The origin of thymic CD4+CD25+ regulatory T cells and their co-stimulatory requirements are determined after elimination of recirculating peripheral CD4+ cells

doi:10.1093/intimm/dxm010

International Immunology Advance Access originally published online on February 20, 2007
International Immunology 2007 19(4):455-463; doi:10.1093/intimm/dxm010

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The origin of thymic CD4⁺CD25⁺ regulatory T cells and their co-stimulatory requirements are determined after elimination of recirculating peripheral CD4⁺ cells

Yifan Zhan, Dorothee Bourges, James A. Dromey, Leonard C. Harrison and Andrew M. Lew

Autoimmunity and Transplantation Division, Walter and Eliza Hall Institute of Medical Research, 1G Royal Parade, Parkville, Victoria 3050, Australia

Correspondence to: Y. Zhan; E-mail: zhan{at}wehi.edu.au or A. M. Lew; E-mail: lew{at}wehi.edu.au

Studies on the thymic ontogeny of naturally arising CD4⁺CD25⁺regulatory T cells (TR cells) are complicated by the contaminationof recirculating cells from the periphery (both activated CD4⁺T and TR cells). We investigated TR cells in anti-CD4 antibodytransgenic (Tg) (GK) mice that continuously deplete peripheralCD4 T cells but not thymocytes so that the generation of thymicTR cells and their developmental requirement can be accuratelyassessed. We show that in the thymuses of mice that lack peripheralCD4⁺ cells, TR cells were present but were fewer in number comparedwith wild-type (WT) mice. Therefore, we show that peripheralTR cells do re-enter the thymus, comprising 20% of TR cellsin the normal thymus. TR cells from both WT and GK mice expressedFoxp3 and GITR, and suppressed the proliferation of CD25^–CD4⁺T cells. Furthermore, the co-stimulation requirements for TRgeneration were evaluated in mice with or without peripheralCD4 cells. Splenic TR cells in CD40L^–/– mice andCTLA4Ig Tg mice were fewer compared with WT mice. Mice deficientin both co-stimulatory pathways had further reduction in splenicTR cells. Unlike the periphery, the reduction in thymic TR cellswas only seen for CD40L^–/– but not for CTLA4Ig Tgmice. Therefore, we found that the co-stimulation requirementsfor the thymic development of TR cells differed from those forperipheral homeostasis.

Keywords: CD4⁺CD25⁺ regulatory T cells, costimulation, thymus, tolerance, transcription factor Foxp3

Transmitting editor: A. Cooke

Received 6 September 2006, accepted 18 January 2007.

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