Intermittent morphine treatment causes long-term desensitization of functional dopamine D sub(2) receptors in rat striatum

Intermittent morphine treatment causes long-term desensitization of functional dopamine D sub(2) receptors in rat striatum

3 weeks following cessation of intermittent morphine administration (10 mg/kg, s.c., once daily for 14 days), [ super(3)H]dopamine and [ super(14)C]acetylcholine release induced by 10 mu M N-methyl-D-aspartate (NMDA) from superfused rat striatal slices appeared to be significantly higher than the re...

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Veröffentlicht in:European journal of pharmacology 1995-12, Vol.294 (2-3), p.771-777
Hauptverfasser: Nestby, P, Tjon, GHK, Visser, DTM, Drukarch, B, Leysen, JE, Mulder, AH, Schoffelmeer, ANM
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container_issue 2-3
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container_title European journal of pharmacology
container_volume 294
creator Nestby, P
Tjon, GHK
Visser, DTM
Drukarch, B
Leysen, JE
Mulder, AH
Schoffelmeer, ANM
description 3 weeks following cessation of intermittent morphine administration (10 mg/kg, s.c., once daily for 14 days), [ super(3)H]dopamine and [ super(14)C]acetylcholine release induced by 10 mu M N-methyl-D-aspartate (NMDA) from superfused rat striatal slices appeared to be significantly higher than the release from striatal slices from saline-treated rats. A similar adaptive increase of the NMDA-evoked release of these neurotransmitters was observed in slices of the nucleus accumbens, whereas that of [ super(3)H]noradrenaline from hippocampal slices remained unchanged. Blockade of dopamine D sub(2) receptors by 10 mu M (-)-sulpiride enhanced NMDA-induced [ super(3)H]dopamine and [ super(14)C]acetylcholine release from striatal slices from saline-treated animals, but was found to be ineffective in this respect following intermittent morphine treatment. Moreover, morphine administration appeared to cause a profound decrease in the apparent affinity of the full dopamine D sub(2) receptor agonist LY171555 (quinpirole) for these release-inhibitory dopamine D sub(2) receptors, indicating the occurrence of dopamine D sub(2) receptor desensitization. It is suggested that such a desensitization of dopamine D sub(2) receptors on dopaminergic nerve terminals as well as on cholinergic interneurons may play a pivotal role in the long-lasting nature of behavioural sensitization upon cessation of treatment with morphine and possibly other drugs of abuse.
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title Intermittent morphine treatment causes long-term desensitization of functional dopamine D sub(2) receptors in rat striatum
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