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Antigen-specific MAIT cell subsets involved in TB immunity (INC2P.420)
Mucosal associated invariant T (MAIT) cells have a semi-invariant TCRVα chain, and depend on riboflavin metabolites (ribityllumazines, RLAg) produced by commensal flora and presented by the nonpolymorphic class Ib molecule MR1 for optimal development. We used MR1/RLAg tetramers and TCR Vα19 transgen...
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Published in: | The Journal of immunology (1950) 2015-05, Vol.194 (1_Supplement), p.55-55.14 |
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Main Authors: | , , , , , , , , , , , |
Format: | Article |
Language: | English |
Online Access: | Get full text |
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Summary: | Mucosal associated invariant T (MAIT) cells have a semi-invariant TCRVα chain, and depend on riboflavin metabolites (ribityllumazines, RLAg) produced by commensal flora and presented by the nonpolymorphic class Ib molecule MR1 for optimal development. We used MR1/RLAg tetramers and TCR Vα19 transgenic mice to study MR1-dependency, subset heterogeneity and protective effector functions important for tuberculosis (TB) immunity. We found that Vβ6/8+NK1.1+ MAIT cell subsets maximally expand peripherally in mice expressing MR1. In addition, we show that MR1/RLAg tetramer+ MAIT cells expressing CD4, CD8 or neither contain populations variably co-expressing Vβ6/8 and/or NK1.1, indicating that MAIT cells are more heterogeneous than previously thought. Furthermore, NK1.1 (NKR-P1C) is minimally expressed on mature Vβ6/8+ tetramer+ MAIT cells in the thymus but progressively increases with peripheral activation. Importantly, after virulent mycobacterial pulmonary infection, heterogeneous subsets of tetramer+ MAIT cells (CD4-CD8->CD4-CD8+>CD4+CD8-) co-expressing Vβ6/8 and NK1.1 and the homing molecules α4β1 and CXCR3, were recruited into the lungs and afforded maximal early protection in MR1-sufficient mice. Surprisingly, MAIT cells developing in the absence of MR1 were partially protective. Overall, we demonstrate diversity of MAIT cells, evidence that NK1.1 is an activation rather than developmental MAIT cell marker, and also that MAIT cells are important for TB protective immunity. |
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ISSN: | 0022-1767 1550-6606 |
DOI: | 10.4049/jimmunol.194.Supp.55.14 |