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Pyrido pyrimidinones as selective agonists of the high affinity niacin receptor GPR109A: optimization of in vitro activity.

Jens-Uwe Peters,Holger Kühne,Henrietta Dehmlow,Uwe Grether,Aurelia Conte,Dominik Hainzl,Cornelia Hertel,Nicole A Kratochwil,Michael Otteneder,Robert Narquizian,Constantinos G Panousis,Fabienne Ricklin,Stephan Röver

Bioorganic & Medicinal Chemistry Letters(2010)

Cited 14|Views19
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Abstract
Pyrido pyrimidinones are selective agonists of the human high affinity niacin receptor GPR109A (HM74A). They show no activity on the highly homologous low affinity receptor GPR109B (HM74). Starting from a high throughput screening hit the in vitro activity of the pyrido pyrimidinones was significantly improved providing lead compounds suitable for further optimization.
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Key words
Flushing,GPR109A,GPR109B,GPCR,Lead identification,Lipolysis,Niacin,Pyrido pyrimidinone
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