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Literature DB >> 4516196

Stereospecific binding of the potent narcotic analgesic (3H) Etorphine to rat-brain homogenate.

Abstract

Etorphine, the most potent narcotic analgesic known, was labeled with tritium by catalytic exchange. This drug exhibits stereospecific, saturable binding to rat-brain homogenate. At saturation, the stereospecific binding is 0.1-0.15 pmol/mg of protein. Specific binding is inhibited high salt concentrations, sulfhydryl reagents, and proteolytic enzymes, but is unaffected by phospholipases A and C, sodium azide, sodium fluoride, and prostaglandins E(1) and E(2). Competition for binding of [(3)H]etorphine correlates with agonist and antagonist potencies. The stable, stereospecific binding of an active narcotic analgesic supports the existence of opiate receptors.

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Year: 1973 PMID： 4516196 PMCID： PMC433639 DOI： 10.1073/pnas.70.7.1947

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

8 in total

1. Protein measurement with the Folin phenol reagent.

Authors: O H LOWRY; N J ROSEBROUGH; A L FARR; R J RANDALL
Journal: J Biol Chem Date: 1951-11 Impact factor: 5.157

Review 2. Biochemistry of addiction.

Authors: V P Dole
Journal: Annu Rev Biochem Date: 1970 Impact factor: 23.643

3. Opiate receptor: demonstration in nervous tissue.

Authors: C B Pert; S H Snyder
Journal: Science Date: 1973-03-09 Impact factor: 47.728

4. Actions of etorphine hydrochloride, (M99): a potent morphine-like agent.

Authors: G F Blane; A L Boura; A E Fitzgerald; R E Lister
Journal: Br J Pharmacol Chemother Date: 1967-05

5. Studies on the intracellular distribution and tissue binding of dihydromorphine-7,8-H3 in the rat.

Authors: D Van Praag; E J Simon
Journal: Proc Soc Exp Biol Med Date: 1966-05

6. On the mechanism of action of phospholipase A and insulin on glucose entry into free adipose cells.

Authors: M Blecher
Journal: Biochem Biophys Res Commun Date: 1966-04-06 Impact factor: 3.575

7. Coupling of a new, active morphine derivative to sepharose for affinity chromatography.

Authors: E J Simon; W P Dole; J M Hiller
Journal: Proc Natl Acad Sci U S A Date: 1972-07 Impact factor: 11.205

8. Stereospecific and nonspecific interactions of the morphine congener levorphanol in subcellular fractions of mouse brain.

Authors: A Goldstein; L I Lowney; B K Pal
Journal: Proc Natl Acad Sci U S A Date: 1971-08 Impact factor: 11.205

8 in total

141 in total

Review 1. Neurochemistry and behavior in man.

Authors: G S Omenn
Journal: West J Med Date: 1976-12

Stereospecific binding of the potent narcotic analgesic (3H) Etorphine to rat-brain homogenate.

1. Protein measurement with the Folin phenol reagent.

Review 2. Biochemistry of addiction.

3. Opiate receptor: demonstration in nervous tissue.

4. Actions of etorphine hydrochloride, (M99): a potent morphine-like agent.

5. Studies on the intracellular distribution and tissue binding of dihydromorphine-7,8-H3 in the rat.

6. On the mechanism of action of phospholipase A and insulin on glucose entry into free adipose cells.

7. Coupling of a new, active morphine derivative to sepharose for affinity chromatography.

8. Stereospecific and nonspecific interactions of the morphine congener levorphanol in subcellular fractions of mouse brain.

Review 1. Neurochemistry and behavior in man.

Review 2. Dealing with sadness, madness and hostility. New psychotropic drug remedies for the future.

3. Expression cloning of cDNA encoding a seven-helix receptor from human placenta with affinity for opioid ligands.

Review 4. Post-transcriptional regulation of opioid receptors in the nervous system.

Review 5. The dynorphin/κ-opioid receptor system and its role in psychiatric disorders.

6. Animal and molecular pharmacology of mixed agonist-antagonist analgesic drugs.

Review 7. Ligand-directed signalling within the opioid receptor family.

8. Opioid peptides, brain and behaviour: a brief review.

9. Striatal regulation of morphine-induced hyperphagia: an anatomical mapping study.

10. Bioinformatic analysis of the human mu opioid receptor (OPRM1) splice and polymorphic variants.