Escherichia coli killing by epidemiologically successful sublineages of Shigella sonnei is mediated by colicins

BACKGROUND: Shigella sp. are enteric pathogens which causes >125 million cases of shigellosis annually. S. sonnei accounts for about a quarter of those cases and is increasingly prevalent in industrialising nations. Being an enteric pathogen, S. sonnei benefits from outcompeting gut commensals su...

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Autores principales: De Silva, P. Malaka, Bennett, Rebecca J., Kuhn, Lauriane, Ngondo, Patryk, Debande, Lorine, Njamkepo, Elisabeth, Ho, Brian, Weill, François-Xavier, Marteyn, Benoît S., Jenkins, Claire, Baker, Kate S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10579285/
https://www.ncbi.nlm.nih.gov/pubmed/37806286
http://dx.doi.org/10.1016/j.ebiom.2023.104822
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author De Silva, P. Malaka
Bennett, Rebecca J.
Kuhn, Lauriane
Ngondo, Patryk
Debande, Lorine
Njamkepo, Elisabeth
Ho, Brian
Weill, François-Xavier
Marteyn, Benoît S.
Jenkins, Claire
Baker, Kate S.
author_facet De Silva, P. Malaka
Bennett, Rebecca J.
Kuhn, Lauriane
Ngondo, Patryk
Debande, Lorine
Njamkepo, Elisabeth
Ho, Brian
Weill, François-Xavier
Marteyn, Benoît S.
Jenkins, Claire
Baker, Kate S.
author_sort De Silva, P. Malaka
collection PubMed
description BACKGROUND: Shigella sp. are enteric pathogens which causes >125 million cases of shigellosis annually. S. sonnei accounts for about a quarter of those cases and is increasingly prevalent in industrialising nations. Being an enteric pathogen, S. sonnei benefits from outcompeting gut commensals such as Escherichia coli to establish itself and cause disease. There are numerous mechanisms that bacterial pathogens use to outcompete its rivals including molecules called colicins. A Type 6 Secretion System (T6SS) was recently described as contributing to E. coli killing in S. sonnei. METHODS: We used Bulk Phenotyping of Epidemiological Replicates (BPER) which combined bacterial Genome Wide Association Studies (bGWAS) and high throughput phenotyping on a collection of S. sonnei surveillance isolates to identify the genetic features associated with E. coli killing and explore their relationship with epidemiological behaviour. We further explored the presence of colicins and T6SS components in the isolates using genomics, laboratory experimentation, and proteomics. FINDINGS: Our bGWAS analysis returned known and novel colicin and colicin related genes as significantly associated with E. coli killing. In silico analyses identified key colicin clusters responsible for the killing phenotype associated with epidemiologically successful sub-lineages. The killing phenotype was not associated with the presence of a T6SS. Laboratory analyses confirmed the presence of the key colicin clusters and that killing was contact-independent. INTERPRETATION: Colicins are responsible for E. coli killing by S. sonnei, not a T6SS. This phenotype contributes to shaping the observed epidemiology of S. sonnei and may contribute to its increasing prevalence globally. BPER is an epidemiologically relevant approach to phenotypic testing that enables the rapid identification of genetic drivers of phenotypic changes, and assessment of their relevance to epidemiology in natural settings. FUNDING: 10.13039/501100000268Biotechnology and Biological Sciences Research Council, Biotechnology and Biological Sciences Research Council Doctoral Training Partnership studentship, 10.13039/100010269Wellcome Trust, 10.13039/501100000265Medical Research Council (UK), 10.13039/501100001665French National Research Agency.
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spelling pubmed-105792852023-10-18 Escherichia coli killing by epidemiologically successful sublineages of Shigella sonnei is mediated by colicins De Silva, P. Malaka Bennett, Rebecca J. Kuhn, Lauriane Ngondo, Patryk Debande, Lorine Njamkepo, Elisabeth Ho, Brian Weill, François-Xavier Marteyn, Benoît S. Jenkins, Claire Baker, Kate S. eBioMedicine Articles BACKGROUND: Shigella sp. are enteric pathogens which causes >125 million cases of shigellosis annually. S. sonnei accounts for about a quarter of those cases and is increasingly prevalent in industrialising nations. Being an enteric pathogen, S. sonnei benefits from outcompeting gut commensals such as Escherichia coli to establish itself and cause disease. There are numerous mechanisms that bacterial pathogens use to outcompete its rivals including molecules called colicins. A Type 6 Secretion System (T6SS) was recently described as contributing to E. coli killing in S. sonnei. METHODS: We used Bulk Phenotyping of Epidemiological Replicates (BPER) which combined bacterial Genome Wide Association Studies (bGWAS) and high throughput phenotyping on a collection of S. sonnei surveillance isolates to identify the genetic features associated with E. coli killing and explore their relationship with epidemiological behaviour. We further explored the presence of colicins and T6SS components in the isolates using genomics, laboratory experimentation, and proteomics. FINDINGS: Our bGWAS analysis returned known and novel colicin and colicin related genes as significantly associated with E. coli killing. In silico analyses identified key colicin clusters responsible for the killing phenotype associated with epidemiologically successful sub-lineages. The killing phenotype was not associated with the presence of a T6SS. Laboratory analyses confirmed the presence of the key colicin clusters and that killing was contact-independent. INTERPRETATION: Colicins are responsible for E. coli killing by S. sonnei, not a T6SS. This phenotype contributes to shaping the observed epidemiology of S. sonnei and may contribute to its increasing prevalence globally. BPER is an epidemiologically relevant approach to phenotypic testing that enables the rapid identification of genetic drivers of phenotypic changes, and assessment of their relevance to epidemiology in natural settings. FUNDING: 10.13039/501100000268Biotechnology and Biological Sciences Research Council, Biotechnology and Biological Sciences Research Council Doctoral Training Partnership studentship, 10.13039/100010269Wellcome Trust, 10.13039/501100000265Medical Research Council (UK), 10.13039/501100001665French National Research Agency. Elsevier 2023-10-06 /pmc/articles/PMC10579285/ /pubmed/37806286 http://dx.doi.org/10.1016/j.ebiom.2023.104822 Text en © 2023 The Author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Articles
De Silva, P. Malaka
Bennett, Rebecca J.
Kuhn, Lauriane
Ngondo, Patryk
Debande, Lorine
Njamkepo, Elisabeth
Ho, Brian
Weill, François-Xavier
Marteyn, Benoît S.
Jenkins, Claire
Baker, Kate S.
Escherichia coli killing by epidemiologically successful sublineages of Shigella sonnei is mediated by colicins
title Escherichia coli killing by epidemiologically successful sublineages of Shigella sonnei is mediated by colicins
title_full Escherichia coli killing by epidemiologically successful sublineages of Shigella sonnei is mediated by colicins
title_fullStr Escherichia coli killing by epidemiologically successful sublineages of Shigella sonnei is mediated by colicins
title_full_unstemmed Escherichia coli killing by epidemiologically successful sublineages of Shigella sonnei is mediated by colicins
title_short Escherichia coli killing by epidemiologically successful sublineages of Shigella sonnei is mediated by colicins
title_sort escherichia coli killing by epidemiologically successful sublineages of shigella sonnei is mediated by colicins
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10579285/
https://www.ncbi.nlm.nih.gov/pubmed/37806286
http://dx.doi.org/10.1016/j.ebiom.2023.104822
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