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脑内生物胺对小鼠乙醇戒断反应及乙醇依赖性形成的影响。

Effects of brain biogenic amines on ethanol withdrawal reactions and the development of ethanol dependence in mice.

作者信息

Yamanaka Y

出版信息

Jpn J Pharmacol. 1982 Jun;32(3):499-508. doi: 10.1254/jjp.32.499.

Abstract

Mice were made physically dependent on ethanol by a four-day period of ethanol inhalation. A single injection of L-dopa tended to enhance ethanol withdrawal reactions and 5HTP tended to suppress it. Daily treatment with PCPA and L-dopa or pretreatment with 6OHDA tended to modify the severity of withdrawal reactions. PCPA slightly decreased the severity, 6OHDA tended to aggravate the severity, and L-dopa tended to decrease the severity. The simultaneous estimation of brain biogenic amine levels suggests that 5HT and DA may be involved in the development of physical dependence on ethanol. Treatment with neuropharmacological drugs during ethanol withdrawal modified the severity of ethanol withdrawal reactions. Pentobarbital and diazepam completely suppressed ethanol withdrawal reactions. GHBA and reserpine suppressed the severity and haloperidol, imipramine, and methylphenidate aggravated it. The simultaneous estimation of brain catecholamine levels suggests that suppression of ethanol withdrawal reactions consistently results from the decreased activities of either noradrenergic or dopaminergic neurons. However, the effects of biogenic amines on ethanol withdrawal reactions may be different from those on the development of physical dependence on ethanol.

摘要

通过四天的乙醇吸入使小鼠对乙醇产生身体依赖性。单次注射左旋多巴倾向于增强乙醇戒断反应,而5-羟色氨酸倾向于抑制该反应。每天用对氯苯丙氨酸和左旋多巴治疗或用6-羟基多巴胺预处理倾向于改变戒断反应的严重程度。对氯苯丙氨酸略微降低了严重程度,6-羟基多巴胺倾向于加重严重程度,而左旋多巴倾向于降低严重程度。对脑内生物胺水平的同时评估表明,5-羟色胺和多巴胺可能参与了对乙醇身体依赖性的形成。在乙醇戒断期间用神经药理学药物治疗改变了乙醇戒断反应的严重程度。戊巴比妥和地西泮完全抑制了乙醇戒断反应。γ-羟基丁酸钠和利血平抑制了严重程度,而氟哌啶醇、丙咪嗪和哌醋甲酯则加重了严重程度。对脑内儿茶酚胺水平的同时评估表明,乙醇戒断反应的抑制始终是由于去甲肾上腺素能或多巴胺能神经元活性降低所致。然而,生物胺对乙醇戒断反应的影响可能与它们对乙醇身体依赖性形成的影响不同。

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