Discovery of a Novel Class of Imidazo[1,2-a]Pyridines with Potent PDGFR Activity and Oral Bioavailability

Erik J Hicken; Fred P Marmsater; Mark C Munson; Stephen T Schlachter; John E Robinson; Shelley Allen; Laurence E Burgess; Robert Kirk DeLisle; James P Rizzi; George T Topalov; Qian Zhao; Julie M Hicks; Nicholas C Kallan; Eugene Tarlton; Andrew Allen; Michele Callejo; April Cox; Sumeet Rana; Nathalie Klopfenstein; Richard Woessner; Joseph P Lyssikatos

doi:10.1021/ml4003953

Discovery of a Novel Class of Imidazo[1,2-a]Pyridines with Potent PDGFR Activity and Oral Bioavailability

ACS Med Chem Lett. 2013 Nov 12;5(1):78-83. doi: 10.1021/ml4003953. eCollection 2014 Jan 9.

Authors

Erik J Hicken¹, Fred P Marmsater¹, Mark C Munson¹, Stephen T Schlachter¹, John E Robinson¹, Shelley Allen¹, Laurence E Burgess¹, Robert Kirk DeLisle¹, James P Rizzi¹, George T Topalov¹, Qian Zhao¹, Julie M Hicks¹, Nicholas C Kallan¹, Eugene Tarlton¹, Andrew Allen¹, Michele Callejo¹, April Cox¹, Sumeet Rana¹, Nathalie Klopfenstein¹, Richard Woessner¹, Joseph P Lyssikatos¹

Affiliation

¹ Department of Drug Discovery, Array BioPharma , 3200 Walnut Street, Boulder, Colorado 80301, United States.

Abstract

The in silico construction of a PDGFRβ kinase homology model and ensuing medicinal chemistry guided by molecular modeling, led to the identification of potent, small molecule inhibitors of PDGFR. Subsequent exploration of structure-activity relationships (SAR) led to the incorporation of a constrained secondary amine to enhance selectivity. Further refinements led to the integration of a fluorine substituted piperidine, which resulted in significant reduction of P-glycoprotein (Pgp) mediated efflux and improved bioavailability. Compound 28 displayed oral exposure in rodents and had a pronounced effect in a pharmacokinetic-pharmacodynamic (PKPD) assay.

Keywords: Pgp; Platelet-derived growth factor; fluorine; fluoro-piperidine.