Secretory Phospholipase A 2 Group V

Author:

Rosengren Birgitta1,Peilot Helena1,Umaerus Mia1,Jönsson-Rylander Ann-Cathrine1,Mattsson-Hultén Lillemor1,Hallberg Carina1,Cronet Philippe1,Rodriguez-Lee Mariam1,Hurt-Camejo Eva1

Affiliation:

1. From AstraZeneca (B.R., M.U., A.-C.J.-R., C.H., P.C., E.H.-C.), R&D, Molecular Pharmacology, Mölndal, Sweden; and Wallenberg Laboratory (H.P., L.M.-H., M.R.-L., E.H.-C.), Sahlgrenska University Hospital, Göteborg, Sweden.

Abstract

Objective— To study the distribution of group V secretory phospholipase A 2 (sPLA 2 ) in human and mouse lesions and compare its expression by human vascular cells, its activity toward lipoproteins, and the interaction with arterial proteoglycans (proteoglycans) with those of sPLA 2 -IIA. In addition, we also investigated the effect of a Western diet and lipopolysaccharide challenge on the aortic expression of these enzymes in mouse models. Methods and Results— Immunohistochemistry showed sPLA 2 -V in human and mouse lesions to be associated with smooth muscle cells and also surrounding foam cells in lipid core areas. mRNA of the enzyme was expressed in human lesions and human vascular cells, supporting the immunohistochemistry data. sPLA 2 -V but not sPLA 2 -IIA was active on lipoproteins in human serum. The association with proteoglycans enhanced 2- to 3-fold sPLA 2 -V activity toward low-density lipoproteins but not that of the group IIA enzyme. Experiments in mouse models showed that treatment with a Western diet induced expression of sPLA 2 -V but not that of sPLA 2 -IIA in aorta. On the other hand, lipopolysaccharide-induced acute inflammation augmented the expression of sPLA 2 -IIA but not that of sPLA 2 -V. Conclusions— These results indicate that these phospholipases could have different roles in atherosclerosis.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

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