SKF 525-A and cytochrome P-450 ligands inhibit with high affinity the binding of [3H]dextromethorphan and sigma ligands to guinea pig brain

SKF 525-A and cytochrome P-450 ligands inhibit with high affinity the binding of [3H]dextromethorphan and sigma ligands to guinea pig brain

The DM1/sigma 1 site binds dextromethorphan (DM) and sigma receptor ligands. The broad binding specificity of this site and its peculiar subcellular distribution prompted us to explore the possibility that this site is a member of the cytochrome P-450 superfamily of enzymes. We tested the effects of...

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Bibliographic Details
Published in:Life sciences (1973) Vol. 48; no. 6; p. 543
Main Authors: Klein, M, Canoll, P D, Musacchio, J M
Format: Journal Article
Language:English
Published: Netherlands 1991
Subjects:
Animals
Binding, Competitive
Brain - metabolism
Cytochrome P-450 CYP2D6
Cytochrome P-450 Enzyme System - metabolism
Debrisoquin - pharmacology
Dextromethorphan - metabolism
Guinea Pigs
Kinetics
Ligands
Lobeline - pharmacology
Mixed Function Oxygenases - metabolism
Neurotransmitter Uptake Inhibitors - pharmacology
Piperazines - pharmacology
Proadifen - pharmacology
Receptors, Opioid - drug effects
Receptors, Opioid - metabolism
Receptors, sigma
Sparteine - pharmacology
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Summary:The DM1/sigma 1 site binds dextromethorphan (DM) and sigma receptor ligands. The broad binding specificity of this site and its peculiar subcellular distribution prompted us to explore the possibility that this site is a member of the cytochrome P-450 superfamily of enzymes. We tested the effects of the liver microsomal monooxygenase inhibitor SKF 525-A (Proadifen), and other P-450 substrates on the binding of [3H]dextromethorphan, [3H]3-(-3-Hydroxyphenyl)-N-(1-propyl)piperidine and (+)-[3H]1,3-Di-o-tolyl-guanidine ([3H]DTG) to the guinea pig brain. SKF 525-A, l-lobeline and GBR-12909 inhibited the binding of the three labeled ligands with nM affinity. Each drug has identical nM Ki values for the high-affinity site labeled by the three ligands. This indicated that they displaced the labeled ligands from the common DM1/sigma 1 site. Debrisoquine and sparteine, prototypical substrates for liver debrisoquine 4-hydroxylase, displayed Ki values of 9-13 and 3-4 microM respectively against the three labeled ligands. These results, the broad specificity of the DM1/sigma 1 binding site, and its peculiar subcellular distribution, raises the possibility that this binding site is a member of the cytochrome P-450 superfamily of isozymes, rather than a neurotransmitter receptor. These findings may have important implications for the understanding of the therapeutic, side effects and toxicity of several neurotropic drugs.
ISSN:0024-3205
DOI:10.1016/0024-3205(91)90469-R