PHARE: a bioinformatics pipeline for compositional profiling of multiclonal Plasmodium falciparum infections from long-read Nanopore sequencing data

Author:

Hosch Salome12ORCID,Wagner Philipp12ORCID,Giger Johanna Nouria12,Dubach Nina12,Saavedra Elis12,Perno Carlo Federico3,Gody Jean-Chrysostome4,Pagonendji Marilou Sonia5,Ngoagouni Carine6,Ndoua Christophe7,Nsanzabana Christian12ORCID,Vickos Ulrich3,Daubenberger Claudia12,Schindler Tobias12

Affiliation:

1. University of Basel , Petersplatz 1, 4001 Basel , Switzerland

2. Department of Medical Parasitology and Infection Biology, Swiss Tropical and Public Health Institute , Kreuzstrasse 2, 4123 Allschwil , Switzerland

3. Department of Microbiology, Ospedale Pediatrico Bambino Gesù , Piazza di Sant’Onofrio, 4, 00165 Roma , Italy

4. Department of Intensive Care, Pediatric University Hospital Centre of Bangui , Bangui , Central African Republic

5. Laboratory of Parasitology, Institut Pasteur of Bangui , Bangui , Central African Republic

6. Medical Entomology Unit, Institut Pasteur of Bangui , Bangui , Central African Republic

7. National Malaria Control Program, Ministry of Health , Bangui , Central African Republic

Abstract

Abstract Background The emergence of drug-resistant clones of Plasmodium falciparum is a major public health concern, and the ability to detect and track the spread of these clones is crucial for effective malaria control and treatment. However, in endemic settings, malaria infected people often carry multiple P. falciparum clones simultaneously making it likely to miss drug-resistant clones using traditional molecular typing methods. Objectives Our goal was to develop a bioinformatics pipeline for compositional profiling in multiclonal P. falciparum samples, sequenced using the Oxford Nanopore Technologies MinION platform. Methods We developed the ‘Finding P. falciparum haplotypes with resistance mutations in polyclonal infections’ (PHARE) pipeline using existing bioinformatics tools and custom scripts written in python. PHARE was validated on three control datasets containing P. falciparum DNA of four laboratory strains at varying mixing ratios. Additionally, the pipeline was tested on clinical samples from children admitted to a paediatric hospital in the Central African Republic. Results The PHARE pipeline achieved high recall and accuracy rates in all control datasets. The pipeline can be used on any gene and was tested with amplicons of the P. falciparum drug resistance marker genes pfdhps, pfdhfr and pfK13. Conclusions The PHARE pipeline helps to provide a more complete picture of drug resistance in the circulating P. falciparum population and can help to guide treatment recommendations. PHARE is freely available under the GNU Lesser General Public License v.3.0 on GitHub: https://github.com/Fippu/PHARE.

Funder

Bioko Island Malaria Elimination Project

Government of Equatorial Guinea

Marathon EG Production Limited

Noble Energy

Atlantic Methanol Production Company

Publisher

Oxford University Press (OUP)

Reference44 articles.

1. Artemisinin-based combination therapy for treating uncomplicated malaria;Sinclair;Cochrane Database Syst Rev,2009

2. Association of Plasmodium falciparum kelch13 R561H genotypes with delayed parasite clearance in Rwanda: an open-label, single-arm, multicentre, therapeutic efficacy study;Uwimana;Lancet Infect Dis,2021

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