Mandoko, Papy Nkoli, Rouvier, Florent, Kakina, Lebon Matendo, Mbongi, Destin Moke, Latour, Christine, Likwela, Joris Losimba, Mumba, Dieudonné Ngoyi, Shamamba, Stomy Karhemere Bi, Muyembe, Jean-Jacques Tamfum, Tshilolo, Léon Muepu, Nkoli Mandoko, Papy, Matendo Kakina, Lebon, Moke Mbongi, Destin, Losimba Likwela, Joris, Ngoyi Mumba, Dieudonné, Bi Shamamba, Stomy Karhemere, Tamfum Muyembe, Jean-Jacques, Muepu Tshilolo, Léon, Parzy, Daniel, and Sinou, Véronique
Background: In 2005, the Democratic Republic of the Congo (DRC) switched to artesunate/amodiaquine as the first-line antimalarial in response to increasing sulfadoxine/pyrimethamine resistance and adopted intermittent preventive treatment using sulfadoxine/pyrimethamine in pregnancy.Objectives: To determine the prevalence of molecular markers of sulfadoxine/pyrimethamine resistance in southwestern DRC 10 years after the new policy was instituted.Methods: From March 2014 to December 2015, blood samples were collected from symptomatic patients presenting to outpatient centres in urban and rural areas. A total of 2030 confirmed Plasmodium falciparum isolates were genotyped at codons associated with sulfadoxine/pyrimethamine resistance.Results: The prevalence of pfdhfr-N51I, C59R and S108N and pfdhps-A437G mutations was consistently high; the prevalence of the pfdhps-K540E mutation was low but increased since its first report in 2008 in the same region, reaching 17.6% by 2015. The pfdhps-A581G mutation increased from ∼4.5% in 2014 to ∼14.0% in 2015 at urban sites while in rural areas it remained low (∼4.0%). The mutations pfdhfr-I164L and pfdhps-A613S were detected for the first time in DRC. Also, 11 (0.8%) isolates revealed the presence of the newly described pfdhps-I431V mutation. Combining pfdhfr and pfdhps alleles, quintuple and sextuple mutations were observed, with the emergence of septuple (IRNI/IAGEGA)- and octuple (IRNI/VAGKGS)-mutant genotypes.Conclusions: Intermittent preventive treatment using sulfadoxine/pyrimethamine during pregnancy remains warranted in southwestern DRC. However, the expansion of pfdhps-K540E mutation and emergence of mutants that cause higher levels of sulfadoxine/pyrimethamine resistance is concerning and may present a challenge for future preventive interventions in the country. [ABSTRACT FROM AUTHOR]