Litcius/Paper detail

Treatment Failure in a UK Malaria Patient Harboring Genetically Variant <i>Plasmodium falciparum</i> From Uganda With Reduced In Vitro Susceptibility to Artemisinin and Lumefantrine

Donelly A. van Schalkwyk, Sade Pratt, Debbie Nolder, Lindsay B. Stewart, Helen Liddy, Julian Muwanguzi-Karugaba, Khalid B. Beshir, D Britten, Emma L. Victory, Claire Rogers, James Millard, Michael Brown, Laura Nabarro, Andrew Taylor, Bernadette Young, Peter L. Chiodini, Colin J. Sutherland

2023Clinical Infectious Diseases43 citationsDOIOpen Access PDF

Abstract

BACKGROUND: Recent cases of clinical failure in malaria patients in the United Kingdom (UK) treated with artemether-lumefantrine have implications for malaria chemotherapy worldwide. METHODS: Parasites were isolated from an index case of confirmed Plasmodium falciparum treatment failure after standard treatment, and from comparable travel-acquired UK malaria cases. Drug susceptibility in vitro and genotypes at 6 resistance-associated loci were determined for all parasite isolates and compared with clinical outcomes for each parasite donor. RESULTS: A traveler, who returned to the UK from Uganda in 2022 with Plasmodium falciparum malaria, twice failed treatment with full courses of artemether-lumefantrine. Parasites from the patient exhibited significantly reduced susceptibility to artemisinin (ring-stage survival, 17.3% [95% confidence interval {CI}, 13.6%-21.1%]; P < .0001) and lumefantrine (effective concentration preventing 50% of growth = 259.4 nM [95% CI, 130.6-388.2 nM]; P = .001). Parasite genotyping identified an allele of pfk13 encoding both the A675V variant in the Pfk13 propeller domain and a novel L145V nonpropeller variant. In vitro susceptibility testing of 6 other P. falciparum lines of Ugandan origin identified reduced susceptibility to artemisinin and lumefantrine in 1 additional line, also from a 2022 treatment failure case. These parasites did not harbor a pfk13 propeller domain variant but rather the novel nonpropeller variant T349I. Variant alleles of pfubp1, pfap2mu, and pfcoronin were also identified among the 7 parasite lines. CONCLUSIONS: We confirm, in a documented case of artemether-lumefantrine treatment failure imported from Uganda, the presence of pfk13 mutations encoding L145V and A675V. Parasites with reduced susceptibility to both artemisinin and lumefantrine may be emerging in Uganda.

Topics & Concepts

Artemether/lumefantrinePlasmodium falciparumLumefantrineArtemisininMalariaArtemetherMedicineInternal medicineGenotypingArtesunateBiologyGenotypeVirologyImmunologyGeneticsGeneMalaria Research and ControlPharmaceutical Quality and CounterfeitingHistorical Medical Research and Treatments