence of DHAp using a modified DOT regimen. 3. To determine the feasibility of reaching 80% coverage for fMDA. 4. To compare the acceptability of fMDA. 5. To compare the costs and cost-effectiveness of fMDA versus RACD. Study site Eastern endemic region of Swaziland, a very low endemic malaria elimination setting. A total of 287 health facilities and their catchment areas are located in this area. Time frame September 2015 - August 2017 Cluster or unit of randomisation At-risk localities will be randomized to either fMDA or RACD using a block stratified randomization based on risk rank and population Target area Individuals residing within 200 m (fMDA arm) or 500 m (RACD arm) of an index case detected in passive surveillance, individuals residing immediately beyond 200 m in the fMDA arm will be included if a minimum of 30 individuals are not enrolled within 200 m. Intervention All individuals residing in study localities will receive vector control preventative measures as per program. In the fMDA arm, all individuals in the target area will receive dihydroartemisinin-piperaquine (DHAp) once daily for 3 days with the first dose taken no later than 5 weeks from the index case presentation (goal within one week). Individuals in RACD target areas will be tested by RDT and taken to the nearest health facility for treatment as per program operating procedures. Evaluation methods The primary outcome measure of incidence will be obtained through routine surveillance data. Secondary outcomes of effectiveness will be measured at study conclusion by collecting a dried blood spot (DBS) from all residents in target areas in both arms. Prevalence of infection will be measured by loop-mediated isothermal amplification (LAMP) and seroprevalence measured by quantifying markers of recent malaria exposure. Secondary outcomes of feasibility will be measured as follows: 1. Safety: number of serious adverse events deemed possibly, probably, or definitely related to DHAp. 2. Adherence: proportion of individuals who completed three days of therapy among all individuals initiated on DHAp in the fMDA arm, assessed by pill count. 3. Coverage: proportion of individuals residing within 200m (fMDA localities) or 500m (RACD localities) of an index case who consented to participate and who completed the initial procedures for their study arm (initial dose of DHAp in the fMDA arm or finger prick for RDT in the RACD arm). 4. Acceptability: proportion of eligible individuals refusing to take part in the study and a qualitative assessment of a subset of individuals in the fMDA arm. 5. Cost: cost per index case-level intervention and cost per case averted. Sample size The sample size is based on the number of study localities that experienced at least one incident case of malaria in the previous season. Within 77 randomized localities, we expect that 63 localities will have an incident case of malaria and receive an intervention. For the primary objective, we hypothesize that mFDA will be more effective than RACD. At the current sample size, the study is powered to detect a difference in cumulative incidence if incidence in the fMDA arm is reduced 50% compared to the RACD arm. Incidence will be measured at the locality level and among the at-risk population, or all individuals in an enumeration area (EA) where at least one case was identified (expected to be approximately 55,928 individuals among a total study population of 211,189, or a harmonic mean of 656 per locality (41,328 effective population)). Secondary outcomes of seroprevalence and prevalence will be measured on individuals residing in target areas (total N=5,400) with a harmonic mean of 60 persons receiving intervention per locality (3,780 effective population). Primary outcome Incidence of malaria cases Secondary outcomes 1. Seroprevalence by ELISA 2. Prevalence of infection 3. Coverage of the intervention: proportion of the target population that receives a finger prick in the RACD arm and receives an initial dose of DHAp in the TPE arm (intention to treat analysis). 4. Adherence to DHAp in TPE arm. 5. Safety of DHAp 6. Acceptance 7. Cost per intervention episode, per case averted ;


Study Design


Related Conditions & MeSH terms


NCT number NCT02315690
Study type Interventional
Source University of California, San Francisco
Contact
Status Completed
Phase Phase 3
Start date September 2015
Completion date July 2017

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