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Dopamine Efflux from Striatum After Chronic Nicotine: Evidence for Autoreceptor Desensitization
Authors:Laszlo G Harsing  Jr    Henry Sershen  Abel Lajtha
Institution:Center for Neurochemistry, N. S. Kline Institute for Psychiatric Research, Orangeburg, New York 10962.
Abstract:We examined the effect of chronic nicotine treatment on dopaminergic activity by measuring the effects of D1 and D2 dopamine (DA) receptor agonists and antagonists on tritium release from mouse striatum preloaded with 3H]DA. The radioactivity released during superfusion was separated on alumina columns and the distribution and efflux of 3H]DA and its main 3H-labeled metabolites were quantified. After preloading by incubation with 3H]DA, the electrical stimulation-evoked tritium overflow was higher in striatum prepared from nicotine-treated mice, whereas in vitro addition of nicotine caused a similar increase in tritium release from striatum of untreated and chronic nicotine-treated mice. The overflow of 3H]DA and its 3H-metabolites exhibited similar distribution patterns in 3H]DA-preloaded striatum dissected from untreated and chronic nicotine-pretreated mice, indicating that repeated injections with nicotine did not alter the metabolism of 3H]DA taken up by the tissue. (-)-Quinpirole, a selective agonist for D2 DA receptors, and apomorphine, a nonselective D1/D2 agonist, inhibited the electrical stimulation-induced tritium efflux from striatum of untreated mice, whereas (+/-)-sulpiride, a D2 DA receptor antagonist, enhanced the evoked release of tritium. These changes in tritium efflux effected by (-)-quinpirole and (+/-)-sulpiride reflected changes in 3H]DA release and not in DA metabolism, as shown by separation of the released radioactivity on alumina columns. The D1 receptor agonist (+/-)-SKF-38393 did not affect the tritium overflow, whereas the D1 receptor antagonist (+)-SCH-23390 exerted a stimulatory action but only at a high concentration.(ABSTRACT TRUNCATED AT 250 WORDS)
Keywords:[3H]Dopamine release  Nicotine  D1 and D2 agonists  D1 and D2 antagonists  Striatum
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