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      Both retention and recirculation contribute to long-lived regulatory T-cell accumulation in the thymus.

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          Abstract

          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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          Author and article information

          Journal
          Eur. J. Immunol.
          European journal of immunology
          1521-4141
          0014-2980
          Sep 2014
          : 44
          : 9
          Affiliations
          [1 ] Department of Pathology and Laboratory Medicine, Perelman School of Medicine at the University of Pennsylvania, Philadelphia, PA, USA.
          Article
          NIHMS608094
          10.1002/eji.201444529
          4177035
          24894919
          f2bdc504-903a-42b4-89f2-d789014248f0
          © 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.
          History

          Cellular immunology,Regulatory T cells,Thymic recirculation,Thymic retention,Thymopoiesis

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