Neutrophil-derived leukotriene B4 is required for inflammatory arthritis

M Chen, BK Lam, Y Kanaoka, PA Nigrovic… - The Journal of …, 2006 - rupress.org
M Chen, BK Lam, Y Kanaoka, PA Nigrovic, LP Audoly, KF Austen, DM Lee
The Journal of experimental medicine, 2006rupress.org
Neutrophils serve as a vanguard of the acute innate immune response to invading
pathogens. Neutrophils are also abundant at sites of autoimmune inflammation, such as the
rheumatoid joint, although their pathophysiologic role is incompletely defined and relevant
effector functions remain obscure. Using genetic and pharmacologic approaches in the
K/BxN serum transfer model of arthritis, we find that autoantibody-driven erosive synovitis is
critically reliant on the generation of leukotrienes, and more specifically on leukotriene B4 …
Neutrophils serve as a vanguard of the acute innate immune response to invading pathogens. Neutrophils are also abundant at sites of autoimmune inflammation, such as the rheumatoid joint, although their pathophysiologic role is incompletely defined and relevant effector functions remain obscure. Using genetic and pharmacologic approaches in the K/BxN serum transfer model of arthritis, we find that autoantibody-driven erosive synovitis is critically reliant on the generation of leukotrienes, and more specifically on leukotriene B4 (LTB4), for disease induction as well as perpetuation. Pursuing the cellular source for this mediator, we find via reconstitution experiments that mast cells are a dispensable source of leukotrienes, whereas arthritis susceptibility can be restored to leukotriene-deficient mice by intravenous administration of wild-type neutrophils. These experiments demonstrate a nonredundant role for LTB4 in inflammatory arthritis and define a neutrophil mediator involved in orchestrating the synovial eruption.
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