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Immune tolerance: Are regulatory T cell subsets needed to explain suppression of autoimmunity?
Author(s) -
Tian Lei,
HumbletBaron Stephanie,
Liston Adrian
Publication year - 2012
Publication title -
bioessays
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.175
H-Index - 184
eISSN - 1521-1878
pISSN - 0265-9247
DOI - 10.1002/bies.201100180
Subject(s) - effector , foxp3 , biology , immune system , autoimmunity , peripheral tolerance , immunology , t cell , immune tolerance , microbiology and biotechnology , regulatory t cell , il 2 receptor
The potential for self‐reactive T cells to cause autoimmune disease is held in check by Foxp3 + regulatory T cells (Tregs), essential mediators of peripheral immunological tolerance. Tregs have the capacity to suppress multiple branches of the immune system, tightly controlling the different subsets of effector T cells across multiple different tissue environments. Recent genetic experiments have found mutations that disrupt specific Treg: effector T cell relationships, leading to the possibility that subsets of Tregs are required to suppress each subset of effector T cells. Here we review the environmental factors and mechanisms that allow Tregs to suppress specific subsets of effector T cells, and find that a parsimonious explanation of the genetic data can be made without invoking Treg subsets. Instead, Tregs show a functional and chemotactic plasticity based on microenvironmental influences that allows the common pool of cells to suppress multiple distinct immune responses.