CCR7 Controls Thymus Recirculation, but Not Production and Emigration, of Foxp3+ T Cells
Summary: Current models of Foxp3+ regulatory T cell (Treg) development involve CCR7-mediated migration of thymocytes into the thymus medulla to enable essential interactions with medullary epithelium. However, increased Foxp3+ thymic Treg numbers in Ccr7−/− mice challenge this view, and the role of...
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doaj-a3f7e5b6fef74e41aca77d559c4a14142020-11-24T21:54:08ZengElsevierCell Reports2211-12472016-02-0114510411048CCR7 Controls Thymus Recirculation, but Not Production and Emigration, of Foxp3+ T CellsJennifer E. Cowan0Nicholas I. McCarthy1Graham Anderson2MRC Centre for Immune Regulation, Institute for Immunology and Immunotherapy, University of Birmingham, Birmingham B15 2TT, UKMRC Centre for Immune Regulation, Institute for Immunology and Immunotherapy, University of Birmingham, Birmingham B15 2TT, UKMRC Centre for Immune Regulation, Institute for Immunology and Immunotherapy, University of Birmingham, Birmingham B15 2TT, UK; Corresponding authorSummary: Current models of Foxp3+ regulatory T cell (Treg) development involve CCR7-mediated migration of thymocytes into the thymus medulla to enable essential interactions with medullary epithelium. However, increased Foxp3+ thymic Treg numbers in Ccr7−/− mice challenge this view, and the role of CCR7 in Treg development, emigration, and/or recirculation is unknown. Here, we have examined CCR7 and Rag2pGFP levels during Treg development and generated Rag2pGFPCcr7−/− mice to study its impact on the intrathymic Treg pool. We reveal surprising developmental heterogeneity in thymocytes described as Treg precursors, showing that they contain recirculating CCR6+CCR7−Rag2pGFP− T cells. Although CCR7 defines bona fide Rag2GFP+ Treg precursors, it is not required for Treg production and emigration. Rather, we show that lack of CCR7 renders the thymus more receptive to Treg thymus homing. Our study reveals a role for CCR7 in limiting Treg recirculation back to the thymus and enables separation of the mechanisms controlling Treg production and thymic recirculation. : Current models of Foxp3+ Treg development indicate that CCR7 controls thymus medulla entry for Treg precursor generation. By redefining newly produced Treg precursors, Cowan et al. show that, while CCR7 is dispensable for Treg development, it influences the intrathymic Treg pool by rate-limiting peripheral Treg recirculation back to the thymus.http://www.sciencedirect.com/science/article/pii/S2211124716000073 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Jennifer E. Cowan Nicholas I. McCarthy Graham Anderson |
spellingShingle |
Jennifer E. Cowan Nicholas I. McCarthy Graham Anderson CCR7 Controls Thymus Recirculation, but Not Production and Emigration, of Foxp3+ T Cells Cell Reports |
author_facet |
Jennifer E. Cowan Nicholas I. McCarthy Graham Anderson |
author_sort |
Jennifer E. Cowan |
title |
CCR7 Controls Thymus Recirculation, but Not Production and Emigration, of Foxp3+ T Cells |
title_short |
CCR7 Controls Thymus Recirculation, but Not Production and Emigration, of Foxp3+ T Cells |
title_full |
CCR7 Controls Thymus Recirculation, but Not Production and Emigration, of Foxp3+ T Cells |
title_fullStr |
CCR7 Controls Thymus Recirculation, but Not Production and Emigration, of Foxp3+ T Cells |
title_full_unstemmed |
CCR7 Controls Thymus Recirculation, but Not Production and Emigration, of Foxp3+ T Cells |
title_sort |
ccr7 controls thymus recirculation, but not production and emigration, of foxp3+ t cells |
publisher |
Elsevier |
series |
Cell Reports |
issn |
2211-1247 |
publishDate |
2016-02-01 |
description |
Summary: Current models of Foxp3+ regulatory T cell (Treg) development involve CCR7-mediated migration of thymocytes into the thymus medulla to enable essential interactions with medullary epithelium. However, increased Foxp3+ thymic Treg numbers in Ccr7−/− mice challenge this view, and the role of CCR7 in Treg development, emigration, and/or recirculation is unknown. Here, we have examined CCR7 and Rag2pGFP levels during Treg development and generated Rag2pGFPCcr7−/− mice to study its impact on the intrathymic Treg pool. We reveal surprising developmental heterogeneity in thymocytes described as Treg precursors, showing that they contain recirculating CCR6+CCR7−Rag2pGFP− T cells. Although CCR7 defines bona fide Rag2GFP+ Treg precursors, it is not required for Treg production and emigration. Rather, we show that lack of CCR7 renders the thymus more receptive to Treg thymus homing. Our study reveals a role for CCR7 in limiting Treg recirculation back to the thymus and enables separation of the mechanisms controlling Treg production and thymic recirculation. : Current models of Foxp3+ Treg development indicate that CCR7 controls thymus medulla entry for Treg precursor generation. By redefining newly produced Treg precursors, Cowan et al. show that, while CCR7 is dispensable for Treg development, it influences the intrathymic Treg pool by rate-limiting peripheral Treg recirculation back to the thymus. |
url |
http://www.sciencedirect.com/science/article/pii/S2211124716000073 |
work_keys_str_mv |
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