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佛波酯对前额叶皮质和纹状体多巴胺能终末的不同作用:取决于刺激的频率和持续时间。

Differential effects of phorbol ester on prefrontal cortex and striatal dopamine terminals: dependence on rate and duration of stimulation.

作者信息

Talmaciu R K, Hoffmann I S, Cubeddu L X

机构信息

Department of Pharmacology, School of Medicine, University of North Carolina, Chapel Hill.

出版信息

J Pharmacol Exp Ther. 1989 Dec;251(3):1160-5.

PMID:2557413
Abstract

Compared to the nigrostriatal dopamine (DA) neurons, the mesocortical DA neurons projecting to the prefrontal cortex (PFC) are able to sustain higher levels of release when driven at high stimulation frequencies. The effect of a well known activator of protein kinase C (PKC), 4-beta-phorbol-12, 13-dibutyrate (PDBu), were compared on PFC and striatal DA terminals. DA release was monitored from slices of the rabbit PFC and striatum obtained from the same animal. The PKC activator, PDBu (30-1000 nM) enhanced the stimulation-evoked release (SER) of DA from PFC and striatum. The magnitude of the facilitation of DA release produced by PDBu was much greater from the PFC than from the striatum. In the striatum, PDBu produced a bell-shaped dose-response curve, i.e., 0.03 and 1 microM PDBu enhanced SER of DA by 25%, whereas 0.1 and 0.3 microM PDBu enhanced DA release by 60 and 100%, respectively (1 Hz, 120 pulses). In the PFC, 0.03 microM enhanced the SER of DA by 70% and 1 microM by 250% (1 Hz, 120 pulses). In addition, in the PFC, PDBu enhance the basal release of DA (+65% at 1 microM); this effect was not seen in the striatum. The inactive isomer, 4-alpha-phorbol-12, 13-dibutyrate (0.03-1 microM) failed to increase the SER and the basal release of DA from PFC or striatum. The SER of DA was dependent on the rate and duration of stimulation. However, under all conditions of stimulation studied DA release from PFC was always greater than from the striatum.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

与黑质纹状体多巴胺(DA)神经元相比,投射到前额叶皮质(PFC)的中皮质DA神经元在高刺激频率驱动时能够维持更高水平的释放。比较了一种著名的蛋白激酶C(PKC)激活剂4-β-佛波醇-12,13-二丁酸酯(PDBu)对PFC和纹状体DA终末的作用。从同一动物获取的兔PFC和纹状体切片监测DA释放。PKC激活剂PDBu(30 - 1000 nM)增强了PFC和纹状体中DA的刺激诱发释放(SER)。PDBu促进DA释放的幅度在PFC比在纹状体大得多。在纹状体中,PDBu产生钟形剂量反应曲线,即0.03和1 microM PDBu使DA的SER分别增强25%,而0.1和0.3 microM PDBu分别使DA释放增强60%和100%(1 Hz,120个脉冲)。在PFC中,0.03 microM使DA的SER增强70%,1 microM增强250%(1 Hz,120个脉冲)。此外,在PFC中,PDBu增强了DA的基础释放(1 microM时增加65%);在纹状体中未观察到这种效应。无活性异构体4-α-佛波醇-12,13-二丁酸酯(0.03 - 1 microM)未能增加PFC或纹状体中DA的SER和基础释放。DA的SER取决于刺激的速率和持续时间。然而,在所有研究的刺激条件下,PFC中DA的释放总是大于纹状体中的释放。(摘要截短于250字)

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