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Identifying species of symbiont bacteria from the human gut that, alone, can induce intestinal Th17 cells in mice.


ABSTRACT: Th17 cells accrue in the intestine in response to particular microbes. In rodents, segmented filamentous bacteria (SFB) induce intestinal Th17 cells, but analogously functioning microbes in humans remain undefined. Here, we identified human symbiont bacterial species, in particular Bifidobacterium adolescentis, that could, alone, induce Th17 cells in the murine intestine. Similar to SFB, B. adolescentis was closely associated with the gut epithelium and engendered cognate Th17 cells without attendant inflammation. However, B. adolescentis elicited a transcriptional program clearly distinct from that of SFB, suggesting an alternative mechanism of promoting Th17 cell accumulation. Inoculation of mice with B. adolescentis exacerbated autoimmune arthritis in the K/BxN mouse model. Several off-the-shelf probiotic preparations that include Bifidobacterium strains also drove intestinal Th17 cell accumulation.

SUBMITTER: Tan TG 

PROVIDER: S-EPMC5167147 | biostudies-literature | 2016 Dec

REPOSITORIES: biostudies-literature

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Identifying species of symbiont bacteria from the human gut that, alone, can induce intestinal Th17 cells in mice.

Tan Tze Guan TG   Sefik Esen E   Geva-Zatorsky Naama N   Kua Lindsay L   Naskar Debdut D   Teng Fei F   Pasman Lesley L   Ortiz-Lopez Adriana A   Jupp Ray R   Wu Hsin-Jung Joyce HJ   Kasper Dennis L DL   Benoist Christophe C   Mathis Diane D  

Proceedings of the National Academy of Sciences of the United States of America 20161123 50


Th17 cells accrue in the intestine in response to particular microbes. In rodents, segmented filamentous bacteria (SFB) induce intestinal Th17 cells, but analogously functioning microbes in humans remain undefined. Here, we identified human symbiont bacterial species, in particular Bifidobacterium adolescentis, that could, alone, induce Th17 cells in the murine intestine. Similar to SFB, B. adolescentis was closely associated with the gut epithelium and engendered cognate Th17 cells without atte  ...[more]

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