| Literature DB >> 30341145 |
Ravi Verma1, Changhon Lee2, Eun-Ji Jeun2, Jaeu Yi2, Kwang Soon Kim1, Ambarnil Ghosh1, Seohyun Byun2, Choong-Gu Lee1, Hye-Ji Kang1, Gi-Cheon Kim1, Chang-Duk Jun3, Gwenaël Jan4, Chang-Hee Suh5, Ju-Yang Jung5, Jonathan Sprent2,6, Dipayan Rudra1,2, Cristina De Castro7,8, Antonio Molinaro8,9, Charles D Surh1,2, Sin-Hyeog Im10,2.
Abstract
Dysregulation of intestinal microflora is linked to inflammatory disorders associated with compromised immunosuppressive functions of Foxp3+ T regulatory (Treg) cells. Although mucosa-associated commensal microbiota has been implicated in Treg generation, molecular identities of the "effector" components controlling this process remain largely unknown. Here, we have defined Bifidobacterium bifidum as a potent inducer of Foxp3+ Treg cells with diverse T cell receptor specificity to dietary antigens, commensal bacteria, and B. bifidum itself. Cell surface β-glucan/galactan (CSGG) polysaccharides of B. bifidum were identified as key components responsible for Treg induction. CSGG efficiently recapitulated the activity of whole bacteria and acted via regulatory dendritic cells through a partially Toll-like receptor 2-mediated mechanism. Treg cells induced by B. bifidum or purified CSGG display stable and robust suppressive capacity toward experimental colitis. By identifying CSGG as a functional component of Treg-inducing bacteria, our studies highlight the immunomodulatory potential of CSGG and CSGG-producing microbes.Entities:
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Year: 2018 PMID: 30341145 DOI: 10.1126/sciimmunol.aat6975
Source DB: PubMed Journal: Sci Immunol ISSN: 2470-9468