Lysophosphatidic acid triggers mast cell-driven atherosclerotic plaque destabilization by increasing vascular inflammation

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DOI http://dx.doi.org/10.1194/jlr.M032862
Reference M. Bot, S.C.A. de Jager, L. MacAleese, H.M. Lagraauw, T.J.C. van Berkel, P.H.A. Quax, J. Kuiper, E.A.L. Biessen, I. Bota and R.M.A. Heeren, Lysophosphatidic acid triggers mast cell-driven atherosclerotic plaque destabilization by increasing vascular inflammation, J. Lipid Res. 54, 1265-1274 (2013)

Lysophosphatidic acid (LPA), a bioactive lysophospholipid, accumulates in the atherosclerotic plaque. It has the capacity to activate mast cells, which potentially exacerbates plaque progression. In this study, we thus aimed to investigate whether LPA contributes to plaque destabilization by modulating mast cell function. Methods and Results: We here show by an imaging mass spectrometry approach that several LPA species are present in atherosclerotic plaques. Subsequently, we demonstrate that LPA is a potent mast cell activator, which unlike other triggers favor release of tryptase. Local perivascular administration of LPA to an atherosclerotic carotid artery segment increases the activation status of perivascular mast cells and promotes intraplaque hemorrhage, macrophage recruitment, without impacting plaque cell apoptosis. The mast cell stabilizer cromolyn could prevent intraplaque hemorrhage elicited by LPA-mediated mast cell activation. Finally, the involvement of mast cells in these events was further emphasized by the lack of effect of perivascular LPA administration in mast cell deficient animals. Conclusions: We demonstrate that increased accumulation of LPA in plaques induces perivascular mast cell activation and in this way contribute to plaque destabilization in vivo. This study points to local LPA availability as an important factor in atherosclerotic plaque stability.