Publication | Open Access
Discovery of Potent Isoxazoline Glycoprotein IIb/IIIa Receptor Antagonists
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Citations
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References
1997
Year
ThrombopoiesisThrombosisMedicinal ChemistryBiochemistryBlood PlateletPotent Antiplatelet AgentMedicineNatural SciencesImmunologyReceptor (Biochemistry)Platelet InhibitionPharmacological AgentPharmacotherapyPlatelet AntagonistPharmacologyCommon Structural FeatureDrug Discovery
Using the isoxazoline as a common structural feature, three series of glycoprotein IIb/IIIa receptor antagonists were evaluated, culminating in the discovery of XR299 (30). In an in vitro assay of platelet inhibition, XR299 had an IC50 of 0.24 microM and was a potent antiplatelet agent when dosed intravenously in a canine model. It was shown through X-ray studies of the cinchonidine salt 49 that the receptor required the 5(R)-stereochemistry for high potency. The ethyl ester prodrug of XR299, XR300 (29), was orally active in the dog.
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