Literature DB >> 29462695

A 3D intestinal tissue model supports Clostridioides difficile germination, colonization, toxin production and epithelial damage.

Lamyaa Shaban1, Ying Chen2, Alyssa C Fasciano3, Yinan Lin2, David L Kaplan2, Carol A Kumamoto4, Joan Mecsas5.   

Abstract

Endospore-forming Clostridioides difficile is a causative agent of antibiotic-induced diarrhea, a major nosocomial infection. Studies of its interactions with mammalian tissues have been hampered by the fact that C. difficile requires anaerobic conditions to survive after spore germination. We recently developed a bioengineered 3D human intestinal tissue model and found that low O2 conditions are produced in the lumen of these tissues. Here, we compared the ability of C. difficile spores to germinate, produce toxin and cause tissue damage in our bioengineered 3D tissue model versus in a 2D transwell model in which human cells form a polarized monolayer. 3D tissue models or 2D polarized monolayers on transwell filters were challenged with the non-toxin producing C. difficile CCUG 37787 serotype X (ATCC 43603) and the toxin producing UK1 C. difficile spores in the presence of the germinant, taurocholate. Spores germinated in both the 3D tissue model as well as the 2D transwell system, however toxin activity was significantly higher in the 3D tissue models compared to the 2D transwells. Moreover, the epithelium damage in the 3D tissue model was significantly more severe than in 2D transwells and damage correlated significantly with the level of toxin activity detected but not with the amount of germinated spores. Combined, these results show that the bioengineered 3D tissue model provides a powerful system with which to study early events leading to toxin production and tissue damage of C. difficile with mammalian cells under anaerobic conditions. Furthermore, these systems may be useful for examining the effects of microbiota, novel drugs and other potential therapeutics directed towards C. difficile infections.
Copyright © 2018 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  2D transwell; 3D intestinal tissue; Clostridioides difficile; Clostridium difficile; Germination; Toxin activity

Mesh:

Substances:

Year:  2018        PMID: 29462695      PMCID: PMC5866244          DOI: 10.1016/j.anaerobe.2018.02.006

Source DB:  PubMed          Journal:  Anaerobe        ISSN: 1075-9964            Impact factor:   3.331


  28 in total

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2.  Human Clostridium difficile infection: inhibition of NHE3 and microbiota profile.

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3.  Human Clostridium difficile infection: altered mucus production and composition.

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Journal:  Am J Physiol Gastrointest Liver Physiol       Date:  2014-12-31       Impact factor: 4.052

4.  The role of toxin A and toxin B in Clostridium difficile infection.

Authors:  Sarah A Kuehne; Stephen T Cartman; John T Heap; Michelle L Kelly; Alan Cockayne; Nigel P Minton
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Journal:  Nature       Date:  2015-06-03       Impact factor: 49.962

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  11 in total

Review 1.  New Age Strategies To Reconstruct Mucosal Tissue Colonization and Growth in Cell Culture Systems.

Authors:  Alyssa C Fasciano; Joan Mecsas; Ralph R Isberg
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2.  An in vitro intestinal platform with a self-sustaining oxygen gradient to study the human gut/microbiome interface.

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4.  Bioengineered 3D Tissue Model of Intestine Epithelium with Oxygen Gradients to Sustain Human Gut Microbiome.

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5.  Bi-layered Tubular Microfiber Scaffolds as Functional Templates for Engineering Human Intestinal Smooth Muscle Tissue.

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Review 9.  A review of co-culture models to study the oral microenvironment and disease.

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10.  Soluble Non-Starch Polysaccharides From Plantain (Musa x paradisiaca L.) Diminish Epithelial Impact of Clostridioides difficile.

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