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首页> 外文期刊>Neurochemistry International: The International Journal for the Rapid Publication of Critical Reviews, Preliminary and Original Research Communications in Neurochemistry >Isoflurane anesthesia inhibits clozapine- and risperidone-induced dopamine release and anesthesia-induced changes in dopamine metabolism was modified by fluoxetine in the rat striatum: an in vivo microdialysis study.
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Isoflurane anesthesia inhibits clozapine- and risperidone-induced dopamine release and anesthesia-induced changes in dopamine metabolism was modified by fluoxetine in the rat striatum: an in vivo microdialysis study.

机译:异氟烷麻醉可抑制氯氮平和利培酮诱导的多巴胺释放,而氟西汀可在大鼠纹状体中修饰麻醉诱导的多巴胺代谢变化:一项体内微透析研究。

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Previously, we have reported that halothane anesthesia increases the extracellular concentrations of dopamine (DA) metabolites in the rat striatum using in vivo microdialysis techniques, and we have suggested that volatile anesthetics affect DA release and metabolism in various ways. The present investigation assesses the effect of isoflurane, widely used in clinical anesthesia, on DA release and metabolism. A microdialysis probe was implanted in the striatum of male Sprague-Dawley rats (n=5-7 per group). After recovery, the probe was perfused with modified Ringer's solution and 40 microl of dialysate were injected into a high performance liquid chromatograph every 20 min. The rats were given saline or the same volume of 10 mg kg(-1) clozapine, risperidone, fluoxetine or citalopram. After the pharmacological treatment, the rats were anesthetized with 1.0% or 2.5% isoflurane for 1h. The data were analyzed using two-way analysis of variance (ANOVA). For each drug with significant (p<0.05) drug-time interactions, the statistical analysis included one-way ANOVA and Newman-Keuls post hoc comparisons. A high concentration of isoflurane (2.5%) anesthesia increased the extracellular concentration of DA metabolites during emergence from anesthesia. The levels of DA metabolites increased in an isoflurane concentration-dependent manner. Isoflurane attenuated DA release induced by clozapine and risperidone. Fluoxetine, but not citalopram, antagonized the isoflurane-induced increase in metabolites. The results of current investigation suggest that isoflurane enhances presynaptic DA metabolism, and that the oxidation of DA might be partially modulated by the activities of the dopaminergic-serotonergic pathway at a presynaptic site in the rat striatum.
机译:以前,我们已经报道了氟烷麻醉使用体内微透析技术增加了大鼠纹状体中多巴胺(DA)代谢产物的细胞外浓度,并且我们已经建议挥发性麻醉剂以各种方式影响DA的释放和代谢。本研究评估了在临床麻醉中广泛使用的异氟烷对DA释放和代谢的影响。将微透析探针植入雄性Sprague-Dawley大鼠的纹状体中(每组n = 5-7)。回收后,将探针用改良的林格氏液灌注,每20分钟将40微升透析液注入高效液相色谱仪中。给予大鼠生理盐水或相同体积的10毫克kg(-1)的氯氮平,利培酮,氟西汀或西酞普兰。药理处理后,将大鼠用1.0%或2.5%异氟烷麻醉1h。使用双向方差分析(ANOVA)分析数据。对于每种具有显着(p <0.05)药物-时间相互作用的药物,统计分析包括单因素方差分析和Newman-Keuls事后比较。麻醉期间,高浓度异氟烷(2.5%)麻醉可增加DA代谢产物的细胞外浓度。 DA代谢物的水平以异氟烷浓度依赖性方式增加。异氟烷减轻了由氯氮平和利培酮引起的DA释放。氟西汀而非西酞普兰能拮抗异氟烷引起的代谢物增加。目前的研究结果表明,异氟烷可增强突触前DA的代谢,并且DA的氧化可能受到大鼠纹状体突触前部位多巴胺能-5-羟色胺能途径的活性的调节。

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