Journal
IMMUNOLOGY AND CELL BIOLOGY
Volume 100, Issue 3, Pages 205-217Publisher
WILEY
DOI: 10.1111/imcb.12520
Keywords
ICOS; ICOSL; negative selection; thymocytes; thymic antigen-presenting cells
Categories
Funding
- Canadian Institutes for Health Research (CIHR) [PJT-168862, PJT-159526]
- Fonds de la recherche en sante du Quebec (FRQ-S)
- L'Oreal-UNESCO For Women in Science
- NSERC graduate fellowship
- FRQ-S
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Negative selection is an important process for T-cell tolerance, and ICOS may play a role in fine-tuning T-cell receptor signals during thymic selection.
Negative selection of developing T cells plays a significant role in T-cell tolerance to self-antigen. This process relies on thymic antigen-presenting cells which express both self-antigens and cosignaling molecules. Inducible T-cell costimulator (ICOS) belongs to the CD28 family of cosignaling molecules and binds to ICOS ligand (ICOSL). The ICOS signaling pathway plays important roles in shaping the immune response to infections, but its role in central tolerance is less well understood. Here we show that ICOSL is expressed by subsets of thymic dendritic cells and medullary thymic epithelial cells as well as thymic B cells. ICOS expression is upregulated as T cells mature in the thymus and correlates with T-cell receptor signal strength during thymic selection. We also provide evidence of a role for ICOS signaling in mediating negative selection. Our findings suggest that ICOS may fine-tune T-cell receptor signals during thymic selection contributing to the generation of a tolerant T-cell population.
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