Mass campaigns with antimalarial drugs: a modelling comparison of artemether-lumefantrine and DHA-piperaquine with and without primaquine as tools for malaria control and elimination
Authored by Edward A Wenger, Jaline Gerardin, Philip Eckhoff
Date Published: 2015
DOI: 10.1186/s12879-015-0887-y
Sponsors:
Bill and Melinda Gates Foundation
Platforms:
EDMOD
Model Documentation:
Other Narrative
Mathematical description
Model Code URLs:
Model code not found
Abstract
Background: Antimalarial drugs are a powerful tool for malaria control
and elimination. Artemisinin-based combination therapies (ACTs) can
reduce transmission when widely distributed in a campaign setting.
Modelling mass antimalarial campaigns can elucidate how to most
effectively deploy drug-based interventions and quantitatively compare
the effects of cure, prophylaxis, and transmission-blocking in
suppressing parasite prevalence.
Methods: A previously established agent-based model that includes innate
and adaptive immunity was used to simulate malaria infections and
transmission. Pharmacokinetics of artemether, lumefantrine, dihydroartemisinin, piperaquine, and primaquine were modelled with a
double-exponential distribution-elimination model including
weight-dependent parameters and age-dependent dosing. Drug killing of
asexual parasites and gametocytes was calibrated to clinical data. Mass
distribution of ACTs and primaquine was simulated with seasonal mosquito
dynamics at a range of transmission intensities.
Results: A single mass campaign with antimalarial drugs is insufficient
to permanently reduce malaria prevalence when transmission is high.
Current diagnostics are insufficiently sensitive to accurately identify
asymptomatic infections, and mass-screen-and-treat campaigns are much
less efficacious than mass drug administrations. Improving campaign
coverage leads to decreased prevalence one month after the end of the
campaign, while increasing compliance lengthens the duration of
protection against reinfection. Use of a long-lasting prophylactic as
part of a mass drug administration regimen confers the most benefit
under conditions of high transmission and moderately high coverage.
Addition of primaquine can reduce prevalence but exerts its largest
effect when coupled with a long-lasting prophylactic.
Conclusions: Mass administration of antimalarial drugs can be a powerful
tool to reduce prevalence for a few months post-campaign. A
slow-decaying prophylactic administered with a parasite-clearing drug
offers strong protection against reinfection, especially in highly
endemic areas. Transmission-blocking drugs have only limited effects
unless administered with a prophylactic under very high coverage.
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