Recovery and stable persistence of chloroquine sensitivity in Plasmodium falciparum parasites after its discontinued use in Northern Uganda

Author:

Balikagala Betty,Sakurai-Yatsushiro Miki,Tachibana Shin-Ichiro,Ikeda Mie,Yamauchi Masato,Katuro Osbert T.,Ntege Edward H.,Sekihara Makoto,Fukuda Naoyuki,Takahashi Nobuyuki,Yatsushiro Shouki,Mori Toshiyuki,Hirai Makoto,Opio Walter,Obwoya Paul S.,Anywar Denis A.,Auma Mary A.,Palacpac Nirianne M. Q.,Tsuboi Takafumi,Odongo-Aginya Emmanuel I.,Kimura Eisaku,Ogwang Martin,Horii Toshihiro,Mita ToshihiroORCID

Abstract

Abstract Background Usage of chloroquine was discontinued from the treatment of Plasmodium falciparum infection in almost all endemic regions because of global spread of resistant parasites. Since the first report in Malawi, numerous epidemiological studies have demonstrated that the discontinuance led to re-emergence of chloroquine-susceptible P. falciparum, suggesting a possible role in future malaria control. However, most studies were cross-sectional, with few studies looking at the persistence of chloroquine recovery in long term. This study fills the gap by providing, for a period of at least 6 years, proof of persistent re-emergence/stable recovery of susceptible parasite populations using both molecular and phenotypic methods. Methods Ex vivo drug-susceptibility assays to chloroquine (n = 319) and lumefantrine (n = 335) were performed from 2013 to 2018 in Gulu, Northern Uganda, where chloroquine had been removed from the official malaria treatment regimen since 2006. Genotyping of pfcrt and pfmdr1 was also performed. Results Chloroquine resistance (≥ 100 nM) was observed in only 3 (1.3%) samples. Average IC50 values for chloroquine were persistently low throughout the study period (17.4–24.9 nM). Parasites harbouring pfcrt K76 alleles showed significantly lower IC50s to chloroquine than the parasites harbouring K76T alleles (21.4 nM vs. 43.1 nM, p-value = 3.9 × 10−8). Prevalence of K76 alleles gradually increased from 71% in 2013 to 100% in 2018. Conclusion This study found evidence of stable persistence of chloroquine susceptibility with the fixation of pfcrt K76 in Northern Uganda after discontinuation of chloroquine in the region. Accumulation of similar evidence in other endemic areas in Uganda could open channels for possible future re-use of chloroquine as an option for malaria treatment or prevention.

Funder

Japan Society for the Promotion of Science

Ministry of Health, Labour and Welfare

Japan Agency for Medical Research and Development

Global Health Innovative Technology Fund

Ministry of Education, Culture, Sports, Science and Technology

Juntendo University

Publisher

Springer Science and Business Media LLC

Subject

Infectious Diseases,Parasitology

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