%0 Journal Article %1 Legoux2015896 %A Legoux, F P %A Lim, J B %A Cauley, A W %A Dikiy, S %A Ertelt, J %A Mariani, T J %A Sparwasser, T %A Way, S S %A Moon, J J %D 2015 %E Immunity, %J Immunity %K sparwasser %N 5 %P 896 - 908 %T CD4+ T Cell Tolerance to Tissue-Restricted Self Antigens Is Mediated by Antigen-Specific Regulatory T Cells Rather Than Deletion %V 43 %X Summary Deletion of self-antigen-specific T cells during thymic development provides protection from autoimmunity. However, it is unclear how efficiently this occurs for tissue-restricted self antigens, or how immune tolerance is maintained for self-antigen-specific T cells that routinely escape deletion. Here we show that endogenous CD4+ T cells with specificity for a set of tissue-restricted self antigens were not deleted at all. For pancreatic self antigen, this resulted in an absence of steady-state tolerance, while for the lung and intestine, tolerance was maintained by the enhanced presence of thymically-derived antigen-specific Foxp3+ regulatory T (Treg) cells. Unlike deletional tolerance, Treg cell-mediated tolerance was broken by successive antigen challenges. These findings reveal that for some tissue-restricted self antigens, tolerance relies entirely on nondeletional mechanisms that are less durable than T cell deletion. This might explain why autoimmunity is often tissue-specific, and it offers a rationale for cancer vaccine strategies targeting tissue-restricted tumor antigens.

@article{Legoux2015896, abstract = {Summary Deletion of self-antigen-specific T cells during thymic development provides protection from autoimmunity. However, it is unclear how efficiently this occurs for tissue-restricted self antigens, or how immune tolerance is maintained for self-antigen-specific T cells that routinely escape deletion. Here we show that endogenous CD4+ T cells with specificity for a set of tissue-restricted self antigens were not deleted at all. For pancreatic self antigen, this resulted in an absence of steady-state tolerance, while for the lung and intestine, tolerance was maintained by the enhanced presence of thymically-derived antigen-specific Foxp3+ regulatory T (Treg) cells. Unlike deletional tolerance, Treg cell-mediated tolerance was broken by successive antigen challenges. These findings reveal that for some tissue-restricted self antigens, tolerance relies entirely on nondeletional mechanisms that are less durable than T cell deletion. This might explain why autoimmunity is often tissue-specific, and it offers a rationale for cancer vaccine strategies targeting tissue-restricted tumor antigens. }, added-at = {2015-12-01T15:17:08.000+0100}, author = {Legoux, F P and Lim, J B and Cauley, A W and Dikiy, S and Ertelt, J and Mariani, T J and Sparwasser, T and Way, S S and Moon, J J}, biburl = {https://www.bibsonomy.org/bibtex/2b613e31ff67c43b460b0bd5536465065/sparwasser}, editor = {Immunity}, interhash = {3eeba328a963e1281dd5adce7c99975a}, intrahash = {b613e31ff67c43b460b0bd5536465065}, journal = {Immunity }, keywords = {sparwasser}, number = 5, pages = {896 - 908}, pubmedurl = {http://www.ncbi.nlm.nih.gov/pubmed/26572061}, timestamp = {2015-12-01T15:17:08.000+0100}, title = {CD4+ T Cell Tolerance to Tissue-Restricted Self Antigens Is Mediated by Antigen-Specific Regulatory T Cells Rather Than Deletion }, volume = 43, year = 2015 }