TY - JOUR T1 - Nucleotides Acting at P2Y Receptors: Connecting Structure and Function JF - Molecular Pharmacology JO - Mol Pharmacol SP - 220 LP - 230 DO - 10.1124/mol.114.095711 VL - 88 IS - 2 AU - Kenneth A. Jacobson AU - Silvia Paoletta AU - Vsevolod Katritch AU - Beili Wu AU - Zhan-Guo Gao AU - Qiang Zhao AU - Raymond C. Stevens AU - Evgeny Kiselev Y1 - 2015/08/01 UR - http://molpharm.aspetjournals.org/content/88/2/220.abstract N2 - Eight G protein–coupled P2Y receptor (P2YR) subtypes are important physiologic mediators. The human P2YRs are fully activated by ATP (P2Y2 and P2Y11), ADP (P2Y1, P2Y12, and P2Y13), UTP (P2Y2 and P2Y4), UDP (P2Y6 and P2Y14), and UDP glucose (P2Y14). Their structural elucidation is progressing rapidly. The X-ray structures of three ligand complexes of the Gi-coupled P2Y12R and two of the Gq-coupled P2Y1Rs were recently determined and will be especially useful in structure-based ligand design at two P2YR subfamilies. These high-resolution structures, which display unusual binding site features, complement mutagenesis studies for probing ligand recognition and activation. The structural requirements for nucleotide agonist recognition at P2YRs are relatively permissive with respect to the length of the phosphate moiety, but less so with respect to base recognition. Nucleotide-like antagonists and partial agonists are also known for P2Y1, P2Y2, P2Y4, and P2Y12Rs. Each P2YR subtype has the ability to be activated by structurally bifunctional agonists, such as dinucleotides, typically, dinucleoside triphosphates or tetraphosphates, and nucleoside polyphosphate sugars (e.g., UDP glucose) as well as the more conventional mononucleotide agonists. A range of dinucleoside polyphosphates, from triphosphates to higher homologs, occurs naturally. Earlier modeling predictions of the P2YRs were not very accurate, but recent findings have provided much detailed structural insight into this receptor family to aid in the rational design of new drugs. ER -