2'FL and LNnT Exert Antipathogenic Effects against C. difficile ATCC 9689 In Vitro, Coinciding with Increased Levels of Bifidobacteriaceae and/or Secondary Bile Acids

Louise Kristine Vigsnaes; Jonas Ghyselinck; Pieter Van den Abbeele; Bruce McConnell; Frédéric Moens; Massimo Marzorati; Danica Bajic

doi:10.3390/pathogens10080927

2'FL and LNnT Exert Antipathogenic Effects against C. difficile ATCC 9689 In Vitro, Coinciding with Increased Levels of Bifidobacteriaceae and/or Secondary Bile Acids

Pathogens. 2021 Jul 22;10(8):927. doi: 10.3390/pathogens10080927.

Authors

Louise Kristine Vigsnaes^{1

2}, Jonas Ghyselinck³, Pieter Van den Abbeele^{3

4}, Bruce McConnell¹, Frédéric Moens³, Massimo Marzorati^{3

5}, Danica Bajic¹

Affiliations

¹ Glycom A/S-DSM Nutritional Products Ltd., Kogle Allé 4, DK-2970 Hørsholm, Denmark.
² Department of Technology, Faculty of Health, University College Copenhagen, DK-2200 Copenhagen, Denmark.
³ ProDigest, 9052 Ghent, Belgium.
⁴ Cryptobiotix, 9052 Ghent, Belgium.
⁵ Center of Microbial Ecology and Technology (CMET), Ghent University, 9000 Ghent, Belgium.

Abstract

Clostridioides difficile (formerly Clostridium difficile) infection (CDI) is one of the most common hospital-acquired infections, which is often triggered by a dysbiosed indigenous gut microbiota (e.g., upon antibiotic therapy). Symptoms can be as severe as life-threatening colitis. The current study assessed the antipathogenic potential of human milk oligosaccharides (HMOs), i.e., 2'-O-fucosyllactose (2'FL), lacto-N-neotetraose (LNnT), and a combination thereof (MIX), against C. difficile ATCC 9689 using in vitro gut models that allowed the evaluation of both direct and, upon microbiota modulation, indirect effects. During a first 48 h fecal batch study, dysbiosis and CDI were induced by dilution of the fecal inoculum. For each of the three donors tested, C. difficile levels strongly decreased (with >4 log CFU/mL) upon treatment with 2'FL, LNnT and MIX versus untreated blanks, coinciding with increased acetate/Bifidobacteriaceae levels. Interindividual differences among donors at an intermediate time point suggested that the antimicrobial effect was microbiota-mediated rather than being a direct effect of the HMOs. During a subsequent 11 week study with the Pathogut^TM model (specific application of the Simulator of the Human Intestinal Microbial Ecosystem (SHIME^®)), dysbiosis and CDI were induced by clindamycin (CLI) treatment. Vancomycin (VNC) treatment cured CDI, but the further dysbiosis of the indigenous microbiota likely contributed to CDI recurrence. Upon co-supplementation with VNC, both 2'FL and MIX boosted microbial activity (acetate and to lesser extent propionate/butyrate). Moreover, 2'FL avoided CDI recurrence, potentially because of increased secondary bile acid production. Overall, while not elucidating the exact antipathogenic mechanisms-of-action, the current study highlights the potential of HMOs to combat CDI recurrence, help the gut microbial community recover after antibiotic treatment, and hence counteract the adverse effects of antibiotic therapies.

Keywords: 2′fucosyl-lactose; Clostridioides difficile infection; deoxycholic acid; human milk oligosaccharides; lacto-N-neotetraose.

Grants and funding

Cut-Off 10: reference number 8404/Eurostars