Literature DB >> 33469019

Clostridioides difficile exploits toxin-mediated inflammation to alter the host nutritional landscape and exclude competitors from the gut microbiota.

Joshua R Fletcher1, Colleen M Pike1, Ruth J Parsons1, Alissa J Rivera1, Matthew H Foley1, Michael R McLaren1, Stephanie A Montgomery2, Casey M Theriot3.   

Abstract

Clostridioides difficile is a bacterial pathogen that causes a range of clinical disease from mild to moderate diarrhea, pseudomembranous colitis, and toxic megacolon. Typically, C. difficile infections (CDIs) occur after antibiotic treatment, which alters the gut microbiota, decreasing colonization resistance against C. difficile. Disease is mediated by two large toxins and the expression of their genes is induced upon nutrient depletion via the alternative sigma factor TcdR. Here, we use tcdR mutants in two strains of C. difficile and omics to investigate how toxin-induced inflammation alters C. difficile metabolism, tissue gene expression and the gut microbiota, and to determine how inflammation by the host may be beneficial to C. difficile. We show that C. difficile metabolism is significantly different in the face of inflammation, with changes in many carbohydrate and amino acid uptake and utilization pathways. Host gene expression signatures suggest that degradation of collagen and other components of the extracellular matrix by matrix metalloproteinases is a major source of peptides and amino acids that supports C. difficile growth in vivo. Lastly, the inflammation induced by C. difficile toxin activity alters the gut microbiota, excluding members from the genus Bacteroides that are able to utilize the same essential nutrients released from collagen degradation.

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Year:  2021        PMID: 33469019      PMCID: PMC7815924          DOI: 10.1038/s41467-020-20746-4

Source DB:  PubMed          Journal:  Nat Commun        ISSN: 2041-1723            Impact factor:   14.919


  69 in total

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Journal:  Biochem Biophys Res Commun       Date:  2000-10-14       Impact factor: 3.575

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3.  Incidence of Clostridium difficile infection in inflammatory bowel disease.

Authors:  Joseph F Rodemann; Erik R Dubberke; Kimberly A Reske; Da Hea Seo; Christian D Stone
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5.  Ecologically meaningful transformations for ordination of species data.

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6.  Cefoperazone-treated Mouse Model of Clinically-relevant Clostridium difficile Strain R20291.

Authors:  Jenessa A Winston; Rajani Thanissery; Stephanie A Montgomery; Casey M Theriot
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Review 7.  Clostridium difficile Toxin Biology.

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Journal:  Annu Rev Microbiol       Date:  2017-06-28       Impact factor: 15.500

8.  A defined growth medium for Clostridium difficile.

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10.  Metabolic Reprogramming of Clostridioides difficile During the Stationary Phase With the Induction of Toxin Production.

Authors:  Julia D Hofmann; Andreas Otto; Mareike Berges; Rebekka Biedendieck; Annika-Marisa Michel; Dörte Becher; Dieter Jahn; Meina Neumann-Schaal
Journal:  Front Microbiol       Date:  2018-08-21       Impact factor: 5.640

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  23 in total

Review 1.  Computational approaches to understanding Clostridioides difficile metabolism and virulence.

Authors:  Matthew L Jenior; Jason A Papin
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2.  A pilot study to investigate the alteration of gut microbial profile in Dip2a knockout mice.

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3.  d-Proline Reductase Underlies Proline-Dependent Growth of Clostridioides difficile.

Authors:  Michael A Johnstone; William T Self
Journal:  J Bacteriol       Date:  2022-07-13       Impact factor: 3.476

4.  Gut microbiome ADP-ribosyltransferases are widespread phage-encoded fitness factors.

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Journal:  Cell Host Microbe       Date:  2021-08-16       Impact factor: 31.316

5.  Akkermansia muciniphila Ameliorates Clostridioides difficile Infection in Mice by Modulating the Intestinal Microbiome and Metabolites.

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6.  Strain Variation in Clostridioides difficile Cytotoxicity Associated with Genomic Variation at Both Pathogenic and Nonpathogenic Loci.

Authors:  Katie Saund; Ali Pirani; D Borden Lacy; Philip C Hanna; Evan Snitkin
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Review 7.  Capturing the environment of the Clostridioides difficile infection cycle.

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8.  Therapeutic Effects of Bifidobacterium breve YH68 in Combination with Vancomycin and Metronidazole in a Primary Clostridioides difficile-Infected Mouse Model.

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9.  Intestinal Inflammation and Altered Gut Microbiota Associated with Inflammatory Bowel Disease Render Mice Susceptible to Clostridioides difficile Colonization and Infection.

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10.  What's a Biofilm?-How the Choice of the Biofilm Model Impacts the Protein Inventory of Clostridioides difficile.

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Journal:  Front Microbiol       Date:  2021-06-10       Impact factor: 5.640

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