Artemisinin Partial Resistance Mutations in Zanzibar and Tanzania Suggest Regional Spread and African Origins, 2023

Sean V Connelly
Julia G Muller
Mohamed Ali
Billy E Ngasala
Wahida Hassan
Bakari Mohamed
Kyaw L Thwai
Jacob M Sadler
Jacob Marglous
Abebe A Fola
Abdallah Zacharia
Shija J Shija
Safia Mohammed
Dominick C Msolo
Hamza Said
Editruda E Peter
Melic Odas
Isaack J Rutha
Mwanaidi Nwange
Karamoko Naire
Shazia Ruybal-Pesántez
Robert Verity
Rebecca Crudale
Varun Goel
Barbara B Choloi
Anders Björkman
Jeffrey A Bailey
Jessica T Lin
Jonathan J Juliano

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Abstract

Artemisinin partial resistance, driven by Plasmodium falciparum K13 mutations, threatens malaria control. Zanzibar is vulnerable to artemisinin partial resistance spread but lacks recent molecular surveillance. We sequenced samples in Zanzibar and mainland Tanzania collected from 2022 to 2024. K13 mutations were found in 2 of 1440 participants (P441L, A675V) in Zanzibar and 6 of 3762 (R561H, P441L) in mainland Tanzania. Based on whole genome sequencing data, K13 mutations appear to be of African origin with regional spread. Frequent parasite importation appears to maintain partner drug mutation frequencies similar to the mainland, where artemether-lumefantrine selects for mutations favoring artesunate-amodiaquine sensitivity. Ongoing molecular surveillance remains essential to track these patterns.

Version published to 10.1093/infdis/jiaf431
Aug 13, 2025
Version published to 10.1101/2025.03.22.25323829 on medRxiv
Mar 23, 2025

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