
Journal of Medicinal Chemistry p. 3187 - 3197 (2017)
Update date:2022-08-02
Topics:
McCoull, William
Bailey, Andrew
Barton, Peter
Birch, Alan M.
Brown, Alastair J. H.
Butler, Hayley S.
Boyd, Scott
Butlin, Roger J.
Chappell, Ben
Clarkson, Paul
Collins, Shelley
Davies, Robert M. D.
Ertan, Anne
Hammond, Clare D.
Holmes, Jane L.
Lenaghan, Carol
Midha, Anita
Morentin-Gutierrez, Pablo
Moore, Jane E.
Raubo, Piotr
Robb, Graeme
GPR120 agonists have therapeutic potential for the treatment of diabetes, but few selective agonists have been reported. We identified an indazole-6-phenylcyclopropylcarboxylic acid series of GPR120 agonists and conducted SAR studies to optimize GPR120 potency. Furthermore, we identified a (S,S)-cyclopropylcarboxylic acid structural motif which gave selectivity against GPR40. Good oral exposure was obtained with some compounds displaying unexpected high CNS penetration. Increased MDCK efflux was utilized to identify compounds such as 33 with lower CNS penetration, and activity in oral glucose tolerance studies was demonstrated. Differential activity was observed in GPR120 null and wild-type mice indicating that this effect operates through a mechanism involving GPR120 agonism.
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