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Self-recognition of the endothelium enables regulatory T-cell trafficking and defines the kinetics of immune regulation.


ABSTRACT: Localization of CD4(+)CD25(+)Foxp3(+) regulatory T (Treg) cells to lymphoid and non-lymphoid tissue is instrumental for the effective control of immune responses. Compared with conventional T cells, Treg cells constitute a minute fraction of the T-cell repertoire. Despite this numeric disadvantage, Tregs efficiently migrate to sites of immune responses reaching an optimal number for the regulation of T effector (Teff) cells. The array and levels of adhesion and chemokine receptor expression by Tregs do not explain their powerful migratory capacity. Here we show that recognition of self-antigens expressed by endothelial cells in target tissue is instrumental for efficient Treg recruitment in vivo. This event relies upon IFN-?-mediated induction of MHC-class-II molecule expression by the endothelium and requires optimal PI3K p110? activation by the T-cell receptor. We also show that, once in the tissue, Tregs inhibit Teff recruitment, further enabling a Teff:Treg ratio optimal for regulation.

SUBMITTER: Fu H 

PROVIDER: S-EPMC3959214 | biostudies-literature | 2014 Mar

REPOSITORIES: biostudies-literature

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Self-recognition of the endothelium enables regulatory T-cell trafficking and defines the kinetics of immune regulation.

Fu Hongmei H   Kishore Madhav M   Gittens Beartice B   Wang Guosu G   Coe David D   Komarowska Izabela I   Infante Elvira E   Ridley Anne J AJ   Cooper Dianne D   Perretti Mauro M   Marelli-Berg Federica M FM  

Nature communications 20140314


Localization of CD4(+)CD25(+)Foxp3(+) regulatory T (Treg) cells to lymphoid and non-lymphoid tissue is instrumental for the effective control of immune responses. Compared with conventional T cells, Treg cells constitute a minute fraction of the T-cell repertoire. Despite this numeric disadvantage, Tregs efficiently migrate to sites of immune responses reaching an optimal number for the regulation of T effector (Teff) cells. The array and levels of adhesion and chemokine receptor expression by T  ...[more]

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2019-12-03 | GSE130810 | GEO