Publication | Open Access
Discovery of Potent, Nonsteroidal, and Highly Selective Glucocorticoid Receptor Antagonists
60
Citations
30
References
2002
Year
Medicinal ChemistryBiochemistryFunctional SelectivityMedicineNatural SciencesG Protein-coupled ReceptorReceptor (Biochemistry)Gr ActivityPharmacological AgentPseudo-c2 SymmetryPharmacotherapyGlucocorticoidNon-peptide LigandGlucocorticoid ReceptorPharmacologyDrug Discovery
An approach to the computer-assisted, pharmacophore design of nonsteroidal templates for the glucocorticoid receptor (GR) that contained an element of pseudo-C2 symmetry was developed. The enatiomer of the initial design, 1Ra, and not the designed molecule, 1S, showed the desired ligand binding to the GR. The pseudo-C2 symmetry of the template allowed for rapid improvements in GR activity resulting in potent, selective, nonsteroidal GR antagonists, CP-394531 and CP-409069.
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