Resolving drug selection and migration in an inbred South American <i>Plasmodium falciparum</i> population with identity-by-descent analysis-Reference-Cited by-同舟云学术

Resolving drug selection and migration in an inbred South American Plasmodium falciparum population with identity-by-descent analysis

Published:2022-02-19 Issue: Volume: Page:
ISSN:
Container-title:
language:
Short-container-title:

Author:

Carrasquilla Manuela^ORCID,Early Angela M^ORCID,Taylor Aimee R^ORCID,Knudson Angélica,Echeverry Diego F,Anderson Timothy JC^ORCID,Mancilla Elvira,Aponte Samanda,Cárdenas Pablo,Buckee Caroline O^ORCID,Rayner Julian C^ORCID,Sáenz Fabián E,Neafsey Daniel E^ORCID,Corredor Vladimir

Abstract

AbstractThe human malaria parasite Plasmodium falciparum is globally widespread, but its prevalence varies significantly between and even within countries. Most population genetic studies in P. falciparum focus on regions of high transmission where parasite populations are large and genetically diverse, such as sub-Saharan Africa. Understanding population dynamics in low transmission settings, however, is of particular importance as these are often where drug resistance first evolves. Here, we use the Pacific Coast of Colombia and Ecuador as a model for understanding the population structure and evolution of Plasmodium parasites in small populations harboring low genetic diversity. The combination of low transmission and a high proportion of monoclonal infections means there are few outcrossing events and clonal lineages persist for long periods of time. Yet despite this, the population is evolutionarily labile and has successfully adapted to multiple drug regimes. Using 166 newly sequenced whole genomes, we measure relatedness between parasites, calculated as identity by descent (IBD), and find 17 distinct but highly related clonal lineages, six of which have persisted in the region for at least a decade. This inbred population structure is captured in more detail with IBD than with other common population structure analyses like PCA, ADMIXTURE, and distance-based trees. We additionally use patterns of intra-chromosomal IBD and an analysis of haplotypic variation to explore the role of recombination in spreading drug resistance mutations throughout the region. Two genes associated with chloroquine resistance, crt and aat1, show evidence of hard selective sweeps, while selection appears soft and/or incomplete at three other key resistance loci (dhps, mdr1, and dhfr). Overall, this work highlights the strength of IBD analyses for studying parasite population structure and resistance evolution in regions of low transmission, and emphasizes that drug resistance can evolve and spread in extremely small populations, as will occur in any region nearing malaria elimination.

Publisher

Cold Spring Harbor Laboratory

Reference81 articles.

1. World Health Organization. World Malaria Report 2021 (2021).

2. Recht, J. et al. Malaria in Brazil, Colombia, Peru and Venezuela: current challenges in malaria control and elimination. Malar. J. 16, 273 (2017).

3. PAHO. Situation of Malaria in the Region of the Americas. (2017).

4. Feged-Rivadeneira, A. et al. Malaria intensity in Colombia by regions and populations. PLoS One 13, e0203673 (2018).

5. Douine, M. et al. Prevalence of Plasmodium spp. in illegal gold miners in French Guiana in 2015: a hidden but critical malaria reservoir. Malar. J. 15, 315 (2016).

Cited by 4 articles. 订阅此论文施引文献订阅此论文施引文献，注册后可以免费订阅5篇论文的施引文献，订阅后可以查看论文全部施引文献

1. Systematic bias in malaria parasite relatedness estimation;2024-04-20

2. Taking identity-by-descent analysis into the wild: Estimating realized relatedness in free-ranging macaques;2024-01-11

3. An amino acid transporter AAT1 plays a pivotal role in chloroquine resistance evolution in malaria parasites;2022-05-26

4. Design and implementation of multiplexed amplicon sequencing panels to serve genomic epidemiology of infectious disease: A malaria case study;Molecular Ecology Resources;2022-05-03