Novel highly-multiplexed AmpliSeq targeted assay for Plasmodium vivax genetic surveillance use cases at multiple geographical scales

Although the power of genetic surveillance tools has been acknowledged widely, there is an urgent need in malaria endemic countries for feasible and cost-effective tools to implement in national malaria control programs (NMCPs) that can generate evidence to guide malaria control and elimination stra...

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Autores principales: Kattenberg, Johanna Helena, Nguyen, Hong Van, Nguyen, Hieu Luong, Sauve, Erin, Nguyen, Ngoc Thi Hong, Chopo-Pizarro, Ana, Trimarsanto, Hidayat, Monsieurs, Pieter, Guetens, Pieter, Nguyen, Xa Xuan, Esbroeck, Marjan Van, Auburn, Sarah, Nguyen, Binh Thi Huong, Rosanas-Urgell, Anna
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Cellular and Infection Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9403277/
https://www.ncbi.nlm.nih.gov/pubmed/36034708
http://dx.doi.org/10.3389/fcimb.2022.953187
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author Kattenberg, Johanna Helena
Nguyen, Hong Van
Nguyen, Hieu Luong
Sauve, Erin
Nguyen, Ngoc Thi Hong
Chopo-Pizarro, Ana
Trimarsanto, Hidayat
Monsieurs, Pieter
Guetens, Pieter
Nguyen, Xa Xuan
Esbroeck, Marjan Van
Auburn, Sarah
Nguyen, Binh Thi Huong
Rosanas-Urgell, Anna
author_facet Kattenberg, Johanna Helena
Nguyen, Hong Van
Nguyen, Hieu Luong
Sauve, Erin
Nguyen, Ngoc Thi Hong
Chopo-Pizarro, Ana
Trimarsanto, Hidayat
Monsieurs, Pieter
Guetens, Pieter
Nguyen, Xa Xuan
Esbroeck, Marjan Van
Auburn, Sarah
Nguyen, Binh Thi Huong
Rosanas-Urgell, Anna
author_sort Kattenberg, Johanna Helena
collection PubMed
description Although the power of genetic surveillance tools has been acknowledged widely, there is an urgent need in malaria endemic countries for feasible and cost-effective tools to implement in national malaria control programs (NMCPs) that can generate evidence to guide malaria control and elimination strategies, especially in the case of Plasmodium vivax. Several genetic surveillance applications (‘use cases’) have been identified to align research, technology development, and public health efforts, requiring different types of molecular markers. Here we present a new highly-multiplexed deep sequencing assay (Pv AmpliSeq). The assay targets the 33-SNP vivaxGEN-geo panel for country-level classification, and a newly designed 42-SNP within-country barcode for analysis of parasite dynamics in Vietnam and 11 putative drug resistance genes in a highly multiplexed NGS protocol with easy workflow, applicable for many different genetic surveillance use cases. The Pv AmpliSeq assay was validated using: 1) isolates from travelers and migrants in Belgium, and 2) routine collections of the national malaria control program at sentinel sites in Vietnam. The assay targets 229 amplicons and achieved a high depth of coverage (mean 595.7 ± 481) and high accuracy (mean error-rate of 0.013 ± 0.007). P. vivax parasites could be characterized from dried blood spots with a minimum of 5 parasites/µL and 10% of minority-clones. The assay achieved good spatial specificity for between-country prediction of origin using the 33-SNP vivaxGEN-geo panel that targets rare alleles specific for certain countries and regions. A high resolution for within-country diversity in Vietnam was achieved using the designed 42-SNP within-country barcode that targets common alleles (median MAF 0.34, range 0.01-0.49. Many variants were detected in (putative) drug resistance genes, with different predominant haplotypes in the pvmdr1 and pvcrt genes in different provinces in Vietnam. The capacity of the assay for high resolution identity-by-descent (IBD) analysis was demonstrated and identified a high rate of shared ancestry within Gia Lai Province in the Central Highlands of Vietnam, as well as between the coastal province of Binh Thuan and Lam Dong. Our approach performed well in geographically differentiating isolates at multiple spatial scales, detecting variants in putative resistance genes, and can be easily adjusted to suit the needs in other settings in a country or region. We prioritize making this tool available to researchers and NMCPs in endemic countries to increase ownership and ensure data usage for decision-making and malaria policy.
