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μ‐Opioid Receptors and Not <i>K</i>‐Opioid Receptors Are Coupled to the Adenylate Cyclase in the Cerebellum
32
Citations
37
References
1990
Year
Synaptic TransmissionNeurotransmitterGuinea Pig CerebellumPutative Regulatory EffectPharmacotherapyPertussis ToxinExperimental PharmacologyMolecular Pharmacologyμ‐Opioid ReceptorsNeurochemistryAnalgesicsAnesthetic PharmacologyHealth SciencesAdenylate CyclaseNeuropharmacologyNervous SystemEndocrinologyPharmacologyPain ResearchNeurophysiologyFunctional SelectivityPhysiologyNeuroscienceCentral Nervous SystemAnesthesiaMedicineDrug Discovery
The putative regulatory effect of opioids on adenylate cyclase was investigated in two different preparations containing, respectively, two different populations of opioid receptors: the rabbit cerebellum (greater than 75% mu-opioid receptors) and the guinea pig cerebellum (greater than 80% kappa-opioid receptors). In the mu-preparation, but not in the kappa-preparation, opioids inhibited the basal and the forskolin-stimulated adenylate cyclase activity in a dose-dependent manner and stereospecifically. The inhibition was in the 20-30% range, required the presence in the assay medium of Mg2+ and of GTP, but was independent of the presence of Na+. Pharmacological characterization of the inhibitory response in the rabbit cerebellum clearly showed that it was under the control of a mu-opioid binding site, with the effect being elicited by non-selective (etorphine and morphine) and mu-selective (Tyr-D-Ala-Gly-Me-Phe-Gly-ol) agonists, whereas delta- and kappa-selective agonists were almost totally ineffective. ADP ribosylation of inhibitory GTP-binding protein by pertussis toxin failed to block the inhibitory effect of opioids, and data presented suggest that this failure is likely to be the consequence of a limited access of the toxin to its substrate in rabbit cerebellum membranes.
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