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Historical trends and new surveillance of Plasmodium falciparum drug resistance markers in Angola

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posted on 2023-10-05, 09:46 authored by Emily R Ebel, Fatima Reis, Dmitri A Petrov, Sandra Beleza
Background: Plasmodium falciparum resistance to chloroquine (CQ) and sulfadoxine-pyrimethamine (SP) has historically posed a major threat to malaria control throughout the world. The country of Angola officially replaced CQ with artemisinin-based combination therapy (ACT) as a first-line treatment in 2006, but malaria cases and deaths have recently been rising. Many classic resistance mutations are relevant for the efficacy of currently available drugs, making it important to continue monitoring their frequency in Angola. Methods: Plasmodium falciparum DNA was sampled from the blood of 50 hospital patients in Cabinda, Angola from October-December of 2018. Each infection was genotyped for 13 alleles in the genes crt, mdr1, dhps, dhfr, and kelch13, which are collectively involved in resistance to six common anti-malarials. To compare frequency patterns over time, P. falciparum genotype data were also collated from studies published from across Angola in the last two decades. Results: The two most important alleles for CQ resistance, crt 76T and mdr1 86Y, were found at respective frequencies of 71.4% and 6.5%. Historical data suggest that mdr1 N86 has been steadily replacing 86Y throughout Angola in the last decade, while the frequency of crt 76T has been more variable across studies. Over a third of new samples from Cabinda were ‘quintuple mutants’ for SP resistance in dhfr/dhps, with a sixth mutation at dhps A581G present at 9.6% frequency. The markers dhfr 51I, dhfr 108N, and dhps 437G have been nearly fixed in Angola since the early 2000s, whereas dhfr 59R may have risen to high frequency more recently. Finally, no non-synonymous polymorphisms were detected in kelch13, which is involved in artemisinin resistance in Southeast Asia. Conclusions: Genetic markers of P. falciparum resistance to CQ are likely declining in frequency in Angola, consistent with the official discontinuation of CQ in 2006. The high frequency of multiple genetic markers of SP resistance is consistent with the continued public and private use of SP. In the future, more complete haplotype data from mdr1, dhfr, and dhps will be critical for understanding the changing efficacy of multiple anti-malarial drugs. These data can be used to support effective drug policy decisions in Angola.

Funding

This study was supported with grants from the Stanford Center for Computational, Evolutionary, and Human Genomics to S.B. and E.R.E.; an MRC award (MR/M01987X/1) to S.B.; and an NIH award (5R35GM118165-05) to D.A.P.

History

Citation

Malaria Journal volume 20, Article number: 175 (2021)

Author affiliation

Department of Genetics and Genome Biology

Version

  • VoR (Version of Record)

Published in

Malaria Journal

Volume

20

Publisher

BioMed Central

issn

1475-2875

eissn

1475-2875

Acceptance date

2021-03-25

Copyright date

2021

Available date

2023-10-05

Spatial coverage

England

Language

English

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