Publications by authors named "M E Rempala"
During the course of our research efforts to develop potent and selective AKT inhibitors, we discovered enatiomerically pure substituted dihydropyridopyrimidinones (DHP) as potent inhibitors of protein kinase B/AKT with excellent selectivity against ROCK. A key challenge in this program was the poor physicochemical properties of the initial lead compound 5. Integration of structure-based drug design and physical properties-based design resulted in replacement of a highly hydrophobic poly fluorinated aryl ring by a simple trifluoromethyl that led to identification of compound 6 with much improved physicochemical properties.
View Article and Find Full Text PDFOwing to the prevalence of the JAK2V617F mutation in myeloproliferative neoplasms (MPNs), its constitutive activity, and ability to recapitulate the MPN phenotype in mouse models, JAK2V617F kinase is an attractive therapeutic target. We report the discovery and initial characterization of the orally bioavailable imidazopyridazine, LY2784544, a potent, selective and ATP-competitive inhibitor of janus kinase 2 (JAK2) tyrosine kinase. LY2784544 was discovered and characterized using a JAK2-inhibition screening assay in tandem with biochemical and cell-based assays.
View Article and Find Full Text PDFArticle Synopsis
- LY2457546 is an effective and orally bioavailable inhibitor targeting multiple receptor tyrosine kinases that are important in processes like angiogenesis and tumor growth.
- It shows superior potency in inhibiting endothelial tube formation compared to sunitinib and demonstrates considerable effectiveness in various tumor models, including complete regression in acute myelogenous leukemia.
- The drug was well-tolerated in non-clinical studies, with observed toxicities resembling those found with other multi-targeted anti-angiogenic medications.