How selective antagonists and genetic modification have helped characterise the expression and functions of vascular P2Y receptors

Markie O Dales; Robert M Drummond; Charles Kennedy

doi:10.1007/s11302-024-10016-z

How selective antagonists and genetic modification have helped characterise the expression and functions of vascular P2Y receptors

Purinergic Signal. 2024 May 13. doi: 10.1007/s11302-024-10016-z. Online ahead of print.

Authors

Markie O Dales¹, Robert M Drummond¹, Charles Kennedy²

Affiliations

¹ Strathclyde Institute of Pharmacy & Biomedical Sciences, University of Strathclyde, 161 Cathedral Street, Glasgow, G4 0RE, UK.
² Strathclyde Institute of Pharmacy & Biomedical Sciences, University of Strathclyde, 161 Cathedral Street, Glasgow, G4 0RE, UK. c.kennedy@strath.ac.uk.

PMID: 38740733
DOI: 10.1007/s11302-024-10016-z

Abstract

Vascular P2Y receptors mediate many effects, but the role of individual subtypes is often unclear. Here we discuss how subtype-selective antagonists and receptor knockout/knockdown have helped identify these roles in numerous species and vessels. P2Y₁ receptor-mediated vasoconstriction and endothelium-dependent vasodilation have been characterised using the selective antagonists, MRS2179 and MRS2216, whilst AR-C118925XX, a P2Y₂ receptor antagonist, reduced endothelium-dependent relaxation, and signalling evoked by UTP or fluid shear stress. P2Y₂ receptor knockdown reduced endothelial signalling and endothelial P2Y₂ receptor knockout produced hypertensive mice and abolished vasodilation elicited by an increase in flow. UTP-evoked vasoconstriction was also blocked by AR-C118925XX, but the effects of P2Y₂ receptor knockout were complex. No P2Y₄ receptor antagonists are available and P2Y₄ knockout did not affect the vascular actions of UTP and UDP. The P2Y₆ receptor antagonist, MRS2578, identified endothelial P2Y₆ receptors mediating vasodilation, but receptor knockout had complex effects. MRS2578 also inhibited, and P2Y₆ knockout abolished, contractions evoked by UDP. P2Y₆ receptors contribute to the myogenic tone induced by a stepped increase in vascular perfusion pressure and possibly to the development of atherosclerosis. The P2Y₁₁ receptor antagonists, NF157 and NF340, inhibited ATP-evoked signalling in human endothelial cells. Vasoconstriction mediated by P2Y₁₂/P2Y₁₃ and P2Y₁₄ receptors was characterised using the antagonists, cangrelor, ticagrelor, AR-C67085 and MRS2211 or PPTN respectively. This has yet to be backed up by receptor knockout experiments. Thus, subtype-selective antagonists and receptor knockout/knockdown have helped identify which P2Y subtypes are functionally expressed in vascular smooth muscle and endothelial cells and the effects that they mediate.

Keywords: AR-C118925XX; Atherosclerosis; Cangrelor; Hypertension; MRS2179; MRS2578; NF340; P2Y receptor; PPTN; Vasoconstriction; Vasodilation.

Publication types

Review