Coexpression of P2Y and P2U Receptors on Aortic Endothelial Cells : Comparison of Cell Localization and Signaling Pathways

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Circulation Research. 1995;76:191-198

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Coexpression of P_2Y and P_2U Receptors on Aortic Endothelial Cells

Comparison of Cell Localization and Signaling Pathways

Didier Communi, Eric Raspe, Sabine Pirotton, Jean-Marie Boeynaems

From the Institute of Interdisciplinary Research, School of Medicine, Université Libre de Bruxelles (Belgium).

Correspondence to Dr D. Communi, Institute of Interdisciplinary Research, Université Libre de Bruxelles, Campus Erasme, Building C, 808 Route de Lennik, 1070 Brussels, Belgium.

Abstract Depending on the vascular bed considered, the actionsof ATP on the endothelium are mediated by either P_2Y or P_2Ureceptors. The two types of receptors seem to coexist on bovineaortic endothelial cells, where they are both coupled to phospholipaseC. In this study, we have investigated whether they are trulycoexpressed on the same cells and whether their signaling pathwaysdiverge beyond phospholipase C activation. Measurements of [Ca²⁺]_iin single cells showed that almost all bovine aortic endothelialcells are responsive to both 2-methylthio-ATP (2MeSATP), anagonist of P_2Y receptors, and UTP, an agonist of P_2U receptors.UTP stimulated the release of prostacyclin from freshly isolatedbovine aortic endothelial cells, even when they were exposed tocycloheximide at the time of their collection: this indicatesthat P_2U receptors must already be expressed on endothelial cellsin situ and do not appear during cell culture. The time courseof inositol phosphate (InsP) accumulation and the relative proportionof Ins(1,4,5)P₃, Ins(1,3,4,5)P₄, and Ins(1,3,4)P₃ were similarin cells stimulated by 2MeSATP or UTP. UTP and 2MeSATP bothstimulated the hydrolysis of phosphatidylcholine by phospholipaseD, as reflected by the release of [³H]choline from prelabeledcells. The responses to both agents were blocked after downregulationof protein kinase C, resulting from a prolonged exposure tophorbol 12-myristate 13-acetate: this blockade occurred at astep distal to phospholipase C activation. A single differencebetween the two pathways has been identified: the effect of2MeSATP on InsP₃ was significantly more inhibited after a shortexposure to phorbol 12-myristate 13-acetate than that of UTP.This discrepancy is consistent with the involvement of distinctG proteins in the activation of phospholipase C by P_2Y and P_2Ureceptors.

Key Words: ATP • P₂ receptors • endothelial cells • inositol phosphates • choline

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				D. Communi, C. Govaerts, M. Parmentier, and J.-M. Boeynaems Cloning of a Human Purinergic P2Y Receptor Coupled to Phospholipase C and Adenylyl Cyclase J. Biol. Chem., December 19, 1997; 272(51): 31969 - 31973. [Abstract] [Full Text] [PDF]

				C. I. Seye, A.-P. Gadeau, D. Daret, F. Dupuch, P. Alzieu, L. Capron, and C. Desgranges Overexpression of the P2Y2 Purinoceptor in Intimal Lesions of the Rat Aorta Arterioscler. Thromb. Vasc. Biol., December 1, 1997; 17(12): 3602 - 3610. [Abstract] [Full Text]

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