Metagenomics-Based, Strain-Level Analysis of Escherichia coli From a Time-Series of Microbiome Samples From a Crohn's Disease Patient

Dysbiosis of the gut microbiome, including elevated abundance of putative leading bacterial triggers such as E. coli in inflammatory bowel disease (IBD) patients, is of great interest. To date, most E. coli studies in IBD patients are focused on clinical isolates, overlooking their relative abundanc...

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Autores principales: Fang, Xin, Monk, Jonathan M., Nurk, Sergey, Akseshina, Margarita, Zhu, Qiyun, Gemmell, Christopher, Gianetto-Hill, Connor, Leung, Nelly, Szubin, Richard, Sanders, Jon, Beck, Paul L., Li, Weizhong, Sandborn, William J., Gray-Owen, Scott D., Knight, Rob, Allen-Vercoe, Emma, Palsson, Bernhard O., Smarr, Larry
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6218438/
https://www.ncbi.nlm.nih.gov/pubmed/30425690
http://dx.doi.org/10.3389/fmicb.2018.02559
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author Fang, Xin
Monk, Jonathan M.
Nurk, Sergey
Akseshina, Margarita
Zhu, Qiyun
Gemmell, Christopher
Gianetto-Hill, Connor
Leung, Nelly
Szubin, Richard
Sanders, Jon
Beck, Paul L.
Li, Weizhong
Sandborn, William J.
Gray-Owen, Scott D.
Knight, Rob
Allen-Vercoe, Emma
Palsson, Bernhard O.
Smarr, Larry
author_facet Fang, Xin
Monk, Jonathan M.
Nurk, Sergey
Akseshina, Margarita
Zhu, Qiyun
Gemmell, Christopher
Gianetto-Hill, Connor
Leung, Nelly
Szubin, Richard
Sanders, Jon
Beck, Paul L.
Li, Weizhong
Sandborn, William J.
Gray-Owen, Scott D.
Knight, Rob
Allen-Vercoe, Emma
Palsson, Bernhard O.
Smarr, Larry
author_sort Fang, Xin
collection PubMed
description Dysbiosis of the gut microbiome, including elevated abundance of putative leading bacterial triggers such as E. coli in inflammatory bowel disease (IBD) patients, is of great interest. To date, most E. coli studies in IBD patients are focused on clinical isolates, overlooking their relative abundances and turnover over time. Metagenomics-based studies, on the other hand, are less focused on strain-level investigations. Here, using recently developed bioinformatic tools, we analyzed the abundance and properties of specific E. coli strains in a Crohns disease (CD) patient longitudinally, while also considering the composition of the entire community over time. In this report, we conducted a pilot study on metagenomic-based, strain-level analysis of a time-series of E. coli strains in a left-sided CD patient, who exhibited sustained levels of E. coli greater than 100X healthy controls. We: (1) mapped out the composition of the gut microbiome over time, particularly the presence of E. coli strains, and found that the abundance and dominance of specific E. coli strains in the community varied over time; (2) performed strain-level de novo assemblies of seven dominant E. coli strains, and illustrated disparity between these strains in both phylogenetic origin and genomic content; (3) observed that strain ST1 (recovered during peak inflammation) is highly similar to known pathogenic AIEC strains NC101 and LF82 in both virulence factors and metabolic functions, while other strains (ST2-ST7) that were collected during more stable states displayed diverse characteristics; (4) isolated, sequenced, experimentally characterized ST1, and confirmed the accuracy of the de novo assembly; and (5) assessed growth capability of ST1 with a newly reconstructed genome-scale metabolic model of the strain, and showed its potential to use substrates found abundantly in the human gut to outcompete other microbes. In conclusion, inflammation status (assessed by the blood C-reactive protein and stool calprotectin) is likely correlated with the abundance of a subgroup of E. coli strains with specific traits. Therefore, strain-level time-series analysis of dominant E. coli strains in a CD patient is highly informative, and motivates a study of a larger cohort of IBD patients.
