Plasmodium falciparum resistant to artemisinin and diagnostics have emerged in Ethiopia

Author:

Fola Abebe A.ORCID,Feleke Sindew M.ORCID,Mohammed HusseinORCID,Brhane Bokretsion G.,Hennelly Christopher M.,Assefa AshenafiORCID,Crudal Rebecca M.ORCID,Reichert Emily,Juliano Jonathan J.ORCID,Cunningham Jane,Mamo HassenORCID,Solomon Hiwot,Tasew Geremew,Petros Beyene,Parr Jonathan B.ORCID,Bailey Jeffrey A.ORCID

Abstract

AbstractDiagnosis and treatment of Plasmodium falciparum infections are required for effective malaria control and are pre-requisites for malaria elimination efforts; hence we need to monitor emergence, evolution and spread of drug- and diagnostics-resistant parasites. We deep sequenced key drug-resistance mutations and 1,832 SNPs in the parasite genomes of 609 malaria cases collected during a diagnostic-resistance surveillance study in Ethiopia. We found that 8.0% (95% CI 7.0–9.0) of malaria cases were caused by P. falciparum carrying the candidate artemisinin partial-resistance kelch13 (K13) 622I mutation, which was less common in diagnostic-resistant parasites mediated by histidine-rich proteins 2 and 3 (pfhrp2/3) deletions than in wild-type parasites (P = 0.03). Identity-by-descent analyses showed that K13 622I parasites were significantly more related to each other than to wild type (P < 0.001), consistent with recent expansion and spread of this mutation. Pfhrp2/3-deleted parasites were also highly related, with evidence of clonal transmissions at the district level. Of concern, 8.2% of K13 622I parasites also carried the pfhrp2/3 deletions. Close monitoring of the spread of combined drug- and diagnostic-resistant parasites is needed.

Publisher

Springer Science and Business Media LLC

Subject

Cell Biology,Microbiology (medical),Genetics,Applied Microbiology and Biotechnology,Immunology,Microbiology

Reference53 articles.

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