Malaria Journal (Mar 2020)

Amplicon deep sequencing of kelch13 in Plasmodium falciparum isolates from Senegal

  • Amy Gaye,
  • Mouhamad Sy,
  • Tolla Ndiaye,
  • Katherine J. Siddle,
  • Daniel J. Park,
  • Awa B. Deme,
  • Aminata Mbaye,
  • Baba Dieye,
  • Yaye Die Ndiaye,
  • Daniel E. Neafsey,
  • Angela Early,
  • Timothy Farrell,
  • Mamadou Samb Yade,
  • Mamadou Alpha Diallo,
  • Khadim Diongue,
  • Amy Bei,
  • Ibrahima Mbaye Ndiaye,
  • Sarah K. Volkman,
  • Aida Sadikh Badiane,
  • Daouda Ndiaye

DOI
https://doi.org/10.1186/s12936-020-03193-w
Journal volume & issue
Vol. 19, no. 1
pp. 1 – 8

Abstract

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Abstract Background In 2006, the Senegalese National Malaria Control Programme recommended artemisinin-based combination therapy (ACT) with artemether–lumefantrine as the first-line treatment for uncomplicated Plasmodium falciparum malaria. To date, multiple mutations associated with artemisinin delayed parasite clearance have been described in Southeast Asia in the Pfk13 gene, such as Y493H, R539T, I543T and C580Y. Even though ACT remains clinically and parasitologically efficacious in Senegal, the spread of resistance is possible as shown by the earlier emergence of resistance to chloroquine in Southeast Asia that subsequently spread to Africa. Therefore, surveillance of artemisinin resistance in malaria endemic regions is crucial and requires the implementation of sensitive tools, such as next-generation sequencing (NGS) which can detect novel mutations at low frequency. Methods Here, an amplicon sequencing approach was used to identify mutations in the Pfk13 gene in eighty-one P. falciparum isolates collected from three different regions of Senegal. Results In total, 10 SNPs around the propeller domain were identified; one synonymous SNP and nine non-synonymous SNPs, and two insertions. Three of these SNPs (T478T, A578S and V637I) were located in the propeller domain. A578S, is the most frequent mutation observed in Africa, but has not previously been reported in Senegal. A previous study has suggested that A578S could disrupt the function of the Pfk13 propeller region. Conclusion As the genetic basis of possible artemisinin resistance may be distinct in Africa and Southeast Asia, further studies are necessary to assess the new SNPs reported in this study.

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