Drug-Resistant Genotypes and Multi-Clonality in Plasmodium falciparum Analysed by Direct Genome Sequencing from Peripheral Blood of Malaria Patients

Naturally acquired blood-stage infections of the malaria parasite Plasmodium falciparum typically harbour multiple haploid clones. The apparent number of clones observed in any single infection depends on the diversity of the polymorphic markers used for the analysis, and the relative abundance of r...

Descripción completa

Detalles Bibliográficos
Autores principales: Robinson, Timothy, Campino, Susana G., Auburn, Sarah, Assefa, Samuel A., Polley, Spencer D., Manske, Magnus, MacInnis, Bronwyn, Rockett, Kirk A., Maslen, Gareth L., Sanders, Mandy, Quail, Michael A., Chiodini, Peter L., Kwiatkowski, Dominic P., Clark, Taane G., Sutherland, Colin J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3154926/
https://www.ncbi.nlm.nih.gov/pubmed/21853089
http://dx.doi.org/10.1371/journal.pone.0023204
_version_ 1782210056701345792
author Robinson, Timothy
Campino, Susana G.
Auburn, Sarah
Assefa, Samuel A.
Polley, Spencer D.
Manske, Magnus
MacInnis, Bronwyn
Rockett, Kirk A.
Maslen, Gareth L.
Sanders, Mandy
Quail, Michael A.
Chiodini, Peter L.
Kwiatkowski, Dominic P.
Clark, Taane G.
Sutherland, Colin J.
author_facet Robinson, Timothy
Campino, Susana G.
Auburn, Sarah
Assefa, Samuel A.
Polley, Spencer D.
Manske, Magnus
MacInnis, Bronwyn
Rockett, Kirk A.
Maslen, Gareth L.
Sanders, Mandy
Quail, Michael A.
Chiodini, Peter L.
Kwiatkowski, Dominic P.
Clark, Taane G.
Sutherland, Colin J.
author_sort Robinson, Timothy
collection PubMed
description Naturally acquired blood-stage infections of the malaria parasite Plasmodium falciparum typically harbour multiple haploid clones. The apparent number of clones observed in any single infection depends on the diversity of the polymorphic markers used for the analysis, and the relative abundance of rare clones, which frequently fail to be detected among PCR products derived from numerically dominant clones. However, minority clones are of clinical interest as they may harbour genes conferring drug resistance, leading to enhanced survival after treatment and the possibility of subsequent therapeutic failure. We deployed new generation sequencing to derive genome data for five non-propagated parasite isolates taken directly from 4 different patients treated for clinical malaria in a UK hospital. Analysis of depth of coverage and length of sequence intervals between paired reads identified both previously described and novel gene deletions and amplifications. Full-length sequence data was extracted for 6 loci considered to be under selection by antimalarial drugs, and both known and previously unknown amino acid substitutions were identified. Full mitochondrial genomes were extracted from the sequencing data for each isolate, and these are compared against a panel of polymorphic sites derived from published or unpublished but publicly available data. Finally, genome-wide analysis of clone multiplicity was performed, and the number of infecting parasite clones estimated for each isolate. Each patient harboured at least 3 clones of P. falciparum by this analysis, consistent with results obtained with conventional PCR analysis of polymorphic merozoite antigen loci. We conclude that genome sequencing of peripheral blood P. falciparum taken directly from malaria patients provides high quality data useful for drug resistance studies, genomic structural analyses and population genetics, and also robustly represents clonal multiplicity.
format Online
Article
Text
id pubmed-3154926
institution National Center for Biotechnology Information
language English
publishDate 2011
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-31549262011-08-18 Drug-Resistant Genotypes and Multi-Clonality in Plasmodium falciparum Analysed by Direct Genome Sequencing from Peripheral Blood of Malaria Patients Robinson, Timothy Campino, Susana G. Auburn, Sarah Assefa, Samuel A. Polley, Spencer D. Manske, Magnus MacInnis, Bronwyn Rockett, Kirk A. Maslen, Gareth L. Sanders, Mandy Quail, Michael A. Chiodini, Peter L. Kwiatkowski, Dominic P. Clark, Taane G. Sutherland, Colin J. PLoS One Research Article Naturally acquired blood-stage infections of the malaria parasite Plasmodium falciparum typically harbour multiple haploid clones. The apparent number of clones observed in any single infection depends on the diversity of the polymorphic markers used for the analysis, and the relative abundance of rare clones, which frequently fail to