Litcius/Paper detail

B7-CD28 co-stimulation modulates central tolerance via thymic clonal deletion and Treg generation through distinct mechanisms

Masashi Watanabe, Ying Lü, Michael Breen, Richard J. Hodes

2020Nature Communications42 citationsDOIOpen Access PDF

Abstract

The molecular and cellular mechanisms mediating thymic central tolerance and prevention of autoimmunity are not fully understood. Here we show that B7-CD28 co-stimulation and B7 expression by specific antigen-presenting cell (APC) types are required for clonal deletion and for regulatory T (Treg) cell generation from endogenous tissue-restricted antigen (TRA)-specific thymocytes. While B7-CD28 interaction is required for both clonal deletion and Treg induction, these two processes differ in their CD28 signaling requirements and in their dependence on B7-expressing dendritic cells, B cells, and thymic epithelial cells. Meanwhile, defective thymic clonal deletion due to altered B7-CD28 signaling results in the accumulation of mature, peripheral TRA-specific T cells capable of mediating destructive autoimmunity. Our findings thus reveal a function of B7-CD28 co-stimulation in shaping the T cell repertoire and limiting autoimmunity through both thymic clonal deletion and Treg cell generation.

Topics & Concepts

AutoimmunityClonal deletionCD28BiologyCentral toleranceCell biologyImmunologyPeripheral toleranceCo-stimulationImmune toleranceT cellT-cell receptorAntigenImmune systemT-cell and B-cell ImmunologyImmunotherapy and Immune ResponsesImmune Cell Function and Interaction
B7-CD28 co-stimulation modulates central tolerance via thymic clonal deletion and Treg generation through distinct mechanisms | Litcius