Ichikawa Junji, Chung Young Chul, Li Zhu, Dai Jin, Meltzer Herbert Y
Division of Psychopharmacology, Department of Psychiatry, Vanderbilt University School of Medicine, Nashville, TN 37212, USA.
Brain Res. 2002 Dec 20;958(1):176-84. doi: 10.1016/s0006-8993(02)03692-2.
Behavioral evidence suggests that muscarinic/cholinergic inhibition of brain dopaminergic activity may be a useful principle for developing novel antipsychotic drugs (APDs). Thus, oxotremorine, a muscarinic agonist, attenuates amphetamine-induced locomotor activity in rodents, an effect also produced by a wide variety of proven APDs, whereas scopolamine, a muscarinic antagonist, has the opposite effect. Since atypical APDs such as clozapine, olanzapine, risperidone, ziprasidone and quetiapine, increase brain acetylcholine as well as dopamine (DA) release in a region-specific manner, their effects on cholinergic and dopaminergic neurotransmission may also contribute to various actions of these drugs. Oxotremorine (0.5-1.5 mg/kg) dose-dependently and preferentially increased DA release in rat medial prefrontal cortex (mPFC), compared to the nucleus accumbens (NAC). However, S-(-)-scopolamine (0.5-1.5 mg/kg) produced similar increases in DA release in the mPFC, but the effect was much less than that of oxotremorine. Whereas a dose of S-(-)-scopolamine of 0.5 mg/kg comparably increased DA release in the mPFC and NAC, 1.5 mg/kg had no effect on DA release in the NAC. Oxotremorine-M (0.5 mg/kg), a M(1/4)-preferring agonist, also increased DA release in the mPFC, but not the NAC, an effect completely abolished by telenzepine (3 mg/kg), a M(1/4)-preferring antagonist, which by itself had no effect on DA release in either region. Oxotremorine (0.5, but not 1.5, mg/kg) attenuated amphetamine (1 mg/kg)-induced DA release in the NAC, whereas S-(-)-scopolamine did not. Oxotremorine (1.5 mg/kg) and S-(-)-scopolamine (0.5 mg/kg) modestly but significantly potentiated amphetamine (1 mg/kg)-induced DA release in the mPFC. These results suggest that stimulation of muscarinic receptors, in particular M(1/4), as indicated by the effect of oxotremorine-M and telenzepine, may preferentially increase cortical DA release and inhibit amphetamine-induced DA release in the NAC.
行为学证据表明,毒蕈碱/胆碱能对脑多巴胺能活性的抑制作用可能是开发新型抗精神病药物(APD)的一个有用原则。因此,毒蕈碱激动剂氧化震颤素可减弱苯丙胺诱导的啮齿动物运动活性,多种已证实的APD也有此作用,而毒蕈碱拮抗剂东莨菪碱则有相反作用。由于非典型APD如氯氮平、奥氮平、利培酮、齐拉西酮和喹硫平以区域特异性方式增加脑乙酰胆碱以及多巴胺(DA)释放,它们对胆碱能和多巴胺能神经传递的影响也可能促成这些药物的多种作用。与伏隔核(NAC)相比,氧化震颤素(0.5 - 1.5毫克/千克)剂量依赖性且优先增加大鼠内侧前额叶皮质(mPFC)中的DA释放。然而,S - (-)-东莨菪碱(0.5 - 1.5毫克/千克)在mPFC中使DA释放有类似增加,但作用远小于氧化震颤素。0.5毫克/千克剂量的S - (-)-东莨菪碱使mPFC和NAC中的DA释放同等增加,而1.5毫克/千克对NAC中的DA释放无影响。氧化震颤素 - M(0.5毫克/千克),一种优先作用于M(1/4)的激动剂,也增加mPFC中的DA释放,但不增加NAC中的,该作用被优先作用于M(1/4)的拮抗剂替仑西平(3毫克/千克)完全消除,替仑西平本身对任一区域的DA释放均无影响。氧化震颤素(0.5毫克/千克,但1.5毫克/千克无此作用)减弱苯丙胺(1毫克/千克)诱导的NAC中的DA释放,而S - (-)-东莨菪碱则不然。氧化震颤素(1.5毫克/千克)和S - (-)-东莨菪碱(0.5毫克/千克)适度但显著增强苯丙胺(1毫克/千克)诱导的mPFC中的DA释放。这些结果表明,如氧化震颤素 - M和替仑西平的作用所示,刺激毒蕈碱受体,特别是M(1/4),可能优先增加皮质DA释放并抑制NAC中苯丙胺诱导的DA释放。
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