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Randomized Controlled Trial
. 2025 Jun;25(6):656-667.
doi: 10.1016/S1473-3099(24)00741-2. Epub 2025 Jan 9.

Effect of mass drug administration on malaria incidence in southeast Senegal during 2020-22: a two-arm, open-label, cluster-randomised controlled trial

El-Hadji Konko Ciré Ba  1 Michelle E Roh  2 Abdoulaye Diallo  1 Tidiane Gadiaga  3 Amadou Seck  1 Sylla Thiam  1 Ari Fogelson  4 Seynabou Gaye  5 Ibrahima Diallo  5 Aminata Colle Lo  1 Elhadji Diouf  6 Oumar Gallo Ba  1 Alioune Badara Gueye  7 Xue Wu  2 Paul Milligan  4 Tabitha Kibuka  8 Moustapha Hama  8 Erin Eckert  8 Julie Thwing  9 Adam Bennett  10 Roly Gosling  11 Jimee Hwang  12 Doudou Sene  5 Fatou Ba  5 Bayal Cissé  3 Katharine Sturm-Ramirez  7 Michelle S Hsiang  13 Jean Louis Ndiaye  1
Affiliations
Randomized Controlled Trial

Effect of mass drug administration on malaria incidence in southeast Senegal during 2020-22: a two-arm, open-label, cluster-randomised controlled trial

El-Hadji Konko Ciré Ba et al. Lancet Infect Dis. 2025 Jun.

Abstract

Background: In Africa, the scale-up of malaria-control interventions has reduced malaria burden, but progress towards elimination has stalled. Mass drug administration (MDA) is promising as a transmission-reducing strategy, but evidence from low-to-moderate transmission settings is needed. We aimed to assess the safety, coverage, and effect of three cycles of MDA with dihydroartemisinin-piperaquine plus single, low-dose primaquine on Plasmodium falciparum incidence and prevalence in southeast Senegal.

Methods: We conducted a two-arm, open-label, cluster-randomised controlled trial in villages in the Tambacounda health district of southeast Senegal. Eligible villages had a population size of 200-800, were within a health-post catchment area with an annual malaria incidence of 60-160 cases per 1000 people, and had an established or planned Prise en Charge à Domicile Plus model. We randomly assigned villages (1:1) using a stratified, constrained randomisation approach to receive either three cycles of MDA with oral dihydroartemisinin-piperaquine plus single, low-dose primaquine administered at 6-week intervals (intervention) or to standard of care, which included three cycles of seasonal malaria chemoprevention (SMC) with oral sulfadoxine-pyrimethamine plus amodiaquine administered at 4-week intervals (control). Participants, the field team, and all investigators, including those who assessed outcomes and analysed data, were unmasked to allocation assignment. Laboratory technicians were masked to intervention assignment. The primary outcome was village-level, P falciparum-confirmed malaria incidence in the post-intervention year (ie, July to December, 2022). Secondary outcomes included malaria incidence during the intervention year (ie, July to December, 2021), coverage and safety of MDA, and adverse events. We conducted analyses using an intention-to-treat approach. The trial is registered with ClinicalTrials.gov (NCT04864444) and is completed.

Findings: Between Sept 1 and Oct 25, 2020, 523 villages were geolocated and screened for eligibility; 111 met the inclusion criteria. Of these, 60 villages were randomly selected and assigned to the intervention arm or control arm. Distribution coverage of all three doses of dihydroartemisinin-piperaquine was 6057 (73·6%) of 8229 participants in the first cycle, 6836 (78·8%) of 8673 participants in the second cycle, and 7065 (81·3%) of 8690 participants in the third cycle. Distribution coverage of single, low-dose primaquine was 6286 (78·6%) of 7999 participants in the first cycle, 6949 (82·1%) of 8462 participants in the second cycle, and 7199 (84·0%) of 8575 participants in the third cycle. Distribution coverage of all three doses of SMC was 3187 (92·2%) of 3457 children aged 3-120 months in the first cycle, 3158 (91·8%) of 3442 children aged 3-120 months in the second cycle, and 3139 (91·4%) of 3434 children aged 3-120 months in the third cycle. In the intervention year (ie, July to December, 2021), the adjusted effect of MDA was 55% (95% CI 28 to 71). In the post-intervention year (ie, July to December 2022), the adjusted MDA effect was 26% (-17 to 53). Malaria incidence during the transmission season of the post-intervention year was 126 cases per 1000 population in the intervention arm and 146 cases per 1000 population in the control arm. No serious adverse events were reported.

Interpretation: In southeast Senegal, a low-to-moderate transmission setting where malaria-control measures have been scaled up, three cycles of MDA with dihydroartemisinin-piperaquine plus single, low-dose primaquine was safe and reduced malaria burden during the intervention year. However, its sustained effect was weak and continuation of MDA or another transmission-reducing strategy could be required.

Funding: US President's Malaria Initiative.

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Conflict of interest statement

Declaration of interests MER is funded by the Eunice Kennedy Shriver National Institute Of Child Health & Human Development of the US National Institutes of Health (K99HD111572). JH, KS-R, and ABG receive or have received salary support and travel expenses from the US President's Malaria Initiative. RG has received salary support from Unitaid, consultancy fees from Population Services International and Pelumbra, and honoraria from the University of Cape Town. All other authors declare no competing interests.

Figures

Figure 1:
Figure 1:
Trial timeline MDA=mass drug administration. PECADOM+=Prise en Charge à Domicile Plus. SMC=seasonal malaria chemoprevention.
Figure 2:
Figure 2:
Trial profile MDA=mass drug administration. PECADOM+=Prise en Charge à Domicile Plus. SMC=seasonal malaria chemoprevention.
See this image and copyright information in PMC

References

    1. WHO. WHO guidelines for malaria, 3 June 2022. 2022. https://iris.who.int/bitstream/handle/10665/354781/WHO-UCN-GMP-2022.01-R... (accessed Aug 2, 2024).
    1. Seasonal Malaria Chemoprevention Alliance. 53 million children living in 18 countries covered with seasonal malaria chemoprevention in 2023. 2024. https://www.smc-alliance.org/53-million-children-living-in-18-countries-... (accessed July 17, 2024).
    1. WHO. World malaria report 2022. 2022. https://www.who.int/teams/global-malaria-programme/reports/world-malaria... (accessed April 6, 2024).
    1. Cairns M, Ceesay SJ, Sagara I, et al. Effectiveness of seasonal malaria chemoprevention (SMC) treatments when SMC is implemented at scale: case-control studies in 5 countries. PLoS Med 2021; 18: e1003727. - PMC - PubMed
    1. Shah MP, Hwang J, Choi L, Lindblade KA, Kachur SP, Desai M. Mass drug administration for malaria. Cochrane Database Syst Rev 2021; 9: CD008846. - PMC - PubMed

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