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Genome-wide screen identifies new candidate genes associated with artemisinin susceptibility in Plasmodium falciparum in Kenya

Abstract:
Early identification of causal genetic variants underlying antimalarial drug resistance could provide robust epidemiological tools for timely public health interventions. Using a novel natural genetics strategy for mapping novel candidate genes we analyzed >75,000 high quality single nucleotide polymorphisms selected from high-resolution whole-genome sequencing data in 27 isolates of Plasmodium falciparum. We identified genetic variants associated with susceptibility to dihydroartemisinin that implicate one region on chromosome 13, a candidate gene on chromosome 1 (PFA0220w, a UBP1 ortholog) and others (PFB0560w, PFB0630c, PFF0445w) with putative roles in protein homeostasis and stress response. There was a strong signal for positive selection on PFA0220w, but not the other candidate loci. Our results demonstrate the power of full-genome sequencing-based association studies for uncovering candidate genes that determine parasite sensitivity to artemisinins. Our study provides a unique reference for the interpretation of results from resistant infections.
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1038/srep03318

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Publisher:
Springer Nature
Journal:
Scientific Reports More from this journal
Volume:
3
Article number:
3318
Publication date:
2013-11-25
Acceptance date:
2013-10-21
DOI:
EISSN:
2045-2322


Language:
English
Keywords:
UUID:
uuid:841d7598-6aa1-4cfd-b74c-d8a742128e0a
Local pid:
pubs:440310
Source identifiers:
440310
Deposit date:
2013-12-11

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