Inflammatory arthritis and dermatitis in thymectomized, CD25+ cell-depleted adult mice

doi:10.1093/rheumatology/keh477

Rheumatology Advance Access originally published online on January 5, 2005
Rheumatology 2005 44(3):299-308; doi:10.1093/rheumatology/keh477

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Inflammatory arthritis and dermatitis in thymectomized, CD25⁺ cell-depleted adult mice

A. Loughry, S. Fairchild², N. Athanasou¹, J. Edwards¹ and F. C. Hall²

Weatherall Institute of Molecular Medicine, John Radcliffe Hospital, ¹ Nuffield Orthopaedic Centre, Oxford and ² Department of Clinical Medicine, Addenbrooke's Hospital, Cambridge, UK.

Correspondence to: F. C. Hall, Box 157, Department of Clinical Medicine, Addenbrooke's Hospital, Cambridge CB2 2QQ, UK. E-mail: fch22{at}medschl.cam.ac.uk

Objective. To investigate the effect of CD25⁺ or CTLA-4⁺ celldepletion on the natural history of collagen-induced and spontaneousarthritis in male DBA1/J mice.

Methods. Male DBA/1J mice were treated with anti-CD25 depletingantibody (PC61) or isotype control (GL113), or with anti-CTLA-4depleting antibody (4F10) at various time-points peri- and post-immunizationwith bovine collagen type II, emulsified in adjuvant. In orderto develop a model system in which long-term depletion of CD25⁺regulatory T cells can be achieved prior to immunization, adultmale DBA/1J mice were thymectomized prior to administrationof either PC61 or GL113. An ELISA demonstrated that PC61 andGL113 antibodies were undetectable by 21 days after administrationand FACS analysis confirmed the long-term depletion of CD25⁺cells in peripheral blood.

Results. In the thymectomized mice treated with PC61, the CD25⁺population was depleted and a spontaneous arthritis developed(P = 0.03). In the non-thymectomized mice, administration ofCTLA-4-depleting antibody prior to immunization exacerbatedarthritis in mice immunized with bovine collagen type II emulsifiedin incomplete Freund's adjuvant (P<0.01). However, no significantdifference in the natural history of arthritis was evident inmice treated with CD25-depleting antibody (PC61) compared withcontrol antibody (GL113).

Conclusions. Two separate models implicate CD25⁺ CTLA-4⁺ constitutivecells in suppression of arthritis in susceptible DBA/1 males:exacerbation of collagen-induced arthritis following CTLA-4depletion at the start of induction and spontaneous arthritisin the thymectomy/CD25⁺ depletion model.

KEY WORDS: Inflammatory arthritis, Dermatitis, CD25, Thymectomy, Mice

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