A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania

A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania

<p>Abstract</p> <p>Background</p> <p>Effective mass drug administration (MDA) with anti-malarial drugs can clear the human infectious reservoir for malaria and thereby interrupt malaria transmission. The likelihood of success of MDA depends on the intensity and seasonal...

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Main Authors: Shekalaghe Seif A, Drakeley Chris, van den Bosch Sven, ter Braak Roel, van den Bijllaardt Wouter, Mwanziva Charles, Semvua Salimu, Masokoto Alutu, Mosha Frank, Teelen Karina, Hermsen Rob, Okell Lucy, Gosling Roly, Sauerwein Robert, Bousema Teun
Format: Article
Language:English
Published: BMC 2011-08-01
Series:Malaria Journal
Online Access:http://www.malariajournal.com/content/10/1/247
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spelling doaj-5cd8b83a33b0480083d440233d60175a2020-11-24T22:09:47ZengBMCMalaria Journal1475-28752011-08-0110124710.1186/1475-2875-10-247A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in TanzaniaShekalaghe Seif ADrakeley Chrisvan den Bosch Sventer Braak Roelvan den Bijllaardt WouterMwanziva CharlesSemvua SalimuMasokoto AlutuMosha FrankTeelen KarinaHermsen RobOkell LucyGosling RolySauerwein RobertBousema Teun<p>Abstract</p> <p>Background</p> <p>Effective mass drug administration (MDA) with anti-malarial drugs can clear the human infectious reservoir for malaria and thereby interrupt malaria transmission. The likelihood of success of MDA depends on the intensity and seasonality of malaria transmission, the efficacy of the intervention in rapidly clearing all malaria parasite stages and the degree to which symptomatic and asymptomatic parasite carriers participate in the intervention. The impact of MDA with the gametocytocidal drug combination sulphadoxine-pyrimethamine (SP) plus artesunate (AS) plus primaquine (PQ, single dose 0.75 mg/kg) on malaria transmission was determined in an area of very low and seasonal malaria transmission in northern Tanzania.</p> <p>Methods</p> <p>In a cluster-randomized trial in four villages in Lower Moshi, Tanzania, eight clusters (1,110 individuals; cluster size 47- 209) were randomized to observed treatment with SP+AS+PQ and eight clusters (2,347 individuals, cluster size 55- 737) to treatment with placebo over three days. Intervention and control clusters were 1km apart; households that were located between clusters were treated as buffer zones where all individuals received SP+AS+PQ but were not selected for the evaluation. Passive case detection was done for the entire cohort and active case detection in 149 children aged 1-10 year from the intervention arm and 143 from the control arm. Four cross-sectional surveys assessed parasite carriage by microscopy and molecular methods during a five-month follow-up period.</p> <p>Results</p> <p>The coverage rate in the intervention arm was 93.0% (1,117/1,201). Parasite prevalence by molecular detection methods was 2.2-2.7% prior to the intervention and undetectable during follow-up in both the control and intervention clusters. None of the slides collected during cross-sectional surveys had microscopically detectable parasite densities. Three clinical malaria episodes occurred in the intervention (n = 1) and control clusters (n = 2).</p> <p>Conclusions</p> <p>This study illustrates the possibility to achieve high coverage with a three-day intervention but also the difficulty in defining suitable outcome measures to evaluate interventions in areas of very low malaria transmission intensity. The decline in transmission intensity prior to the intervention made it impossible to assess the impact of MDA in the chosen study setting.</p> <p>Trial Registration</p> <p>ClinicalTrials.gov: <a href="http://www.clinicaltrials.gov/ct2/show/NCT00509015">NCT00509015</a></p> http://www.malariajournal.com/content/10/1/247
collection DOAJ
language English
format Article
sources DOAJ
author Shekalaghe Seif A
Drakeley Chris
van den Bosch Sven
ter Braak Roel
van den Bijllaardt Wouter
Mwanziva Charles
Semvua Salimu
Masokoto Alutu
Mosha Frank
Teelen Karina
Hermsen Rob
Okell Lucy
Gosling Roly
Sauerwein Robert
Bousema Teun
spellingShingle Shekalaghe Seif A
Drakeley Chris
van den Bosch Sven
ter Braak Roel
van den Bijllaardt Wouter
Mwanziva Charles
Semvua Salimu
Masokoto Alutu
Mosha Frank
Teelen Karina
Hermsen Rob
Okell Lucy
Gosling Roly
Sauerwein Robert
Bousema Teun
A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania
Malaria Journal
author_facet Shekalaghe Seif A
Drakeley Chris
van den Bosch Sven
ter Braak Roel
van den Bijllaardt Wouter
Mwanziva Charles
Semvua Salimu
Masokoto Alutu
Mosha Frank
Teelen Karina
Hermsen Rob
Okell Lucy
Gosling Roly
Sauerwein Robert
Bousema Teun
author_sort Shekalaghe Seif A
title A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania
title_short A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania
title_full A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania
title_fullStr A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania
title_full_unstemmed A cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in Tanzania
title_sort cluster-randomized trial of mass drug administration with a gametocytocidal drug combination to interrupt malaria transmission in a low endemic area in tanzania
publisher BMC
series Malaria Journal
issn 1475-2875
publishDate 2011-08-01
description <p>Abstract</p> <p>Background</p> <p>Effective mass drug administration (MDA) with anti-malarial drugs can clear the human infectious reservoir for malaria and thereby interrupt malaria transmission. The likelihood of success of MDA depends on the intensity and seasonality of malaria transmission, the efficacy of the intervention in rapidly clearing all malaria parasite stages and the degree to which symptomatic and asymptomatic parasite carriers participate in the intervention. The impact of MDA with the gametocytocidal drug combination sulphadoxine-pyrimethamine (SP) plus artesunate (AS) plus primaquine (PQ, single dose 0.75 mg/kg) on malaria transmission was determined in an area of very low and seasonal malaria transmission in northern Tanzania.</p> <p>Methods</p> <p>In a cluster-randomized trial in four villages in Lower Moshi, Tanzania, eight clusters (1,110 individuals; cluster size 47- 209) were randomized to observed treatment with SP+AS+PQ and eight clusters (2,347 individuals, cluster size 55- 737) to treatment with placebo over three days. Intervention and control clusters were 1km apart; households that were located between clusters were treated as buffer zones where all individuals received SP+AS+PQ but were not selected for the evaluation. Passive case detection was done for the entire cohort and active case detection in 149 children aged 1-10 year from the intervention arm and 143 from the control arm. Four cross-sectional surveys assessed parasite carriage by microscopy and molecular methods during a five-month follow-up period.</p> <p>Results</p> <p>The coverage rate in the intervention arm was 93.0% (1,117/1,201). Parasite prevalence by molecular detection methods was 2.2-2.7% prior to the intervention and undetectable during follow-up in both the control and intervention clusters. None of the slides collected during cross-sectional surveys had microscopically detectable parasite densities. Three clinical malaria episodes occurred in the intervention (n = 1) and control clusters (n = 2).</p> <p>Conclusions</p> <p>This study illustrates the possibility to achieve high coverage with a three-day intervention but also the difficulty in defining suitable outcome measures to evaluate interventions in areas of very low malaria transmission intensity. The decline in transmission intensity prior to the intervention made it impossible to assess the impact of MDA in the chosen study setting.</p> <p>Trial Registration</p> <p>ClinicalTrials.gov: <a href="http://www.clinicaltrials.gov/ct2/show/NCT00509015">NCT00509015</a></p>
url http://www.malariajournal.com/content/10/1/247
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