A Worldwide Map of<i>Plasmodium falciparum</i>K13-Propeller Polymorphisms

Ménard, Didier; Khim, Nimol; Beghain, Johann; Adegnika, Ayôla Akim; Alam, Mohammad Shafiul; Amodu, Olukemi K.; Rahim-Awab, Ghulam; Barnadas, Céline; Berry, Antoine; Boum, Yap; Bustos, Maria Dorina; Cao, Jun; Chen, Jun Hu; Collet, Louis; Cui, Liwang; Thakur, Garib Das; Dièye, Alioune; Djallé, Djibrine; Dorkenoo, A; Eboumbou-Moukoko, Carole E.; Espino, Fe; Fandeur, Thierry; Ferreira-da-Cruz, M. F.; Fola, Abebe A.; Fuehrer, Hans‐Peter; Hassan, Abdillahi Mohamed; Herrera, Sócrates; Hongvanthong, Bouasy; Houzé, Sandrine; Ibrahim, Maman Laminou; Jahirul-Karim, Mohammad; Jiang, Lubin; Kano, Shigeyuki; Ali-Khan, Wasif; Khanthavong, Maniphone; Kremsner, Peter G.; Lacerda, Marcus Vinícius Guimarães; Leang, Rithea; Leelawong, Mindy; Li, Mei; Lin, Khin; Mazarati, Jean Baptiste; Ménard, Sandie; Morlais, Isabelle; Mavoko, Hypolite Muhindo; Musset, Lise; Na‐Bangchang, Kesara; Nambozi, Michael; Niaré, Karamoko; Noedl, Harald; Ouédraogo, Alphonse; Pillai, Dylan R.; Pradines, Bruno; Quang-Phuc, Bui; Ramharter, Michael; Randrianarivelojosia, Milijaona; Sattabongkot, Jetsumon; Sheikh-Omar, Abdiqani; Silué, Kigbafori D.; Sirima, Sodiomon B.; Sutherland, Colin J.; Syafruddin, Din; Tahar, Rachida; Tang, Lin; Touré, Offianan André; Tshibangu-Wa-Tshibangu, Patrick; Vigan-Womas, Inès; Warsame, Marian; Wini, Lyndes; Zakeri, Sedigheh; Kim, Saorin; Eam, Rotha; Berne, Laura; Khean, Chanra; Chy, Sophy; Ken, Malen; Loch, Kaknika; Canier, Lydie; Duru, Valentine; Legrand, Eric; Barale, Jean-Christophe; Stokes, Barbara H.; Straimer, Judith; Witkowski, Benoît; Fidock, David A.; Rogier, Christophe; Ringwald, Pascal; Ariey, Frédéric; Mercereau‐Puijalon, Odile

doi:10.1056/nejmoa1513137

Cited by 467 publications

(611 citation statements)

References 57 publications

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“…The predominant polymorphisms previously reported in Senegal are alleles K189T and K189N, outside the propeller domain (25,26), consistent with our own findings (Table S1). The mutant allele A578S, which is not associated with artemisinin resistance, has been reported in multiple regions in Africa (18,19,24,28) (Table S2). In comparison, we observed a different amino acid substitution at this codon position in a single sample, from alanine (A) to aspartic acid (D) (Table S2).…”

Section: Discussionmentioning

confidence: 99%

Molecular Epidemiology of Plasmodium falciparum kelch13 Mutations in Senegal Determined by Using Targeted Amplicon Deep Sequencing

Talundzic

Ndiaye

Déme

et al. 2017

Antimicrob Agents Chemother

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The emergence of Plasmodium falciparum resistance to artemisinin in Southeast Asia threatens malaria control and elimination activities worldwide. Multiple polymorphisms in the P. falciparum kelch gene found in chromosome 13 (Pfk13) have been associated with artemisinin resistance. Surveillance of potential drug resistance loci within a population that may emerge under increasing drug pressure is an important public health activity. In this context, P. falciparum infections from an observational surveillance study in Senegal were genotyped using targeted amplicon deep sequencing (TADS) for Pfk13 polymorphisms. The results were compared to previously reported Pfk13 polymorphisms from around the world. A total of 22 Pfk13 propeller domain polymorphisms were identified in this study, of which 12 have previously not been reported. Interestingly, of the 10 polymorphisms identified in the present study that were also previously reported, all had a different amino acid substitution at these codon positions. Most of the polymorphisms were present at low frequencies and were confined to single isolates, suggesting they are likely transient polymorphisms that are part of naturally evolving parasite populations. The results of this study underscore the need to identify potential drug resistance loci existing within a population, which may emerge under increasing drug pressure.

