Interleukin-6 modulates production of T lymphocyte-derived cytokines in antigen-induced arthritis and drives inflammation-induced osteoclastogenesis

Wong, PKK; Quinn, JMW; Sims, NA; van Nieuwenhuijze, Annemarie; Campbell, IK; Wicks, IP

doi:10.1002/art.21537

Interleukin-6 modulates production of T lymphocyte-derived cytokines in antigen-induced arthritis and drives inflammation-induced osteoclastogenesis

Author:

Wong, PKK

Quinn, JMW ; Sims, NA ; van Nieuwenhuijze, Annemarie ; Campbell, IK ; Wicks, IP

Keywords:

Science & Technology, Life Sciences & Biomedicine, Rheumatology, NF-KAPPA-B, MONOCLONAL-ANTIBODY TREATMENT, COLLAGEN-INDUCED ARTHRITIS, LEUKEMIA INHIBITORY FACTOR, NECROSIS-FACTOR-ALPHA, RHEUMATOID-ARTHRITIS, RECEPTOR ACTIVATOR, BONE-RESORPTION, ONCOSTATIN-M, OSTEOPROTEGERIN LIGAND, Animals, Antigens, Arthritis, Cytokines, Interleukin-6, Mice, Osteoclasts, T-Lymphocytes

Abstract:

OBJECTIVE: To determine the cellular mediators of antigen-induced arthritis (AIA) and the relative contribution of members of the interleukin-6 (IL-6) family and tumor necrosis factor (TNF) in AIA. METHODS: AIA was induced in mice deficient in T and B lymphocytes, IL-6 (IL-6(-/-)), TNF (TNF(-/-)), IL-11 receptor, and oncostatin M receptor, by immunization with methylated bovine serum albumin (mBSA) followed 7 days later by intraarticular injection of mBSA. Arthritis severity was assessed histologically, and T lymphocyte responses were assessed in vitro. Anti-TNF neutralizing antibody was administered to wild-type mice during AIA. Bone marrow osteoclasts were generated in vitro via culture with RANKL and macrophage colony-stimulating factor. RESULTS: AIA was dependent on CD4+ T lymphocytes, but not CD8+ T lymphocytes or B cells. IL-6(-/-) mice had reduced AIA severity and fewer osteoclasts at sites of bone erosion. This protective effect was not seen with a deficiency of other IL-6 family members and was similar to that in TNF(-/-) mice or wild-type mice receiving TNF blockade treatment. IL-6(-/-) CD4+ T lymphocytes from draining lymph nodes had reduced antigen-induced proliferation and produced less IL-17 and less RANKL, relative to osteoprotegerin, than cells from wild-type mice. Bone marrow from IL-6(-/-) mice generated fewer osteoclasts in vitro than bone marrow from either wild-type or TNF(-/-) mice. CONCLUSION: AIA is driven by CD4+ T lymphocytes. IL-6 is an important mediator of bone destruction in AIA because it regulates T lymphocyte production of key osteoclastogenic cytokines and inflammation-induced bone marrow osteoclast differentiation. These findings have implications for reducing bone and joint damage in rheumatoid arthritis.