Genomic analysis of Plasmodium vivax identifies putative drivers of adaptation and connectivity across diverse districts in Ethiopia

Author:

Kebede Alebachew Messele1,Sutanto Edwin2,Trimarsanto Hidayat3,Benavente Ernest Diez4,Barnes Mariana3,Pearson Richard5,Siegel Sasha5,Erko Berhanu1,Assefa Ashenafi6,Getachew Sisay7,Aseffa Abraham8,Petros Beyene1,Lo Eugenia9,Mohammed Rezika10,Yilma Daniel11,Rumaseb Angela3,Nosten Francois12,Noviyanti Rintis13,Rayner Julian14,Kwiatkowski Dominic5,Price Ric3,Golassa Lemu1,Auburn Sarah3

Affiliation:

1. Addis Ababa University

2. Exeins Health Initiative

3. Menzies School of Health Research

4. University Medical Center Utrecht

5. Wellcome Sanger Institute

6. Ethiopian Public Health Institute

7. Millipore Sigma (Bioreliance)

8. Armauer Hansen Research Institute

9. Drexel University

10. University of Gondar

11. Jimma University

12. Shoklo Malaria Research Unit

13. Eijkman Institute for Molecular Biology

14. University of Cambridge

Abstract

Abstract Ethiopia has the greatest burden of Plasmodium vivax in Africa, but little is known about the epidemiological landscape of parasites across the country. We analysed the genomic diversity of 137 P. vivax isolates collected nine Ethiopian districts from 2012-16. Signatures of selection were detected by cross-country comparisons with isolates from Thailand (n = 104) and Indonesia (n = 111), representing regions with low and high chloroquine resistance respectively. 26% (35/137) of Ethiopian infections were polyclonal, and 48.5% (17/35) of these comprised highly related clones (within-host identity-by-descent > 25%), indicating frequent co-transmission and superinfection. Parasite gene flow between districts could not be explained entirely by geographic distance, with economic and cultural factors hypothesised to have an impact on connectivity. Amplification of the duffy binding protein gene (pvdbp1) was prevalent across all districts (16%-75%). Cross-population haplotype homozygosity revealed positive selection in a region proximal to the putative chloroquine resistance transporter gene (pvcrt-o). An S25P variant in amino acid transporter 1 (pvaat1), whose homologue has recently been implicated in P. falciparum chloroquine resistance evolution, was prevalent in Ethiopia (96%) but not Thailand or Indonesia (35–53%). The genomic architecture in Ethiopia highlights circulating variants of potential public health concern in an endemic setting with evidence of stable transmission.

Publisher

Research Square Platform LLC

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