Brain uptake and receptor binding of two [ 11C]labelled selective high affinity NK1-antagonists, GR203040 and GR205171 — PET studies in rhesus monkey

Brain uptake and receptor binding of two [ 11C]labelled selective high affinity NK1-antagonists, GR203040 and GR205171 — PET studies in rhesus monkey

Two high affinity and selective NK1-receptor antagonists, GR203040 and GR205171, were labelled with 11C and used in a series of experiments in rhesus monkeys. The purpose of these studies was to evaluate the brain uptake pattern and to explore the potential use of these compounds as PET ligands to c...

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Bibliographic Details
Published in:Neuropharmacology Vol. 39; no. 4; pp. 664 - 670
Main Authors: Bergström, M, Fasth, K.-J, Kilpatrick, G, Ward, P, Cable, K.M, Wipperman, M.D, Sutherland, D.R, Långström, B
Format: Journal Article
Language:English
Published: Oxford Elsevier Ltd 01-01-2000
Elsevier
Subjects:
Animals
Biological and medical sciences
Brain
Brain - diagnostic imaging
Brain - metabolism
Carbon Radioisotopes
Ligands
Macaca mulatta
Medical sciences
Miscellaneous
Neurokinin-1 Receptor Antagonists
Neuropharmacology
Neurotransmitters. Neurotransmission. Receptors
NK1
PET
Pharmacokinetics
Pharmacology. Drug treatments
Piperidines - metabolism
Piperidines - pharmacokinetics
Primates
Protein Binding
Receptors, Neurokinin-1 - metabolism
Tetrazoles - metabolism
Tetrazoles - pharmacokinetics
Tomography, Emission-Computed
Primates
Brain
Pharmacokinetics
NK1
PET
NK1 Tachykinin receptor
Intravenous administration
Monkey
Central nervous system
Molecular interaction
Radioactive tracers
Blood
Blood plasma
Vertebrata
Mammalia
Animal
Medical imagery
Antagonist
Brain (vertebrata)
Positron
Emission tomography
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Summary:Two high affinity and selective NK1-receptor antagonists, GR203040 and GR205171, were labelled with 11C and used in a series of experiments in rhesus monkeys. The purpose of these studies was to evaluate the brain uptake pattern and to explore the potential use of these compounds as PET ligands to characterise NK1-receptor binding. Seventeen studies were carried out with [ 11C]GR205171 and five experiments with [ 11C]GR203040, including baseline studies and studies performed after a 5 min infusion of cold compound at doses between 0.05 and 1 mg/kg. Both compounds demonstrated a significant and rapid uptake in the brain, but the uptake of [ 11C]GR205171 was more than double the uptake of [ 11C]GR203040. At tracer doses of [ 11C]GR205171 and all doses of [ 11C]GR203040 the uptake reached a plateau with no washout during the examination time, whereas [ 11C]GR205171 after pre-treatment with cold GR205171 showed a significant washout. Using a model with the cerebellum as reference, a method for quantitation was applied to the studies with [ 11C]GR205171 and the results indicated that the highest specific binding was in the striatum. The pre-treatment dose of cold GR205171 needed for 50% inhibition of binding was less than 0.04 mg/kg. The studies indicated that [ 11C]GR205171 could be used for the in vivo characterisation of NK1-receptor binding.
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ISSN:0028-3908
1873-7064
DOI:10.1016/S0028-3908(99)00182-3