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spelling pubmed-94032772022-08-26 Novel highly-multiplexed AmpliSeq targeted assay for Plasmodium vivax genetic surveillance use cases at multiple geographical scales Kattenberg, Johanna Helena Nguyen, Hong Van Nguyen, Hieu Luong Sauve, Erin Nguyen, Ngoc Thi Hong Chopo-Pizarro, Ana Trimarsanto, Hidayat Monsieurs, Pieter Guetens, Pieter Nguyen, Xa Xuan Esbroeck, Marjan Van Auburn, Sarah Nguyen, Binh Thi Huong Rosanas-Urgell, Anna Front Cell Infect Microbiol Cellular and Infection Microbiology Although the power of genetic surveillance tools has been acknowledged widely, there is an urgent need in malaria endemic countries for feasible and cost-effective tools to implement in national malaria control programs (NMCPs) that can generate evidence to guide malaria control and elimination strategies, especially in the case of Plasmodium vivax. Several genetic surveillance applications (‘use cases’) have been identified to align research, technology development, and public health efforts, requiring different types of molecular markers. Here we present a new highly-multiplexed deep sequencing assay (Pv AmpliSeq). The assay targets the 33-SNP vivaxGEN-geo panel for country-level classification, and a newly designed 42-SNP within-country barcode for analysis of parasite dynamics in Vietnam and 11 putative drug resistance genes in a highly multiplexed NGS protocol with easy workflow, applicable for many different genetic surveillance use cases. The Pv AmpliSeq assay was validated using: 1) isolates from travelers and migrants in Belgium, and 2) routine collections of the national malaria control program at sentinel sites in Vietnam. The assay targets 229 amplicons and achieved a high depth of coverage (mean 595.7 ± 481) and high accuracy (mean error-rate of 0.013 ± 0.007). P. vivax parasites could be characterized from dried blood spots with a minimum of 5 parasites/µL and 10% of minority-clones. The assay achieved good spatial specificity for between-country prediction of origin using the 33-SNP vivaxGEN-geo panel that targets rare alleles specific for certain countries and regions. A high resolution for within-country diversity in Vietnam was achieved using the designed 42-SNP within-country barcode that targets common alleles (median MAF 0.34, range 0.01-0.49. Many variants were detected in (putative) drug resistance genes, with different predominant haplotypes in the pvmdr1 and pvcrt genes in different provinces in Vietnam. The capacity of the assay for high resolution identity-by-descent (IBD) analysis was demonstrated and identified a high rate of shared ancestry within Gia Lai Province in the Central Highlands of Vietnam, as well as between the coastal province of Binh Thuan and Lam Dong. Our approach performed well in geographically differentiating isolates at multiple spatial scales, detecting variants in putative resistance genes, and can be easily adjusted to suit the needs in other settings in a country or region. We prioritize making this tool available to researchers and NMCPs in endemic countries to increase ownership and ensure data usage for decision-making and malaria policy. Frontiers Media S.A. 2022-08-11 /pmc/articles/PMC9403277/ /pubmed/36034708 http://dx.doi.org/10.3389/fcimb.2022.953187 Text en Copyright © 2022 Kattenberg, Nguyen, Nguyen, Sauve, Nguyen, Chopo-Pizarro, Trimarsanto, Monsieurs, Guetens, Nguyen, Esbroeck, Auburn, Nguyen and Rosanas-Urgell https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Cellular and Infection Microbiology
Kattenberg, Johanna Helena
Nguyen, Hong Van
Nguyen, Hieu Luong
Sauve, Erin
Nguyen, Ngoc Thi Hong
Chopo-Pizarro, Ana
Trimarsanto, Hidayat
Monsieurs, Pieter
Guetens, Pieter
Nguyen, Xa Xuan
Esbroeck, Marjan Van
Auburn, Sarah
Nguyen, Binh Thi Huong
Rosanas-Urgell, Anna
Novel highly-multiplexed AmpliSeq targeted assay for Plasmodium vivax genetic surveillance use cases at multiple geographical scales
title Novel highly-multiplexed AmpliSeq targeted assay for Plasmodium vivax genetic surveillance use cases at multiple geographical scales
title_full Novel highly-multiplexed AmpliSeq targeted assay for Plasmodium vivax genetic surveillance use cases at multiple geographical scales
title_fullStr Novel highly-multiplexed AmpliSeq targeted assay for Plasmodium vivax genetic surveillance use cases at multiple geographical scales
title_full_unstemmed Novel highly-multiplexed AmpliSeq targeted assay for Plasmodium vivax genetic surveillance use cases at multiple geographical scales
title_short Novel highly-multiplexed AmpliSeq targeted assay for Plasmodium vivax genetic surveillance use cases at multiple geographical scales
title_sort novel highly-multiplexed ampliseq targeted assay for plasmodium vivax genetic surveillance use cases at multiple geographical scales
topic Cellular and Infection Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9403277/
https://www.ncbi.nlm.nih.gov/pubmed/36034708
http://dx.doi.org/10.3389/fcimb.2022.953187
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