The identification of 4,7-disubstituted naphthoic acid derivatives as UDP-competitive antagonists of P2Y14

The identification of 4,7-disubstituted naphthoic acid derivatives as UDP-competitive antagonists of P2Y14

A weak, UDP-competitive antagonist of the pyrimidinergic receptor P2RY(14) with a naphthoic acid core was identified through high-throughput screening. Optimization provided compounds with improved potency but poor pharmacokinetics. Acylglucuronidation was determined to be the major route of metabol...

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Veröffentlicht in:Bioorganic & medicinal chemistry letters 2011-05, Vol.21 (10), p.2836-2839
Hauptverfasser: YVES GAUTHIER, Jacques, BELLEY, Michel, LAVALLEE, Geneviève, LEVESQUE, Jean-François, LIANHAI LI, MAMANE, Yael, MANCINI, Joseph, MORIN, Nicolas, MULROONEY, Erin, ROBICHAUD, Joel, THERIEN, Michel, TRANMER, Geoffrey, DESCHENES, Denis, ZHAOYIN WANG, JIN WU, BLACK, W. Cameron, FOURNIER, Jean-François, GAGNE, Sébastien, GAREAU, Yves, HAMEL, Martine, HENAULT, Martin, HYJAZIE, Huda, KARGMAN, Stacia
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Binding, Competitive
Biological and medical sciences
Carboxylic Acids - chemical synthesis
Carboxylic Acids - chemistry
Carboxylic Acids - pharmacokinetics
Carboxylic Acids - pharmacology
Medical sciences
Mice
Molecular Structure
Naphthalenes - chemical synthesis
Naphthalenes - chemistry
Naphthalenes - pharmacokinetics
Naphthalenes - pharmacology
Neuropharmacology
Neurotransmitters. Neurotransmission. Receptors
Pan troglodytes
Peptidergic system (neuropeptide, opioid peptide, opiates...). Adenosinergic and purinergic systems
Pharmacology. Drug treatments
Protein Binding - drug effects
Purinergic P2 Receptor Antagonists - chemical synthesis
Purinergic P2 Receptor Antagonists - chemistry
Purinergic P2 Receptor Antagonists - pharmacokinetics
Purinergic P2 Receptor Antagonists - pharmacology
Receptors, Purinergic P2
Receptors, Purinergic P2Y
Structure-Activity Relationship
Uridine Diphosphate
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Zusammenfassung:A weak, UDP-competitive antagonist of the pyrimidinergic receptor P2RY(14) with a naphthoic acid core was identified through high-throughput screening. Optimization provided compounds with improved potency but poor pharmacokinetics. Acylglucuronidation was determined to be the major route of metabolism. Increasing the electron-withdrawing nature of the substituents markedly reduced glucuronidation and improved the pharmacokinetic profile. Additional optimization led to the identification of compound 38 which is an 8 nM UDP-competitive antagonist of P2Y(14) with a good pharmacokinetic profile.
ISSN:0960-894X
1464-3405
DOI:10.1016/j.bmcl.2011.03.081