Publication | Open Access
Both retention and recirculation contribute to long‐lived regulatory <scp>T</scp>‐cell accumulation in the thymus
36
Citations
21
References
2014
Year
Lymphocyte DevelopmentT-regulatory CellImmunologyImmune RegulationRegulatory T CellsCellular PhysiologyTranscriptional RegulationCell RegulationNatural Treg CellsCellular Regulatory MechanismThymus BiologyCell SignalingRegulatory T Cell BiologyCell PhysiologyAutoimmunityT Cell ImmunityHumoral ImmunitySelf-toleranceTreg CellsTolerance InductionCell BiologyT Cell BiologyRecirculation ContributeSignal TransductionDevelopmental BiologyImmune Cell DevelopmentPhysiologyDevelopmental ImmunologyCellular Immune ResponsePeripheral Treg CellsMedicineCell Development
Natural Treg cells acquire their lineage-determining transcription factor Foxp3 during development in the thymus and are important in maintaining immunologic tolerance. Here, we analyzed the composition of the thymic Treg-cell pool using RAG2-GFP/FoxP3-RFP dual reporter mice and found that a population of long-lived GFP(-) Treg cells exists in the thymus. These long-lived Treg cells substantially increased with age, to a point where they represent >90% of the total thymic Treg-cell pool at 6 months of age. In contrast, long-lived conventional T cells remained at ∼ 15% of the total thymic pool at 6 months of age. Consistent with these studies, we noticed that host-derived Treg cells represented a large fraction (∼ 10%) of the total thymic Treg-cell pool in bone marrow chimeras, suggesting that long-lived Treg cells also reside in the thymus of these mice. The pool of long-lived Treg cells in the thymus was sustained by retention of Treg cells in the thymus and by recirculation of peripheral Treg cells back into the thymus. These long-lived thymic Treg cells suppressed T-cell proliferation to an equivalent extent to splenic Treg cells. Together, these data demonstrate that long-lived Treg cells accumulate in the thymus by both retention and recirculation.
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