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去甲肾上腺素能神经元对一种非苯丙胺类中枢神经系统兴奋剂的电生理和生化反应。

Electrophysiological and biochemical responses of noradrenergic neurons to a non-amphetamine CNS stimulant.

作者信息

German D C, Sanghera M K, Kiser R S, McMillen B A, Shore P A

出版信息

Brain Res. 1979 Apr 27;166(2):331-9. doi: 10.1016/0006-8993(79)90218-x.

Abstract

Amfonelic acid (AFA), a potent non-amphetamine CNS stimulant, has been shown previously to have marked effects on dopamine (DA) metabolism and DA neuronal activity, but no effect on norepinephrine (NE) metabolism. AFA is known to inhibit the NE neuronal uptake mechanism. Other NE uptake inhibitors, such as desipramine (DMI), have been shown to decrease the firing rate of NE-containing locus coeruleus (LC) neurons. The purpose of the present study was to compare the actions of AFA and DMI electrophysiologically on LC neurons, and biochemically on NE metabolism in whg rate, with DMI being more potent. Brain NE metabolism was not influenced by either AFA or DMI at doses considerably higher than those which were effective in reducing NE neuronal impulse flow. Thus, NE uptake inhibition coupled with a decrease in impulse flow results in no net change in NE metabolite formation. The effects of AFA on LC unit activity do not seem to be due to its marked effects on brain DA, since DA receptor blockade with haloperidol had little effect on LC unit responsiveness to AFA (or amphetamine). Whereas AFA has dramatic effects on DA metabolism via enhanced release per impulse, the drug has minimal effects on NE metabolism, and this specificity of action may be related to differences in NE and DA transmitter storage mechanisms. It is concluded that the effects of AFA on NE neuronal firing rate are likely due to the drug's DMI-like action and not to enhanced NE release per impulse.

摘要

安福芬尼酸(AFA)是一种强效的非苯丙胺类中枢神经系统兴奋剂,先前已证明它对多巴胺(DA)代谢和DA神经元活动有显著影响,但对去甲肾上腺素(NE)代谢无影响。已知AFA可抑制NE神经元摄取机制。其他NE摄取抑制剂,如地昔帕明(DMI),已被证明可降低含NE的蓝斑(LC)神经元的放电频率。本研究的目的是用电生理学方法比较AFA和DMI对LC神经元的作用,并从生物化学角度比较它们对NE代谢的影响,结果显示DMI的作用更强。在远高于有效降低NE神经元冲动发放频率的剂量下,AFA和DMI均未影响脑内NE代谢。因此,NE摄取抑制与冲动发放频率降低相结合,不会导致NE代谢产物生成的净变化。AFA对LC单位活动的影响似乎并非因其对脑内DA有显著作用,因为用氟哌啶醇阻断DA受体对LC单位对AFA(或苯丙胺)的反应性影响很小。虽然AFA通过增强每次冲动的释放对DA代谢有显著影响,但该药物对NE代谢的影响极小,这种作用的特异性可能与NE和DA递质储存机制的差异有关。得出的结论是,AFA对NE神经元放电频率的影响可能是由于该药物类似DMI的作用,而不是每次冲动时NE释放增加所致。

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