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Escherichia coli Sequence Type 410 Is Causing New International High-Risk Clones

Escherichia coli sequence type 410 (ST410) has been reported worldwide as an extraintestinal pathogen associated with resistance to fluoroquinolones, third-generation cephalosporins, and carbapenems. In the present study, we investigated national epidemiology of ST410 E. coli isolates from Danish pa...

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Autores principales: Roer, Louise, Overballe-Petersen, Søren, Hansen, Frank, Schønning, Kristian, Wang, Mikala, Røder, Bent L., Hansen, Dennis S., Justesen, Ulrik S., Andersen, Leif P., Fulgsang-Damgaard, David, Hopkins, Katie L., Woodford, Neil, Falgenhauer, Linda, Chakraborty, Trinad, Samuelsen, Ørjan, Sjöström, Karin, Johannesen, Thor B., Ng, Kim, Nielsen, Jens, Ethelberg, Steen, Stegger, Marc, Hammerum, Anette M., Hasman, Henrik
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6052333/
https://www.ncbi.nlm.nih.gov/pubmed/30021879
http://dx.doi.org/10.1128/mSphere.00337-18
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author Roer, Louise
Overballe-Petersen, Søren
Hansen, Frank
Schønning, Kristian
Wang, Mikala
Røder, Bent L.
Hansen, Dennis S.
Justesen, Ulrik S.
Andersen, Leif P.
Fulgsang-Damgaard, David
Hopkins, Katie L.
Woodford, Neil
Falgenhauer, Linda
Chakraborty, Trinad
Samuelsen, Ørjan
Sjöström, Karin
Johannesen, Thor B.
Ng, Kim
Nielsen, Jens
Ethelberg, Steen
Stegger, Marc
Hammerum, Anette M.
Hasman, Henrik
author_facet Roer, Louise
Overballe-Petersen, Søren
Hansen, Frank
Schønning, Kristian
Wang, Mikala
Røder, Bent L.
Hansen, Dennis S.
Justesen, Ulrik S.
Andersen, Leif P.
Fulgsang-Damgaard, David
Hopkins, Katie L.
Woodford, Neil
Falgenhauer, Linda
Chakraborty, Trinad
Samuelsen, Ørjan
Sjöström, Karin
Johannesen, Thor B.
Ng, Kim
Nielsen, Jens
Ethelberg, Steen
Stegger, Marc
Hammerum, Anette M.
Hasman, Henrik
author_sort Roer, Louise
collection PubMed
description Escherichia coli sequence type 410 (ST410) has been reported worldwide as an extraintestinal pathogen associated with resistance to fluoroquinolones, third-generation cephalosporins, and carbapenems. In the present study, we investigated national epidemiology of ST410 E. coli isolates from Danish patients. Furthermore, E. coli ST410 was investigated in a global context to provide further insight into the acquisition of the carbapenemase genes bla(OXA-181) and bla(NDM-5) of this successful lineage. From 127 whole-genome-sequenced isolates, we reconstructed an evolutionary framework of E. coli ST410 which portrays the antimicrobial-resistant clades B2/H24R, B3/H24Rx, and B4/H24RxC. The B2/H24R and B3/H24Rx clades emerged around 1987, concurrently with the C1/H30R and C2/H30Rx clades in E. coli ST131. B3/H24Rx appears to have evolved by the acquisition of the extended-spectrum β-lactamase (ESBL)-encoding gene bla(CTX-M-15) and an IncFII plasmid, encoding IncFIA and IncFIB. Around 2003, the carbapenem-resistant clade B4/H24RxC emerged when ST410 acquired an IncX3 plasmid carrying a bla(OXA-181) carbapenemase gene. Around 2014, the clade B4/H24RxC acquired a second carbapenemase gene, bla(NDM-5), on a conserved IncFII plasmid. From an epidemiological investigation of 49 E. coli ST410 isolates from Danish patients, we identified five possible regional outbreaks, of which one outbreak involved nine patients with bla(OXA-181)- and bla(NDM-5)-carrying B4/H24RxC isolates. The accumulated multidrug resistance in E. coli ST410 over the past two decades, together with its proven potential of transmission between patients, poses a high risk in clinical settings, and thus, E. coli ST410 should be considered a lineage with emerging “high-risk” clones, which should be monitored closely in the future. IMPORTANCE Extraintestinal pathogenic Escherichia coli (ExPEC) is the main cause of urinary tract infections and septicemia. Significant attention has been given to the ExPEC sequence type ST131, which has been categorized as a “high-risk” clone. High-risk clones are globally distributed clones associated with various antimicrobial resistance determinants, ease of transmission, persistence in hosts, and effective transmission between hosts. The high-risk clones have enhanced pathogenicity and cause severe and/or recurrent infections. We show that clones of the E. coli ST410 lineage persist and/or cause recurrent infections in humans, including bloodstream infections. We found evidence of ST410 being a highly resistant globally distributed lineage, capable of patient-to-patient transmission causing hospital outbreaks. Our analysis suggests that the ST410 lineage should be classified with the potential to cause new high-risk clones. Thus, with the clonal expansion over the past decades and increased antimicrobial resistance to last-resort treatment options, ST410 needs to be monitored prospectively.