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Section: Discussionmentioning

confidence: 99%

Molecular Epidemiology of Plasmodium falciparum kelch13 Mutations in Senegal Determined by Using Targeted Amplicon Deep Sequencing

Talundzic

Ndiaye

Déme

et al. 2017

Antimicrob Agents Chemother

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“…A worldwide map of P. falciparum K13-propeller polymorphism was recently published from a study involving 41 partner institutions and 14,037 samples collected from 163 sites (in 59 countries in which malaria is endemic), providing a global overview of the distribution of artemisinin resistance and fundamental data for drug policy makers and future surveillance activities. 59 The main findings of the KARMA study (K13 Artemisinin Resistance Multicenter Assessment) suggest that artemisinin resistance remains confined to southeast Asia (including Cambodia, PDR of Laos, Thailand, Vietnam, and Myanmar) and China. In these two regions, the proportions of parasites with K13 mutations were estimated at 51.8% (95% CI: 48.5-55.3%) and 25.6% (95% CI: 19.3-33.3%), respectively.…”

Section: Resistance To Artemisinin Derivatives: Past and Present Resementioning

confidence: 99%

Plasmodium falciparum Resistance to Artemisinin Derivatives and Piperaquine: A Major Challenge for Malaria Elimination in Cambodia

Duru

Witkowski

Ménard

2016

The American Journal of Tropical Medicine and Hygiene

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Abstract. Artemisinin-based combination therapies (ACTs) are the cornerstone of current strategies for fighting malaria. Over the last decade, ACTs have played a major role in decreasing malaria burden. However, this progress is being jeopardized by the emergence of artemisinin-resistant Plasmodium falciparum parasites. Artemisinin resistance was first detected in western Cambodia in 2008 and has since been observed in neighboring countries in southeast Asia. The problem of antimalarial drug resistance has recently worsened in Cambodia, with reports of parasites resistant to piperaquine, the latest generation of partner drug used in combination with dihydroartemisinin, leading to worrying rates of clinical treatment failure. The monitoring and the comprehension of both types of resistance are crucial to prevent the spread of multidrug-resistant parasites outside southeast Asia, and particularly to Africa, where the public health consequences would be catastrophic. To this end, new tools are required for studying the biological and molecular mechanisms underlying resistance to antimalarial drugs and for monitoring the geographic distribution of the resistant parasites. In this review, we detail the major advances in our understanding of resistance to artemisinin and piperaquine and define the challenges that the malaria community will have to face in the coming years. BACKGROUND

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“…Pfk13 was one of a few loci in the genome of the cultureadapted Tanzanian P. falciparum isolate F32 that, during this extensive selection process, had accumulated mutations in concert with decreasing DHA susceptibility as measured by the RSA. Alone among these few loci, mutations in pfk13 were also found to correlate with ex vivo DHA susceptibility of Cambodian parasites in the RSA, although the exact mutation identified in mutant F32 parasites has still not been encountered in any wild P. falciparum isolates to date [9]. The identification of key variants of pfk13 that correlate both with slow clearance in patients receiving artesunate monotherapy [3] and with ex vivo RSA data [6] has enabled subsequent research on pfk13.…”

Section: A New Artemisinin Susceptibility Phenotype Arises In Asiamentioning

confidence: 99%

“…• studies of the distribution of polymorphisms in the field, particularly in Africa [9][10][11][12][13];…”

Section: A New Artemisinin Susceptibility Phenotype Arises In Asiamentioning

confidence: 99%

Genetic markers of artemisinin resistance in Plasmodium spp. parasites

Sutherland

2017

Emerging Topics in Life Sciences

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The vast majority of malaria patients worldwide are currently treated with combination therapy comprising one of the artemisinin family of drugs, characterised by rapid action and short plasma half-life, co-formulated with a longer-lasting drug from the amino arylalcohol or quinoline families. There is now a widely perceived threat to treatment efficacy, as reduced susceptibility to rapid artemisinin clearance in vivo has become prevalent among populations of Plasmodium falciparum in the Greater Mekong subregion since 2008. In vitro and in vivo drug selection studies, heterologous cell expression experiments and genetic epidemiology have identified many candidate markers of reduced ring-stage susceptibility to artemisinin. Certain variants of the P. falciparum pfk13 gene, which encodes a kelch domain protein implicated in the unfolded protein response, are strongly associated with slow parasite clearance by artemisinin in the Mekong subregion. However, anomalies in the epidemiological association of pfk13 variants with true treatment failure in vivo and the curious cell-cycle stage specificity of this phenotype in vitro warrant exploration in some depth. Taken together, available data suggest that the emergence of P. falciparum expressing K13 variants has not yet precipitated a public health emergency. Alternative candidate markers of artemisinin susceptibility are also described, as K13-independent treatment failure has been observed in African P. falciparum and in the rodent malaria parasite Plasmodium chabaudi.

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A Worldwide Map ofPlasmodium falciparumK13-Propeller Polymorphisms

Cited by 467 publications

References 57 publications

Molecular Epidemiology of Plasmodium falciparum kelch13 Mutations in Senegal Determined by Using Targeted Amplicon Deep Sequencing

Molecular Epidemiology of Plasmodium falciparum kelch13 Mutations in Senegal Determined by Using Targeted Amplicon Deep Sequencing

Plasmodium falciparum Resistance to Artemisinin Derivatives and Piperaquine: A Major Challenge for Malaria Elimination in Cambodia

Genetic markers of artemisinin resistance in Plasmodium spp. parasites

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