| Literature DB >> 35536673 |
Sothea Touch1,2, Emmanuelle Godefroy3, Nathalie Rolhion1,2, Camille Danne1,2,4, Cyriane Oeuvray1,2, Marjolène Straube1,2, Chloé Galbert1,2, Loïc Brot1,2, Iria Alonso Salgueiro1,2, Sead Chadi4, Tatiana Ledent1, Jean-Marc Chatel4, Philippe Langella4, Francine Jotereau3, Frédéric Altare3, Harry Sokol1,2,4.
Abstract
Abundance of Faecalibacterium prausnitzii, a dominant bacterium of the human microbiota that exhibits antiinflammatory effects, is decreased in patients with inflammatory bowel diseases (IBD). In humans, colonic lamina propria contains IL-10-secreting, Foxp3- Tregs characterized by a double expression of CD4 and CD8α (DP8α) and a specificity for F. prausnitzii. This Treg subset is decreased in IBD. The in vivo effect of DP8α cells has not been evaluated yet to our knowledge. Here, using a humanized model of a NSG immunodeficient mouse strain that expresses the HLA D-related allele HLA-DR*0401 but not murine class II (NSG-Ab° DR4) molecules, we demonstrated a protective effect of a HLA-DR*0401-restricted DP8α Treg clone combined with F. prausnitzii administration in a colitis model. In a cohort of patients with IBD, we showed an independent association between the frequency of circulating DP8α cells and disease activity. Finally, we pointed out a positive correlation between F. prausnitzii-specific DP8α Tregs and the amount of F. prausnitzii in fecal microbiota in healthy individuals and patients with ileal Crohn's disease.Entities:
Keywords: Gastroenterology; Inflammatory bowel disease; Mouse models; T cells
Mesh:
Year: 2022 PMID: 35536673 PMCID: PMC9309064 DOI: 10.1172/jci.insight.154722
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708