Publication | Open Access
Discovery of Biaryl Anthranilides as Full Agonists for the High Affinity Niacin Receptor
36
Citations
14
References
2007
Year
Drug TargetImmunologyPharmacotherapyMedicinal ChemistryReceptor Gpr109aAnti-cancer AgentSerum ShiftBiaryl AnthranilidesBiochemistryG Protein-coupled ReceptorReceptor (Biochemistry)Mechanism Of ActionNon-peptide LigandPharmacologyFunctional SelectivityNatural SciencesMedicineFull AgonistsDrug Discovery
Biaryl anthranilides are reported as potent and selective full agonists for the high affinity niacin receptor GPR109A. The SAR presented outlines approaches to reduce serum shift and both CYPCYP2C8 and CYP2C9 liabilities, while improving PK and maintaining excellent receptor activity. Compound 2i exhibited good in vivo antilipolytic efficacy while providing a significantly improved therapeutic index over vasodilation (flushing) with respect to niacin in the mouse model.
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