P2Y receptors (version 2019.4) in the IUPHAR/BPS Guide to Pharmacology Database

Author:

Abbracchio Maria-PiaORCID,Boeynaems Jean-Marie,Boyer José L.,Burnstock GeoffreyORCID,Ceruti StefaniaORCID,Fumagalli MartaORCID,Gachet ChristianORCID,Hills Rebecca,Humphries Robert G.,Inoue Kazu,Jacobson Kenneth A.ORCID,Kennedy CharlesORCID,King Brian F.,Lecca DavideORCID,Müller Christa E.,Miras-Portugal Maria Teresa,Ralevic Vera,Weisman Gary A.ORCID

Abstract

P2Y receptors (nomenclature as agreed by the NC-IUPHAR Subcommittee on P2Y Receptors [3, 5]) are activated by the endogenous ligands ATP, ADP, uridine triphosphate, uridine diphosphate and UDP-glucose. The relationship of many of the cloned receptors to endogenously expressed receptors is not yet established and so it might be appropriate to use wording such as 'uridine triphosphate-preferring (or ATP-, etc.) P2Y receptor' or 'P2Y1-like', etc., until further, as yet undefined, corroborative criteria can be applied [46, 109, 187, 375, 388].Clinically used drugs acting on these receptors include the dinucleoside polyphosphate diquafosol, agonist of the P2Y2 receptor subtype, approved in Japan for the management of dry eye disease [236], and the P2Y12 receptor antagonists prasugrel, ticagrelor and cangrelor, all approved as antiplatelet drugs [52, 316].

Publisher

Edinburgh University Library

Subject

General Medicine

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