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Vol. 295, Issue 1, 328-336, October 2000
Department of Physiology and Pharmacology, Center for the
Neurobiological Investigation of Drug Abuse, and Center for
Investigative Neuroscience, Wake Forest University School of Medicine,
Winston-Salem, North Carolina
To investigate differences in agonist affinity, potency, and efficacy
across rat brain regions, five representative cannabinoid compounds
were investigated in membranes from three different rat brain regions
for their ability to maximally stimulate
[35S]guanosine-5'-O-(3-thio)triphosphate
(GTP
S) binding and bind to cannabinoid receptors (measured by
inhibition of [3H]antagonist binding) under identical
assay conditions. In all three brain regions, the rank order of potency
for the stimulation of [35S]GTP
S binding and the
inhibition of [3H]SR141716A binding for these compounds
were identical, with CP55940
levonantradol > WIN55212-2
9-tetrahydrocannabinol
(
9-THC) > methanandamide. The rank order of
efficacy was not related to potency, and relative maximal agonist
effects varied across regions. Receptor binding fit to a three-site
model for most agonists, stimulation of [35S]GTP
S
binding fit to a two-site model for all agonists, and high-affinity
receptor binding did not appear to produce any stimulation of
[35S]GTP
S binding. WIN55212-2, methanandamide, and
9-THC also were assayed for the inhibition of adenylyl
cyclase in cerebellar membranes. The rank orders of potency and
efficacy were similar to those for [35S]GTP
S binding,
but the efficacies and potencies of methanandamide and
9-THC compared with WIN55212-2 were higher for adenylyl
cyclase inhibition, implying receptor/G-protein reserve.
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