Delta Opioid Receptor Down-Regulation Is Independent of Functional G Protein yet Is Dependent on Agonist Efficacy

Chronic treatment of C6 glioma cells stably expressing the rat delta opioid receptor (C6δ) with full agonists resulted in receptor down-regulation. Chronic [ d -Ser 2 , l -Leu 5 ]enkephalyl-Thr treatment caused a decrease in cell surface as well as a decrease in agonist-stimulated [ 35 S]guanosine-...

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Bibliographic Details
Published in:The Journal of pharmacology and experimental therapeutics 1998-11, Vol.287 (2), p.625-632
Main Authors: Remmers, A E, Clark, M J, Liu, X Y, Medzihradsky, F
Format: Article
Language:English
Subjects:
Adenylyl Cyclase Inhibitors
Animals
Colforsin - pharmacology
Cyclic AMP - metabolism
Down-Regulation
Enkephalin, D-Penicillamine (2,5)
Enkephalin, Leucine - analogs & derivatives
Enkephalin, Leucine - pharmacology
Enkephalins - pharmacology
GTP-Binding Proteins - metabolism
Guanosine 5'-O-(3-Thiotriphosphate) - metabolism
Rats
Receptors, Opioid - agonists
Receptors, Opioid - metabolism
Tumor Cells, Cultured
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Summary:Chronic treatment of C6 glioma cells stably expressing the rat delta opioid receptor (C6δ) with full agonists resulted in receptor down-regulation. Chronic [ d -Ser 2 , l -Leu 5 ]enkephalyl-Thr treatment caused a decrease in cell surface as well as a decrease in agonist-stimulated [ 35 S]guanosine-5′-O-(3-thio)triphosphate binding. Treatment with full agonists for 12 hr resulted in a 90% decrease in receptor number that was paralleled by a decrease in the ability of agonist to stimulate [ 35 S]guanosine-5′-O-(3-thio)triphosphate binding and inhibit forskolin-stimulated adenylyl cyclase. Of the remaining receptors, a smaller fraction of receptors (41 ± 4 vs. 56 ± 4% in control) exhibited high affinity for agonist as compared to receptors in control membranes. Elimination of functional guanosine triphosphate binding protein (G protein) by Pertussis toxin pretreatment did not alter the ability of agonist to down regulate receptor. We hypothesized that agonist affinity (not efficacy) would be a predictor of an agonist’s ability to down-regulate receptor. However, we found that only full agonists were able to down-regulate receptor number, G protein activation and adenylyl cyclase inhibition. Chronic exposure to partial agonist 7-spiroindinooxymorphone, which has a very high affinity for the receptor, as well as morphine, did not cause receptor down-regulation. Taken together, these results suggest that full agonists alter receptor conformation such that the altered conformation is recognized by G protein as well as proteins involved in receptor down-regulation. In addition, down-regulation is independent of agonist-mediated G protein activation and subsequent down-stream signaling.
ISSN:0022-3565
1521-0103