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Burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles

Burkholderia pseudomallei (Bp) is the causative agent of the infectious disease melioidosis. To investigate population diversity, recombination, and horizontal gene transfer in closely related Bp isolates, we performed whole-genome sequencing (WGS) on 106 clinical, animal, and environmental strains...

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Autores principales: Nandi, Tannistha, Holden, Matthew T.G., Didelot, Xavier, Mehershahi, Kurosh, Boddey, Justin A., Beacham, Ifor, Peak, Ian, Harting, John, Baybayan, Primo, Guo, Yan, Wang, Susana, How, Lee Chee, Sim, Bernice, Essex-Lopresti, Angela, Sarkar-Tyson, Mitali, Nelson, Michelle, Smither, Sophie, Ong, Catherine, Aw, Lay Tin, Hoon, Chua Hui, Michell, Stephen, Studholme, David J., Titball, Richard, Chen, Swaine L., Parkhill, Julian, Tan, Patrick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory Press 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4317168/
https://www.ncbi.nlm.nih.gov/pubmed/25236617
http://dx.doi.org/10.1101/gr.177543.114
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author Nandi, Tannistha
Holden, Matthew T.G.
Didelot, Xavier
Mehershahi, Kurosh
Boddey, Justin A.
Beacham, Ifor
Peak, Ian
Harting, John
Baybayan, Primo
Guo, Yan
Wang, Susana
How, Lee Chee
Sim, Bernice
Essex-Lopresti, Angela
Sarkar-Tyson, Mitali
Nelson, Michelle
Smither, Sophie
Ong, Catherine
Aw, Lay Tin
Hoon, Chua Hui
Michell, Stephen
Studholme, David J.
Titball, Richard
Chen, Swaine L.
Parkhill, Julian
Tan, Patrick
author_facet Nandi, Tannistha
Holden, Matthew T.G.
Didelot, Xavier
Mehershahi, Kurosh
Boddey, Justin A.
Beacham, Ifor
Peak, Ian
Harting, John
Baybayan, Primo
Guo, Yan
Wang, Susana
How, Lee Chee
Sim, Bernice
Essex-Lopresti, Angela
Sarkar-Tyson, Mitali
Nelson, Michelle
Smither, Sophie
Ong, Catherine
Aw, Lay Tin
Hoon, Chua Hui
Michell, Stephen
Studholme, David J.
Titball, Richard
Chen, Swaine L.
Parkhill, Julian
Tan, Patrick
author_sort Nandi, Tannistha
collection PubMed
description Burkholderia pseudomallei (Bp) is the causative agent of the infectious disease melioidosis. To investigate population diversity, recombination, and horizontal gene transfer in closely related Bp isolates, we performed whole-genome sequencing (WGS) on 106 clinical, animal, and environmental strains from a restricted Asian locale. Whole-genome phylogenies resolved multiple genomic clades of Bp, largely congruent with multilocus sequence typing (MLST). We discovered widespread recombination in the Bp core genome, involving hundreds of regions associated with multiple haplotypes. Highly recombinant regions exhibited functional enrichments that may contribute to virulence. We observed clade-specific patterns of recombination and accessory gene exchange, and provide evidence that this is likely due to ongoing recombination between clade members. Reciprocally, interclade exchanges were rarely observed, suggesting mechanisms restricting gene flow between clades. Interrogation of accessory elements revealed that each clade harbored a distinct complement of restriction-modification (RM) systems, predicted to cause clade-specific patterns of DNA methylation. Using methylome sequencing, we confirmed that representative strains from separate clades indeed exhibit distinct methylation profiles. Finally, using an E. coli system, we demonstrate that Bp RM systems can inhibit uptake of non-self DNA. Our data suggest that RM systems borne on mobile elements, besides preventing foreign DNA invasion, may also contribute to limiting exchanges of genetic material between individuals of the same species. Genomic clades may thus represent functional units of genetic isolation in Bp, modulating intraspecies genetic diversity.
