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Acetylcholine release in rat nucleus accumbens is regulated through dopamine D2-receptors
Authors:K Wedzony  N Limberger  L Späth  T Wichmann  K Starke
Institution:(1) Pharmakologisches Institut, Hermann-Herder-Strasse 5, D-7800 Freiburg i. Br., Federal Republic of Germany;(2) Present address: Institute of Pharmacology, Polish Academy of Sciences, 12 Smetna Street, PL-31-343 Krakow, Poland
Abstract:Summary Experiments in slices of rat nucleus accumbens were carried out in order to investigate whether the release of acetylcholine in this tissue is modulated through dopamine receptors. The slices were preincubated with 3H-choline and then superfused and stimulated electrically twice for 2 min each at a frequency of 3 Hz.The electrically evoked overflow of tritium averaged 2.9–3.9% of the tritium content of the tissue in the various groups. The D2-selective agonist quinpirole (0.01–1 mgrmol/l) reduced the evoked overflow of tritium by maximally 56%, an effect antagonized by the D2-selective antagonist (–)-sulpiride (1 mgrmol/l). The D1-selective agonist 2,3,4,5-tetrahydro-7,8-dihydroxy-1-phenyl-1H-3-benzazepine (SKF 38393) caused a slight decrease only at the high concentration of 10 mgrmol/l. (–)-Sulpiride (0.1–10 mgrmol/l) moderately increased the evoked overflow of tritium when given alone. The dopamine uptake inhibitor nomifensine (10 mgrmol/l) caused a decrease, and in its presence the increase produced by (–)-sulpiride became much more marked, amounting to maximally 149%. (+)-Sulpiride (0.1–1 mgrmol/l) failed to change the evoked overflow of tritium in the presence of nomifensine. The dopamine-releasing agent (±)-amphetamine (1 mgrmol/l) also reduced the evoked overflow, an effect abolished by (–)-sulpiride. Finally, bretylium (1 mmol/l), which blocks the release of dopamine, increased the evoked overflow. (–)-Sulpiride (1 mgrmol/l) lost its facilitatory effect in slices treated with bretylium.We conclude that the release of acetylcholine in rat nucleus accumbens, like its release in the nucleus caudatusputamen, is modulated through dopamine D2-receptors. The receptors are activated by endogenous dopamine under the conditions of these experiments. Send offprint requests to K. Starke at the above address
Keywords:Rat nucleus accumbens  Rat nucleus caudatusputamen  Acetylcholine release  Dopamine receptors
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