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spelling pubmed-60523332018-07-27 Escherichia coli Sequence Type 410 Is Causing New International High-Risk Clones Roer, Louise Overballe-Petersen, Søren Hansen, Frank Schønning, Kristian Wang, Mikala Røder, Bent L. Hansen, Dennis S. Justesen, Ulrik S. Andersen, Leif P. Fulgsang-Damgaard, David Hopkins, Katie L. Woodford, Neil Falgenhauer, Linda Chakraborty, Trinad Samuelsen, Ørjan Sjöström, Karin Johannesen, Thor B. Ng, Kim Nielsen, Jens Ethelberg, Steen Stegger, Marc Hammerum, Anette M. Hasman, Henrik mSphere Research Article Escherichia coli sequence type 410 (ST410) has been reported worldwide as an extraintestinal pathogen associated with resistance to fluoroquinolones, third-generation cephalosporins, and carbapenems. In the present study, we investigated national epidemiology of ST410 E. coli isolates from Danish patients. Furthermore, E. coli ST410 was investigated in a global context to provide further insight into the acquisition of the carbapenemase genes bla(OXA-181) and bla(NDM-5) of this successful lineage. From 127 whole-genome-sequenced isolates, we reconstructed an evolutionary framework of E. coli ST410 which portrays the antimicrobial-resistant clades B2/H24R, B3/H24Rx, and B4/H24RxC. The B2/H24R and B3/H24Rx clades emerged around 1987, concurrently with the C1/H30R and C2/H30Rx clades in E. coli ST131. B3/H24Rx appears to have evolved by the acquisition of the extended-spectrum β-lactamase (ESBL)-encoding gene bla(CTX-M-15) and an IncFII plasmid, encoding IncFIA and IncFIB. Around 2003, the carbapenem-resistant clade B4/H24RxC emerged when ST410 acquired an IncX3 plasmid carrying a bla(OXA-181) carbapenemase gene. Around 2014, the clade B4/H24RxC acquired a second carbapenemase gene, bla(NDM-5), on a conserved IncFII plasmid. From an epidemiological investigation of 49 E. coli ST410 isolates from Danish patients, we identified five possible regional outbreaks, of which one outbreak involved nine patients with bla(OXA-181)- and bla(NDM-5)-carrying B4/H24RxC isolates. The accumulated multidrug resistance in E. coli ST410 over the past two decades, together with its proven potential of transmission between patients, poses a high risk in clinical settings, and thus, E. coli ST410 should be considered a lineage with emerging “high-risk” clones, which should be monitored closely in the future. IMPORTANCE Extraintestinal pathogenic Escherichia coli (ExPEC) is the main cause of urinary tract infections and septicemia. Significant attention has been given to the ExPEC sequence type ST131, which has been categorized as a “high-risk” clone. High-risk clones are globally distributed clones associated with various antimicrobial resistance determinants, ease of transmission, persistence in hosts, and effective transmission between hosts. The high-risk clones have enhanced pathogenicity and cause severe and/or recurrent infections. We show that clones of the E. coli ST410 lineage persist and/or cause recurrent infections in humans, including bloodstream infections. We found evidence of ST410 being a highly resistant globally distributed lineage, capable of patient-to-patient transmission causing hospital outbreaks. Our analysis suggests that the ST410 lineage should be classified with the potential to cause new high-risk clones. Thus, with the clonal expansion over the past decades and increased antimicrobial resistance to last-resort treatment options, ST410 needs to be monitored prospectively. American Society for Microbiology 2018-07-18 /pmc/articles/PMC6052333/ /pubmed/30021879 http://dx.doi.org/10.1128/mSphere.00337-18 Text en Copyright © 2018 Roer et al. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Roer, Louise
Overballe-Petersen, Søren
Hansen, Frank
Schønning, Kristian
Wang, Mikala
Røder, Bent L.
Hansen, Dennis S.
Justesen, Ulrik S.
Andersen, Leif P.
Fulgsang-Damgaard, David
Hopkins, Katie L.
Woodford, Neil
Falgenhauer, Linda
Chakraborty, Trinad
Samuelsen, Ørjan
Sjöström, Karin
Johannesen, Thor B.
Ng, Kim
Nielsen, Jens
Ethelberg, Steen
Stegger, Marc
Hammerum, Anette M.
Hasman, Henrik
Escherichia coli Sequence Type 410 Is Causing New International High-Risk Clones
title Escherichia coli Sequence Type 410 Is Causing New International High-Risk Clones
title_full Escherichia coli Sequence Type 410 Is Causing New International High-Risk Clones
title_fullStr Escherichia coli Sequence Type 410 Is Causing New International High-Risk Clones
title_full_unstemmed Escherichia coli Sequence Type 410 Is Causing New International High-Risk Clones
title_short Escherichia coli Sequence Type 410 Is Causing New International High-Risk Clones
title_sort escherichia coli sequence type 410 is causing new international high-risk clones
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6052333/
https://www.ncbi.nlm.nih.gov/pubmed/30021879
http://dx.doi.org/10.1128/mSphere.00337-18
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