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spelling pubmed-62184382018-11-13 Metagenomics-Based, Strain-Level Analysis of Escherichia coli From a Time-Series of Microbiome Samples From a Crohn's Disease Patient Fang, Xin Monk, Jonathan M. Nurk, Sergey Akseshina, Margarita Zhu, Qiyun Gemmell, Christopher Gianetto-Hill, Connor Leung, Nelly Szubin, Richard Sanders, Jon Beck, Paul L. Li, Weizhong Sandborn, William J. Gray-Owen, Scott D. Knight, Rob Allen-Vercoe, Emma Palsson, Bernhard O. Smarr, Larry Front Microbiol Microbiology Dysbiosis of the gut microbiome, including elevated abundance of putative leading bacterial triggers such as E. coli in inflammatory bowel disease (IBD) patients, is of great interest. To date, most E. coli studies in IBD patients are focused on clinical isolates, overlooking their relative abundances and turnover over time. Metagenomics-based studies, on the other hand, are less focused on strain-level investigations. Here, using recently developed bioinformatic tools, we analyzed the abundance and properties of specific E. coli strains in a Crohns disease (CD) patient longitudinally, while also considering the composition of the entire community over time. In this report, we conducted a pilot study on metagenomic-based, strain-level analysis of a time-series of E. coli strains in a left-sided CD patient, who exhibited sustained levels of E. coli greater than 100X healthy controls. We: (1) mapped out the composition of the gut microbiome over time, particularly the presence of E. coli strains, and found that the abundance and dominance of specific E. coli strains in the community varied over time; (2) performed strain-level de novo assemblies of seven dominant E. coli strains, and illustrated disparity between these strains in both phylogenetic origin and genomic content; (3) observed that strain ST1 (recovered during peak inflammation) is highly similar to known pathogenic AIEC strains NC101 and LF82 in both virulence factors and metabolic functions, while other strains (ST2-ST7) that were collected during more stable states displayed diverse characteristics; (4) isolated, sequenced, experimentally characterized ST1, and confirmed the accuracy of the de novo assembly; and (5) assessed growth capability of ST1 with a newly reconstructed genome-scale metabolic model of the strain, and showed its potential to use substrates found abundantly in the human gut to outcompete other microbes. In conclusion, inflammation status (assessed by the blood C-reactive protein and stool calprotectin) is likely correlated with the abundance of a subgroup of E. coli strains with specific traits. Therefore, strain-level time-series analysis of dominant E. coli strains in a CD patient is highly informative, and motivates a study of a larger cohort of IBD patients. Frontiers Media S.A. 2018-10-30 /pmc/articles/PMC6218438/ /pubmed/30425690 http://dx.doi.org/10.3389/fmicb.2018.02559 Text en Copyright © 2018 Fang, Monk, Nurk, Akseshina, Zhu, Gemmell, Gianetto-Hill, Leung, Szubin, Sanders, Beck, Li, Sandborn, Gray-Owen, Knight, Allen-Vercoe, Palsson and Smarr. http://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 Microbiology
Fang, Xin
Monk, Jonathan M.
Nurk, Sergey
Akseshina, Margarita
Zhu, Qiyun
Gemmell, Christopher
Gianetto-Hill, Connor
Leung, Nelly
Szubin, Richard
Sanders, Jon
Beck, Paul L.
Li, Weizhong
Sandborn, William J.
Gray-Owen, Scott D.
Knight, Rob
Allen-Vercoe, Emma
Palsson, Bernhard O.
Smarr, Larry
Metagenomics-Based, Strain-Level Analysis of Escherichia coli From a Time-Series of Microbiome Samples From a Crohn's Disease Patient
title Metagenomics-Based, Strain-Level Analysis of Escherichia coli From a Time-Series of Microbiome Samples From a Crohn's Disease Patient
title_full Metagenomics-Based, Strain-Level Analysis of Escherichia coli From a Time-Series of Microbiome Samples From a Crohn's Disease Patient
title_fullStr Metagenomics-Based, Strain-Level Analysis of Escherichia coli From a Time-Series of Microbiome Samples From a Crohn's Disease Patient
title_full_unstemmed Metagenomics-Based, Strain-Level Analysis of Escherichia coli From a Time-Series of Microbiome Samples From a Crohn's Disease Patient
title_short Metagenomics-Based, Strain-Level Analysis of Escherichia coli From a Time-Series of Microbiome Samples From a Crohn's Disease Patient
title_sort metagenomics-based, strain-level analysis of escherichia coli from a time-series of microbiome samples from a crohn's disease patient
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6218438/
https://www.ncbi.nlm.nih.gov/pubmed/30425690
http://dx.doi.org/10.3389/fmicb.2018.02559
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