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Selective opioid agonist and antagonist competition for [3H]-naloxone binding in amphibian spinal cord
- Publication Year :
- 2000
-
Abstract
- Opioids elicit antinociception in mammals through three distinct types of receptors designated as mu, kappa and delta. However, it is not clear what type of opioid receptor mediates antinociception in non-mammalian vertebrates. Radioligand binding techniques were employed to characterize the site(s) of opioid action in the amphibian, Rana pipiens. Naloxone is a general opioid antagonist that has not been characterized in Rana pipiens. Using the non-selective opioid antagonist, [3H]-naloxone, opioid binding sites were characterized in amphibian spinal cord. Competitive binding assays were done using selective opioid agonists and highly-selective opioid antagonists. Naloxone bound to a single-site with an affinity of 11.3 nM and 18.7 nM for kinetic and saturation studies, respectively. A B(max) value of 2725 fmol/mg protein in spinal cord was observed. The competition constants (K(i)) of unlabeled mu, kappa and delta ranged from 2.58 nM to 84 microM. The highly-selective opioid antagonists yielded similar K(i) values ranging from 5.37 to 31.1 nM. These studies are the first to examine opioid binding in amphibian spinal cord. In conjunction with previous behavioral data, these results suggest that non-mammalian vertebrates express a unique opioid receptor which mediates the action of selective mu, kappa and delta opioid agonists.
- Subjects :
- Agonist
medicine.medical_specialty
medicine.drug_class
Narcotic Antagonists
Pain
(+)-Naloxone
Pharmacology
Tritium
Binding, Competitive
Article
Opioid receptor
Internal medicine
medicine
Animals
Molecular Biology
Neurons
Chemistry
Narcotic antagonist
Naloxone
General Neuroscience
Rana pipiens
Antagonist
Nociceptors
Analgesics, Opioid
Kinetics
Endocrinology
Opioid
Spinal Cord
Models, Animal
Receptors, Opioid
Nociceptor
Neurology (clinical)
Opioid antagonist
Developmental Biology
medicine.drug
Subjects
Details
- Language :
- English
- Database :
- OpenAIRE
- Accession number :
- edsair.doi.dedup.....9f8e3fdcad00b881fae310e5d04415a1