1. Forskolin Carbamates: Binding and Activation Studies with Type I Adenylyl Cyclase
- Author
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Robbins, J. D., Boring, D. L., Tang, W.-J., Shank, R., and Seamon, K. B.
- Abstract
Three series of analogs were regioselectively prepared from a protected forskolin precursor to afford 7-carbamoyl-7-desacetylforskolins (series 1), 6-carbamoyl-7-desacetylforskolins (series 2), and 6-carbamoylforskolins (series 3). The analogs were pharmacologically evaluated for binding (IC
50 ) to and activation (EC50 ) of type I adenylyl cyclase in membranes from stably transfected Sf9 cell lines expressing a single adenylate cyclase subtype. The following ranges were determined for the IC50 's and EC50 's of each individual series: series 1, IC50 = 43−1600 nM, EC50 = 0.5−9.6 μM; series 2, IC50 = 65−680 nM, EC50 = 0.63−6.5 μM; series 3, IC50 = 21−271 nM, EC50 = 0.5−8.1 μM (forskolin IC50 = 41 nM and EC50 = 0.5 μM). Activation paralleled binding; however, some analogs exhibited poor binding and good activation whereas others demonstrated good binding but poor activation. Steric bulk tended to diminish binding and activation when at the 6- or 7-position, although bulk was accommodated at the 6-position if the 7-site was reacetylated. Acylation of the 7-position by the carbamoyl linker or acetyl was important for obtaining good binding and activation; however, the effect was more pronounced with binding. For both binding and activation, small, linear, lipophilic substituents (propyl, allyl, isopropyl) are well tolerated at the 7-position but less so in the 6-position, even when the 7-site is reacetylated. Planar aromatic moieties (phenyl and 2-pyridinyl) demonstrated moderate to good potency for binding and activation when located at either the 6- or 7-positions. There is an overall trend toward increasing potency for both binding and activation with polar substituents.- Published
- 1996