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spelling pubmed-43171682015-07-01 Burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles Nandi, Tannistha Holden, Matthew T.G. Didelot, Xavier Mehershahi, Kurosh Boddey, Justin A. Beacham, Ifor Peak, Ian Harting, John Baybayan, Primo Guo, Yan Wang, Susana How, Lee Chee Sim, Bernice Essex-Lopresti, Angela Sarkar-Tyson, Mitali Nelson, Michelle Smither, Sophie Ong, Catherine Aw, Lay Tin Hoon, Chua Hui Michell, Stephen Studholme, David J. Titball, Richard Chen, Swaine L. Parkhill, Julian Tan, Patrick Genome Res Research Burkholderia pseudomallei (Bp) is the causative agent of the infectious disease melioidosis. To investigate population diversity, recombination, and horizontal gene transfer in closely related Bp isolates, we performed whole-genome sequencing (WGS) on 106 clinical, animal, and environmental strains from a restricted Asian locale. Whole-genome phylogenies resolved multiple genomic clades of Bp, largely congruent with multilocus sequence typing (MLST). We discovered widespread recombination in the Bp core genome, involving hundreds of regions associated with multiple haplotypes. Highly recombinant regions exhibited functional enrichments that may contribute to virulence. We observed clade-specific patterns of recombination and accessory gene exchange, and provide evidence that this is likely due to ongoing recombination between clade members. Reciprocally, interclade exchanges were rarely observed, suggesting mechanisms restricting gene flow between clades. Interrogation of accessory elements revealed that each clade harbored a distinct complement of restriction-modification (RM) systems, predicted to cause clade-specific patterns of DNA methylation. Using methylome sequencing, we confirmed that representative strains from separate clades indeed exhibit distinct methylation profiles. Finally, using an E. coli system, we demonstrate that Bp RM systems can inhibit uptake of non-self DNA. Our data suggest that RM systems borne on mobile elements, besides preventing foreign DNA invasion, may also contribute to limiting exchanges of genetic material between individuals of the same species. Genomic clades may thus represent functional units of genetic isolation in Bp, modulating intraspecies genetic diversity. Cold Spring Harbor Laboratory Press 2015-01 /pmc/articles/PMC4317168/ /pubmed/25236617 http://dx.doi.org/10.1101/gr.177543.114 Text en © 2015 Nandi et al.; Published by Cold Spring Harbor Laboratory Press http://creativecommons.org/licenses/by-nc/4.0/ This article is distributed exclusively by Cold Spring Harbor Laboratory Press for the first six months after the full-issue publication date (see http://genome.cshlp.org/site/misc/terms.xhtml). After six months, it is available under a Creative Commons License (Attribution-NonCommercial 4.0 International), as described at http://creativecommons.org/licenses/by-nc/4.0/.
spellingShingle Research
Nandi, Tannistha
Holden, Matthew T.G.
Didelot, Xavier
Mehershahi, Kurosh
Boddey, Justin A.
Beacham, Ifor
Peak, Ian
Harting, John
Baybayan, Primo
Guo, Yan
Wang, Susana
How, Lee Chee
Sim, Bernice
Essex-Lopresti, Angela
Sarkar-Tyson, Mitali
Nelson, Michelle
Smither, Sophie
Ong, Catherine
Aw, Lay Tin
Hoon, Chua Hui
Michell, Stephen
Studholme, David J.
Titball, Richard
Chen, Swaine L.
Parkhill, Julian
Tan, Patrick
Burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles
title Burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles
title_full Burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles
title_fullStr Burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles
title_full_unstemmed Burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles
title_short Burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles
title_sort burkholderia pseudomallei sequencing identifies genomic clades with distinct recombination, accessory, and epigenetic profiles
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4317168/
https://www.ncbi.nlm.nih.gov/pubmed/25236617
http://dx.doi.org/10.1101/gr.177543.114
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