Amelioration of arthritis through mobilization of peptide-specific CD8+ regulatory T cells
Jianmei W. Leavenworth, … , Xiaoyang Wang, Harvey Cantor
Jianmei W. Leavenworth, … , Xiaoyang Wang, Harvey Cantor
Published February 8, 2013
Citation Information: J Clin Invest. 2013;123(3):1382-1389. https://doi.org/10.1172/JCI66938.
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Research Article Inflammation

Amelioration of arthritis through mobilization of peptide-specific CD8+ regulatory T cells

Abstract

Current therapies to treat autoimmune disease focus mainly on downstream targets of autoimmune responses, including effector cells and cytokines. A potentially more effective approach would entail targeting autoreactive T cells that initiate the disease cascade and break self tolerance. The murine MHC class Ib molecule Qa-1b (HLA-E in humans) exhibits limited polymorphisms and binds to 2 dominant self peptides: Hsp60p216 and Qdm. We found that peptide-induced expansion of tetramer-binding CD8+ Tregs that recognize Qa-1–Hsp60p216 but not Qa-1–Qdm strongly inhibited collagen-induced arthritis, an animal model of human rheumatoid arthritis. Perforin-dependent elimination of autoreactive follicular Th (TFH) and Th17 cells by CD8+ Tregs inhibited disease development. Infusion of in vitro–expanded CD8+ Tregs increased the efficacy of methotrexate treatment and halted disease progression after clinical onset, suggesting an alternative approach to this first-line treatment. Moreover, infusion of small numbers of Qa-1–Hsp60p216–specific CD8+ Tregs resulted in robust inhibition of autoimmune arthritis, confirming the inhibitory effects of Hsp60p216 peptide immunization. These results suggest that strategies designed to expand Qa-1–restricted (HLA-E–restricted), peptide-specific CD8+ Tregs represent a promising therapeutic approach to autoimmune disorders.

Authors

Jianmei W. Leavenworth, Xiaolei Tang, Hye-Jung Kim, Xiaoyang Wang, Harvey Cantor

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Figure 1

Selective expansion of Hsp60p216-specific Qa-1–restricted CD8+ Tregs inhibits arthritis.

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Selective expansion of Hsp60p216-specific Qa-1–restricted CD8+ Tregs inh...
(A) Arthritis was induced in B6 mice as described in Methods. Irradiated LPS-activated Kb–/–Db–/– BM-derived DCs were loaded with or without Hsp60p216 or Qdm peptide and injected subcutaneously (6 × 105/ mouse) at the tail base at day 27, day 36, and day 49 (diamonds). Arthritis scores are shown for 5–6 mice per group. The group injected with DCs alone versus the group given Hsp60p216-loaded DCs differed significantly. *P < 0.05. (B) Flow cytometry of dLN cells from CII-immune B6 mice injected with DC-pulsed peptides as in A, after incubation with Qa-1 tetramers labeled with phycoerythrin (Tet-PE) or allophycocyanin (Tet-APC); analysis is shown before and after enrichment by magnetic bead columns for tet+ CD8+ cells. Numbers in plots before enrichment and after enrichment (upper left quadrant) indicate percentage of tet+ CD8+ cells. (C) B6 mice were immunized with either unpulsed Kb–/–Db–/– DCs or DCs that had been loaded with the indicated peptide as described in A. CD8+ cells from dLNs from each group were analyzed at day 42 for binding to Qa-1.R72A–Qdm-tetramer or Qa-1–Hsp60p216-tetramer. Representative FACS plots are shown. Gates represent percentages of tet+ CD8+ cells. (D) The percentages and numbers of Hsp60p216-tet+ CD8+ cells that expressed the CD122+Ly49+ surface profile and CD122+Ly49 surface profile are shown. *P < 0.05.