TY - JOUR T1 - The Interaction of Phenoxybenzamine with the Mouse Brain Opiate Receptor JF - Molecular Pharmacology JO - Mol Pharmacol SP - 587 LP - 595 VL - 14 IS - 4 AU - VINA SPIEHLER AU - ALAN S. FAIRHURST AU - LOWELL O. RANDALL Y1 - 1978/07/01 UR - http://molpharm.aspetjournals.org/content/14/4/587.abstract N2 - Phenoxybenzamine was found to displace stereospecifically bound [3H]naloxone from mouse brain homogenates in a dose-related manner, with an IC50 of 4.6 µM. In the presence of 100 mM Na+, the dose-response curve shifted to give an IC50 of 19 µM and an Na+ response ratio of 4.3, which is similar to that of a mixed agonist-antagonist. Scatchard plots of the binding data showed that phenoxybenzamine reduced the number of receptor binding sites for naloxone but did not change the affinity of the unreacted receptors for naloxone. Levallorphan protected the receptor from phenoxybenzamine, but the inhibition of binding activity produced by phenoxybenzamine could not be reversed by repeated washing of the receptor preparation. It thus appears that phenoxybenzamine acts as an irreversible, non-equilibrium inhibitor with binding characteristics similar to those of the agonist-antagonist narcotics. Washed brain homogenates from mice treated in vivo with antinociceptive doses of phenoxybenzamine exhibited enhanced binding of [3H]naloxone and [3H]morphine, which may indicate the displacement of an endogenous material from the opiate receptors in vivo by phenoxybenzamine. ER -