Systematic in vitro evolution in Plasmodium falciparum reveals key determinants of drug resistance
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Godinez-Macias, Karla P
Chen, Daisy
Okombo, John
Thathy, Vandana
Cheng, Xiu
Daggupati, Sindhu
Davies, Heledd
Dhingra, Satish K
Economy, Jan M
Edgar, Rebecca CS
Gomez-Lorenzo, Maria G
Istvan, Eva S
Jado, Juan Carlos
LaMonte, Gregory M
et al.
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Abstract
Surveillance of drug resistance and the discovery of novel targets—key objectives in the fight against malaria—rely on identifying resistance-conferring mutations in Plasmodium parasites. Current approaches, while successful, require laborious experimentation or large sample sizes. To elucidate shared determinants of antimalarial resistance that can empower in silico inference, we examined the genomes of 724 Plasmodium falciparum clones, each selected in vitro for resistance to one of 118 compounds. We identified 1448 variants in 128 recurrently mutated genes, including drivers of antimalarial multidrug resistance. In contrast to naturally occurring variants, those selected in vitro are more likely to be missense or frameshift, involve bulky substitutions, and occur in conserved, ordered protein domains. Collectively, our dataset reveals mutation features that predict drug resistance in eukaryotic pathogens.
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Science
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386
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6725
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Medical microbiology
Medical physiology
Clinical sciences
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Luth, MR; Godinez-Macias, KP; Chen, D; Okombo, J; Thathy, V; Cheng, X; Daggupati, S; Davies, H; Dhingra, SK; Economy, JM; Edgar, RCS; Gomez-Lorenzo, MG; Istvan, ES; Jado, JC; LaMonte, GM; et al., Systematic in vitro evolution in Plasmodium falciparum reveals key determinants of drug resistance, Science, 2024, 386 (6725)