| Literature DB >> 21516197 |
Anil R Ekkati1, Valsan Madiyan, Krishna P Ravindranathan, Jae H Bae, Joseph Schlessinger, William L Jorgensen.
Abstract
Optimization of thienopyrimidinone derivatives as FGFR1 kinase inhibitors is being pursued. The present results confirm predictions of computational modeling that an aryl subtituent can be introduced at the 2-position in strucure 3. The substituent is anticipated to project deeper into the binding site and provide opportunities for enhanced activity and selectivity. The most potent analog reported here, 13, has a 4-hydroxyphenyl substituent and yields an IC(50) of 6 μM for inhibition of phosphorylation by FGFR1 kinase. It was also found that the western anisole-containing substituent in 3 can be replaced by a propionic acid group with no loss in potency and with potentially significant gains in pharmacologically relevant properties.Entities:
Year: 2011 PMID: 21516197 PMCID: PMC3079261 DOI: 10.1016/j.tetlet.2010.12.081
Source DB: PubMed Journal: Tetrahedron Lett ISSN: 0040-4039 Impact factor: 2.415