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Overcoming retinoic acid receptor-α based testicular toxicity in the optimisation of glucokinase activators
18
Citations
11
References
2011
Year
SpermatogenesisGlycobiologyRetinoic Acid Receptor-αLead SeriesGlucocorticoidMolecular PharmacologyGlycosylationAndrologyBiochemistryG Protein-coupled ReceptorHormonal ReceptorType 2Glucokinase ActivatorsReceptor (Biochemistry)Testicular ToxicityEndocrinologyPharmacologyMolecular MedicineNatural SciencesSmall Molecule ActivatorsCellular BiochemistryMedicineEndocrine ResearchDrug Discovery
Small molecule activators of the glucokinase enzyme have the potential to deliver a level of glycaemic control that is superior to current oral agents and hence have great promise as new therapies for Type 2 Diabetes. As such, attempts to discover glucokinase activators suitable for clinical development have been the focus of many major pharmaceutical research programmes. Here we describe how we have overcome a testicular toxicological liability in our pyridine acid lead series, which we show can be ascribed to antagonism of the retinoic acid receptor-α.
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