4.5 Article

Phenotyping of Fecal Microbiota of Winnie, a Rodent Model of Spontaneous Chronic Colitis, Reveals Specific Metabolic, Genotoxic, and Pro-inflammatory Properties

Journal

INFLAMMATION
Volume 45, Issue 6, Pages 2477-2497

Publisher

SPRINGER/PLENUM PUBLISHERS
DOI: 10.1007/s10753-022-01706-0

Keywords

Winnie intestinal microbiota; phenotyping; inflammation; genotoxicity

Funding

  1. Universita del Salento within the CRUI-CARE Agreement
  2. Italian Ministry for Universities and Research
  3. Europe Union FSE, within the program PON Ricerca e Innovazione 2014-2020
  4. FSC, Asse 2, Azione II, 2 Cluster -Ricerca industriale e sviluppo sperimentale -Area di specializzazione Salute -Project [ARS0101220]

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This study demonstrates that the intestinal environment of mice with a missense mutation in the MUC2 mucin gene selects a specific intestinal microbial community characterized by pro-inflammatory, genotoxic, and metabolic features, suggesting its direct involvement in the pathogenesis of chronic intestinal inflammation.
Winnie, a mouse carrying a missense mutation in the MUC2 mucin gene, is a valuable model for inflammatory bowel disease (IBD) with signs and symptoms that have multiple similarities with those observed in patients with ulcerative colitis. MUC2 mucin is present in Winnie, but is not firmly compacted in a tight inner layer. Indeed, these mice develop chronic intestinal inflammation due to the primary epithelial defect with signs of mucosal damage, including thickening of muscle and mucosal layers, goblet cell loss, increased intestinal permeability, enhanced susceptibility to luminal inflammation-inducing toxins, and alteration of innervation in the distal colon. In this study, we show that the intestinal environment of the Winnie mouse, genetically determined by MUC2 mutation, selects an intestinal microbial community characterized by specific pro-inflammatory, genotoxic, and metabolic features that could imply a direct involvement in the pathogenesis of chronic intestinal inflammation. We report results obtained by using a variety of in vitro approaches for fecal microbiota functional characterization. These approaches include Caco-2 cell cultures and Caco-2/THP-1 cell co-culture models for evaluation of geno-cytotoxic and pro-inflammatory properties using a panel of 43 marker RNAs assayed by RT-qPCR, and cell-based phenotypic testing for metabolic profiling of the intestinal microbial communities by Biolog EcoPlates. While adding a further step towards understanding the etiopathogenetic mechanisms underlying IBD, the results of this study provide a reliable method for phenotyping gut microbial communities, which can complement their structural characterization by providing novel functional information.

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