| Literature DB >> 28618267 |
Sophie Thiemann1, Nathiana Smit1, Urmi Roy1, Till Robin Lesker1, Eric J C Gálvez1, Julia Helmecke1, Marijana Basic2, Andre Bleich2, Andrew L Goodman3, Ulrich Kalinke4, Richard A Flavell5, Marc Erhardt6, Till Strowig7.
Abstract
The microbiota contributes to colonization resistance against invading pathogens by competing for metabolites, producing inhibitory substances, and priming protective immune responses. However, the specific commensal bacteria that promote host resistance and immune-mediated protection remain largely elusive. Using isogenic mouse lines with distinct microbiota profiles, we demonstrate that severity of disease induced by enteric Salmonella Typhimurium infection is strongly modulated by microbiota composition in individual lines. Transferring a restricted community of cultivable intestinal commensals from protected into susceptible mice decreases S. Typhimurium tissue colonization and consequently disease severity. This reduced tissue colonization, along with ameliorated weight loss and prolonged survival, depends on microbiota-enhanced IFNγ production, as IFNγ-deficient mice do not exhibit protective effects. Innate cells and CD4+ T cells increase in number and show high levels of IFNγ after transfer of the commensal community. Thus, distinct microbiota members prevent intestinal Salmonella infection by enhancing antibacterial IFNγ responses.Entities:
Keywords: 16S rRNA sequencing; CD4(+) T cells; IFNγ; Salmonella Typhimurium; bacterial cultivation; colonization resistance; enteric infections; intestinal microbiota
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Year: 2017 PMID: 28618267 DOI: 10.1016/j.chom.2017.05.005
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023