To further investigate the effects of interleukin‐1 (IL‐1) in immune‐mediated joint inflammation, we examined the role of IL‐2, Th1 interferon‐γ (IFNγ), and Th2 (IL‐4) cytokines, joint macrophages, and macrophage‐derived cytokines (IL‐12 p40, IL‐6, leukemia inhibitory factor [LIF], oncostatin M [OSM], and granulocyte–macrophage colony‐stimulating factor [GM‐CSF]) in a CD4+ T lymphocyte–dependent model of acute arthritis.

Methylated bovine serum albumin (mBSA)/IL‐1–induced arthritis was elicited in wild‐type, gene‐knockout, and monoclonal antibody–treated mice. Synovial lining macrophages were selectively depleted by intraarticular injection of clodronate liposomes prior to disease induction. The severity of arthritis was assessed histologically.

Mice deficient in IL‐2 were almost completely protected from arthritis, and neutralization of IL‐4 reduced the severity of disease. In contrast, arthritis severity and resolution appeared to be independent of IFNγ. Synovial lining macrophage depletion markedly reduced arthritis severity. IL‐6 or LIF deficiency was only modestly protective, although as previously reported, GM‐CSF deficiency conferred profound disease resistance. IL‐12 p40–deficient mice (which lack IL‐12 and IL‐23) and OSM receptor–deficient mice were susceptible to mBSA/IL‐1–induced arthritis.

Acute mBSA/IL‐1–induced arthritis is dependent on IL‐2 and IL‐4, but not IFNγ. In vivo, the Th1/Th2 paradigm may be distorted by the presence of macrophage‐derived cytokines such as IL‐1. Synovial lining macrophages are essential in mBSA/IL‐1–induced arthritis. However, the requirement for macrophage‐derived cytokines is selective; that is, IL‐6, LIF, and especially GM‐CSF are necessary, but IL‐12, IL‐23, and OSM are dispensable. IL‐1 may therefore influence both adaptive and innate immune mechanisms in acute inflammatory arthritis.