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Modelling the incremental benefit of introducing malaria screening strategies to antenatal care in Africa.

Patrick G T WalkerMatthew E CairnsHannah SlaterJulie R GutmanKassoum KayentaoJohn E WilliamsSheick O CoulibalyCarole KhairallahSteve TaylorSteven R MeshnickJenny HillVictor MwapasaLinda Kalilani-PhiriKalifa BojangSimon KariukiHarry TagborJamie T GriffinMwayi MadanitsaAzra C H GhaniMeghna DesaiFeiko O Ter Kuile
Published in: Nature communications (2020)
Plasmodium falciparum in pregnancy is a major cause of adverse pregnancy outcomes. We combine performance estimates of standard rapid diagnostic tests (RDT) from trials of intermittent screening and treatment in pregnancy (ISTp) with modelling to assess whether screening at antenatal visits improves upon current intermittent preventative therapy with sulphadoxine-pyrimethamine (IPTp-SP). We estimate that RDTs in primigravidae at first antenatal visit are substantially more sensitive than in non-pregnant adults (OR = 17.2, 95% Cr.I. 13.8-21.6), and that sensitivity declines in subsequent visits and with gravidity, likely driven by declining susceptibility to placental infection. Monthly ISTp with standard RDTs, even with highly effective drugs, is not superior to monthly IPTp-SP. However, a hybrid strategy, recently adopted in Tanzania, combining testing and treatment at first visit with IPTp-SP may offer benefit, especially in areas with high-grade SP resistance. Screening and treatment in the first trimester, when IPTp-SP is contraindicated, could substantially improve pregnancy outcomes.
Keyphrases
  • pregnancy outcomes
  • pregnant women
  • plasmodium falciparum
  • preterm birth
  • high grade
  • healthcare
  • emergency department
  • palliative care
  • quality improvement
  • combination therapy
  • bone marrow
  • adverse drug