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Commensal epitopes drive differentiation of colonic Tregs.


ABSTRACT: The gut microbiome is the largest source of intrinsic non-self-antigens that are continuously sensed by the immune system but typically do not elicit lymphocyte responses. CD4+ T cells are critical to sustain uninterrupted tolerance to microbial antigens and to prevent intestinal inflammation. However, clinical interventions targeting commensal bacteria-specific CD4+ T cells are rare, because only a very limited number of commensal-derived epitopes have been identified. Here, we used a new approach to study epitopes and identify T cell receptors expressed by CD4+Foxp3+ (Treg) cells specific for commensal-derived antigens. Using this approach, we found that antigens from Akkermansia muciniphila reprogram naïve CD4+ T cells to the Treg lineage, expand preexisting microbe specific Tregs, and limit wasting disease in the CD4+ T cell transfer model of colitis. These data suggest that the administration of specific commensal epitopes may help to widen the repertoire of specific Tregs that control intestinal inflammation.

SUBMITTER: Kuczma MP 

PROVIDER: S-EPMC7164940 | biostudies-literature | 2020 Apr

REPOSITORIES: biostudies-literature

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Commensal epitopes drive differentiation of colonic T<sub>regs</sub>.

Kuczma Michal P MP   Szurek Edyta A EA   Cebula Anna A   Chassaing Benoit B   Jung Yu-Jin YJ   Kang Sang-Moo SM   Fox James G JG   Stecher Bärbel B   Ignatowicz Leszek L  

Science advances 20200417 16


The gut microbiome is the largest source of intrinsic non-self-antigens that are continuously sensed by the immune system but typically do not elicit lymphocyte responses. CD4<sup>+</sup> T cells are critical to sustain uninterrupted tolerance to microbial antigens and to prevent intestinal inflammation. However, clinical interventions targeting commensal bacteria-specific CD4<sup>+</sup> T cells are rare, because only a very limited number of commensal-derived epitopes have been identified. Her  ...[more]

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