be detected among PCR products derived from numerically dominant clones. However, minority clones are of clinical interest as they may harbour genes conferring drug resistance, leading to enhanced survival after treatment and the possibility of subsequent therapeutic failure. We deployed new generation sequencing to derive genome data for five non-propagated parasite isolates taken directly from 4 different patients treated for clinical malaria in a UK hospital. Analysis of depth of coverage and length of sequence intervals between paired reads identified both previously described and novel gene deletions and amplifications. Full-length sequence data was extracted for 6 loci considered to be under selection by antimalarial drugs, and both known and previously unknown amino acid substitutions were identified. Full mitochondrial genomes were extracted from the sequencing data for each isolate, and these are compared against a panel of polymorphic sites derived from published or unpublished but publicly available data. Finally, genome-wide analysis of clone multiplicity was performed, and the number of infecting parasite clones estimated for each isolate. Each patient harboured at least 3 clones of P. falciparum by this analysis, consistent with results obtained with conventional PCR analysis of polymorphic merozoite antigen loci. We conclude that genome sequencing of peripheral blood P. falciparum taken directly from malaria patients provides high quality data useful for drug resistance studies, genomic structural analyses and population genetics, and also robustly represents clonal multiplicity. Public Library of Science 2011-08-11 /pmc/articles/PMC3154926/ /pubmed/21853089 http://dx.doi.org/10.1371/journal.pone.0023204 Text en Robinson et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Robinson, Timothy
Campino, Susana G.
Auburn, Sarah
Assefa, Samuel A.
Polley, Spencer D.
Manske, Magnus
MacInnis, Bronwyn
Rockett, Kirk A.
Maslen, Gareth L.
Sanders, Mandy
Quail, Michael A.
Chiodini, Peter L.
Kwiatkowski, Dominic P.
Clark, Taane G.
Sutherland, Colin J.
Drug-Resistant Genotypes and Multi-Clonality in Plasmodium falciparum Analysed by Direct Genome Sequencing from Peripheral Blood of Malaria Patients
title Drug-Resistant Genotypes and Multi-Clonality in Plasmodium falciparum Analysed by Direct Genome Sequencing from Peripheral Blood of Malaria Patients
title_full Drug-Resistant Genotypes and Multi-Clonality in Plasmodium falciparum Analysed by Direct Genome Sequencing from Peripheral Blood of Malaria Patients
title_fullStr Drug-Resistant Genotypes and Multi-Clonality in Plasmodium falciparum Analysed by Direct Genome Sequencing from Peripheral Blood of Malaria Patients
title_full_unstemmed Drug-Resistant Genotypes and Multi-Clonality in Plasmodium falciparum Analysed by Direct Genome Sequencing from Peripheral Blood of Malaria Patients
title_short Drug-Resistant Genotypes and Multi-Clonality in Plasmodium falciparum Analysed by Direct Genome Sequencing from Peripheral Blood of Malaria Patients
title_sort drug-resistant genotypes and multi-clonality in plasmodium falciparum analysed by direct genome sequencing from peripheral blood of malaria patients
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3154926/
https://www.ncbi.nlm.nih.gov/pubmed/21853089
http://dx.doi.org/10.1371/journal.pone.0023204
work_keys_str_mv AT robinsontimothy drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT campinosusanag drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT auburnsarah drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT assefasamuela drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT polleyspencerd drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT manskemagnus drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT macinnisbronwyn drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT rockettkirka drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT maslengarethl drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT sandersmandy drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT quailmichaela drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT chiodinipeterl drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT kwiatkowskidominicp drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT clarktaaneg drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients
AT sutherlandcolinj drugresistantgenotypesandmulticlonalityinplasmodiumfalciparumanalysedbydirectgenomesequencingfromperipheralbloodofmalariapatients

Ejemplares similares