Mycobacterium tuberculosis (Mtb) frequently establishes persistent infections that may be facilitated by mechanisms that dampen immunity. T regulatory (T reg) cells, a subset of CD4+ T cells that are essential for preventing autoimmunity, can also suppress antimicrobial immune responses. We use Foxp3-GFP mice to track the activity of T reg cells after aerosol infection with Mtb. We report that during tuberculosis, T reg cells proliferate in the pulmonary lymph nodes (pLNs), change their cell surface phenotype, and accumulate in the pLNs and lung at a rate parallel to the accumulation of effector T cells. In the Mtb-infected lung, T reg cells accumulate in high numbers in all sites where CD4+ T cells are found, including perivascular/peribronchiolar regions and within lymphoid aggregates of granulomas. To determine the role of T reg cells in the immune response to tuberculosis, we generated mixed bone marrow chimeric mice in which all cells capable of expressing Foxp3 expressed Thy1.1. When T reg cells were depleted by administration of anti-Thy1.1 before aerosol infection with Mtb, we observed ∼1 log less of colony-forming units of Mtb in the lungs. Thus, after aerosol infection, T reg cells proliferate and accumulate at sites of infection, and have the capacity to suppress immune responses that contribute to the control of Mtb.
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3 September 2007
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August 20 2007
Expansion and function of Foxp3-expressing T regulatory cells during tuberculosis
James P. Scott-Browne,
James P. Scott-Browne
1Department of Pediatrics
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Shahin Shafiani,
Shahin Shafiani
1Department of Pediatrics
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Glady's Tucker-Heard,
Glady's Tucker-Heard
1Department of Pediatrics
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Kumiko Ishida-Tsubota,
Kumiko Ishida-Tsubota
1Department of Pediatrics
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Jason D. Fontenot,
Jason D. Fontenot
2Department of Immunology,
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Alexander Y. Rudensky,
Alexander Y. Rudensky
2Department of Immunology,
3Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195
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Michael J. Bevan,
Michael J. Bevan
2Department of Immunology,
3Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195
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Kevin B. Urdahl
Kevin B. Urdahl
1Department of Pediatrics
2Department of Immunology,
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James P. Scott-Browne
1Department of Pediatrics
Shahin Shafiani
1Department of Pediatrics
Glady's Tucker-Heard
1Department of Pediatrics
Kumiko Ishida-Tsubota
1Department of Pediatrics
Jason D. Fontenot
2Department of Immunology,
Alexander Y. Rudensky
2Department of Immunology,
3Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195
Michael J. Bevan
2Department of Immunology,
3Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195
Kevin B. Urdahl
1Department of Pediatrics
2Department of Immunology,
CORRESPONDENCE Kevin B. Urdahl:[email protected]
Abbreviations used: ICOS, inducible costimulatory molecule; mLN, mesenteric LN; Mtb, Mycobacterium tuberculosis; pLN, pulmonary lymph node; RFP, red fluorescent protein.
J.P. Scott-Browne's present address is Integrated Dept. of Immunology, University of Colorado Health Sciences Center, National Jewish Medical Research Center, Denver, CO 80209.
Received:
October 02 2006
Accepted:
July 18 2007
Online ISSN: 1540-9538
Print ISSN: 0022-1007
The Rockefeller University Press
2007
J Exp Med (2007) 204 (9): 2159–2169.
Article history
Received:
October 02 2006
Accepted:
July 18 2007
Citation
James P. Scott-Browne, Shahin Shafiani, Glady's Tucker-Heard, Kumiko Ishida-Tsubota, Jason D. Fontenot, Alexander Y. Rudensky, Michael J. Bevan, Kevin B. Urdahl; Expansion and function of Foxp3-expressing T regulatory cells during tuberculosis . J Exp Med 3 September 2007; 204 (9): 2159–2169. doi: https://doi.org/10.1084/jem.20062105
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