Direct presentation of inflammation-associated self-antigens by thymic innate-like T cells induces elimination of autoreactive CD8+ thymocytes

Author:

You Yuanyuan,Dunst Josefine,Ye Kewei,Sandoz Patrick A.ORCID,Reinhardt Annika,Sandrock Inga,Comet Natalia R.,Sarkar Rupak DeyORCID,Yang EmilyORCID,Duprez EstelleORCID,Agudo Judith,Brown Brian D.ORCID,Utz Paul J.ORCID,Kastenmüller WolfgangORCID,Gerlach CarmenORCID,Prinz Immo,Önfelt BjörnORCID,Kreslavsky TarasORCID

Abstract

AbstractUpregulation of diverse self-antigens that constitute components of the inflammatory response overlaps spatially and temporally with the emergence of pathogen-derived foreign antigens. Therefore, discrimination between these inflammation-associated self-antigens and pathogen-derived molecules represents a unique challenge for the adaptive immune system. Here, we demonstrate that CD8+ T cell tolerance to T cell-derived inflammation-associated self-antigens is efficiently induced in the thymus and supported by redundancy in cell types expressing these molecules. In addition to thymic epithelial cells, this included thymic eosinophils and innate-like T cells, a population that expressed molecules characteristic for all major activated T cell subsets. We show that direct T cell-to-T cell antigen presentation by minute numbers of innate-like T cells was sufficient to eliminate autoreactive CD8+ thymocytes. Tolerance to such effector molecules was of critical importance, as its breach caused by decreased thymic abundance of a single model inflammation-associated self-antigen resulted in autoimmune elimination of an entire class of effector T cells.

Funder

Cancerfonden

Barncancerfonden

Radiumhemmets Forskningsfonder

China Scholarship Council

Deutsche Forschungsgemeinschaft

Publisher

Springer Science and Business Media LLC

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