Use of Small-Molecule Crystal Structures To Address Solubility in a Novel Series of G Protein Coupled Receptor 119 Agonists: Optimization of a Lead and in Vivo Evaluation

James S Scott,Katy J Brocklehurst,Per H Svensson,Adrian Pickup,Sam D Groombridge,Andrew G Leach,Julian A Hudson,Philip A Macfaul,David Laber,Pernilla Sörme,Roger J Butlin,Alan M Birch,Darren Mckerrecher,Anne Ertan,Öjvind Davidsson,Kristin Goldberg,Anders Broo,Joanne Teague,Hayley Brown ,Paul N Schofield ,D S Clarke

doi:10.1021/jm300310c

Use of Small-Molecule Crystal Structures To Address Solubility in a Novel Series of G Protein Coupled Receptor 119 Agonists: Optimization of a Lead and in Vivo Evaluation

James S Scott, Katy J Brocklehurst + Show 19 more

https://doi.org/10.1021/jm300310c

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Journal: Journal of Medicinal Chemistry	Publication Date: May 17, 2012
Citations: 64

Affiliation: AstraZeneca (United Kingdom), AstraZeneca (Sweden)

#Small-molecule Crystallography #Vivo Evaluation + Show 8 more

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Abstract

G protein coupled receptor 119 (GPR119) is viewed as an attractive target for the treatment of type 2 diabetes and other elements of the metabolic syndrome. During a program toward discovering agonists of GPR119, we herein describe optimization of an initial lead compound, 2, into a development candidate, 42. A key challenge in this program of work was the insolubility of the lead compound. Small-molecule crystallography was utilized to understand the intermolecular interactions in the solid state and resulted in a switch from an aryl sulphone to a 3-cyanopyridyl motif. The compound was shown to be effective in wild-type but not knockout animals, confirming that the biological effects were due to GPR119 agonism.

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