Mast cells promote atherosclerosis by releasing proinflammatory cytokines

doi:doi:10.1038/nm1601

Mast cells contribute importantly to allergic and innate immune responses by releasing various preformed and newly synthesized mediators^1,². Previous studies have shown mast cell accumulation in human atherosclerotic lesions³. This report establishes the direct participation of mast cells in atherogenesis in low-density lipoprotein receptor–deficient (Ldlr^-/-) mice⁴. Atheromata from compound mutant Ldlr^-/- Kit^W-sh^/W-sh mice⁵ showed decreased lesion size, lipid deposition, T-cell and macrophage numbers, cell proliferation and apoptosis, but increased collagen content and fibrous cap development. In vivo, adoptive transfer of syngeneic wild-type or tumor necrosis factor (TNF)- alpha -deficient mast cells restored atherogenesis to Ldlr^-/-Kit^W-sh/W-sh mice. Notably, neither interleukin (IL)-6- nor interferon (IFN)- gamma -deficient mast cells did so, indicating that the inhibition of atherogenesis in Ldlr^-/-Kit^W-sh/W-sh mice resulted from the absence of mast cells and mast cell–derived IL-6 and IFN- gamma . Compared with wild-type or TNF- alpha -deficient mast cells, those lacking IL-6 or IFN- gamma did not induce expression of proatherogenic cysteine proteinase cathepsins from vascular cells in vitro or affect cathepsin and matrix metalloproteinase activities in atherosclerotic lesions, implying that mast cell–derived IL-6 and IFN- gamma promote atherogenesis by augmenting the expression of matrix-degrading proteases. These observations establish direct participation of mast cells and mast cell–derived IL-6 and IFN- gamma in mouse atherogenesis and provide new mechanistic insight into the pathogenesis of this common disease.

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