A series of bicyclic analogues having indan and tetrahydronaphthalene templates in the A- region were designed as conformationally constrained analogues of our previously reported potent TRPV1 antagonists (1, 3). The activities for rat TRPV1 of the conformationally restricted analogues were moderately or markedly diminished, particularly in the case of the tetrahydronaphthalene analogues. The analysis indicated that steric constraints at the ...
[Harris III, Ralph N.; Stabler, Russel S.; Repke, David B.; Kress, James M.; Walker, Keith A.; Martin, Renee S.; Brothers, Julie M.; Ilnicka, Mariola; Lee, Simon W.; Mirzadegan, Tara Bioorganic and Medicinal Chemistry Letters, 2010 , vol. 20, # 11 p. 3436 - 3440]
