Atherogenic properties of LDL particles modified by human group X secreted phospholipase A2 on human endothelial cell function

doi:10.1096/fj.06-6018fje

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Atherogenic properties of LDL particles modified by human group X secreted phospholipase A2 on human endothelial cell function

Sonia-Athina Karabina, Isabelle Brochériou, Gilles Le Naour, Monique Agrapart, Hervé Durand, Michael Gelb ${ddagger}$ , Gérard Lambeau, and Ewa Ninio

E-mail contact: akarampi@chups.jussieu.fr

Increasing evidence suggests that secreted phospholipases A2(sPLA2s) play an important role in the pathophysiology of atherosclerosis.Among sPLA2s, the human group X (hGX) enzyme has the highestcatalytic activity toward phosphatidylcholine, one of the majorphospholipid species of cell membranes and low-density lipoprotein(LDL). Our study examined the presence of hGX sPLA2 in humanatherosclerotic lesions and investigated the ability of hGXmodified LDL to alter human endothelial cell (HUVEC) function.Our results show that hGX sPLA2 is present in human atheroscleroticlesions and that the hydrolysis of LDL by hGX sPLA2 resultsin a modified particle that induces lipid accumulation in humanmonocyte-derived macrophages. Acting on endothelial cells, hGX-modifiedLDL activates the MAP kinase pathway, which leads to increasedarachidonic acid release, increased expression of adhesion moleculeson the surface of HUVEC, and increased adhesion of monocytesto HUVEC monolayers. Together, our data suggest that LDL modifiedby hGX, rather than hGX itself may have strong proinflammatoryand proatherogenic properties, which could play an importantrole in the propagation of atherosclerosis.--Karabina, S. A.,Brocheriou, I., Le Naour, G., Agrapart, M., Durand, H., Gelb,M., Lambeau, G., Ninio, E. Atherogenic properties of LDL particlesmodified by human group X secreted phospholipase A2 on humanendothelial cell function.

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