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血清素能系统与多巴胺能系统在右芬氟拉明诱导大鼠纹状体神经元中c-fos和jun B基因激活过程中的相互作用。

Interaction between the serotoninergic and dopaminergic systems in d-fenfluramine-induced activation of c-fos and jun B genes in rat striatal neurons.

作者信息

Gardier A M, Moratalla R, Cuéllar B, Sacerdote M, Guibert B, Lebrec H, Graybiel A M

机构信息

Laboratoire de Neuropharmacologie UPRES EAD MENRT, IFR-ISIT Institut de Signalisation et Innovation Thérapeutique, Amiens, France.

出版信息

J Neurochem. 2000 Apr;74(4):1363-73. doi: 10.1046/j.1471-4159.2000.0741363.x.

Abstract

To test for the relative contributions of the dopaminergic and serotoninergic systems in the striatum to the effects of d-fenfluramine, an indirect serotonin receptor agonist, we assessed the expression of Fos/Jun proteins induced by d-fenfluramine given alone or in the presence of dopaminergic or serotoninergic agents. To determine the neuronal targets of d-fenfluramine in the striatum, we identified the phenotypes of striatal neurons in which d-fenfluramine induced Fos expression. Our results demonstrated that d-fenfluramine evokes nuclear expression of Fos/Jun B proteins in the striatum, and that the Fos expression was dose-dependent and accompanied by transient induction of c-fos mRNA. Fos expression was blocked by p-chloroamphetamine, a serotoninergic neurotoxin. Pretreatment with SCH 23390, a D1-dopamine receptor antagonist, led to a marked decrease in Fos/Jun B expression in the caudoputamen, but not in the cortex, whereas pretreatment with methiothepin, a nonselective serotonin 5-HT1 receptor antagonist, blocked Fos expression completely in the cortex and only partially in the caudoputamen. The expression of Fos/Jun B in the striatum occurred mainly in dynorphin-containing neurons and in a subpopulation of striatal interneurons that exhibited NADPH-diaphorase activity. Most of the enkephalin-containing neurons of the striatum did not show Fos/Jun B staining. These results suggest that the mechanism by which d-fenfluramine induces c-fos and jun B expression in the rat caudoputamen depends at least in part on activation of the dopaminergic system by serotonin.

摘要

为了测试纹状体中多巴胺能和5-羟色胺能系统对间接5-羟色胺受体激动剂d-芬氟拉明作用的相对贡献,我们评估了单独给予d-芬氟拉明或在多巴胺能或5-羟色胺能药物存在的情况下,由d-芬氟拉明诱导的Fos/Jun蛋白的表达。为了确定d-芬氟拉明在纹状体中的神经元靶点,我们鉴定了纹状体神经元中d-芬氟拉明诱导Fos表达的表型。我们的结果表明,d-芬氟拉明在纹状体中引起Fos/Jun B蛋白的核表达,并且Fos表达呈剂量依赖性,并伴有c-fos mRNA的短暂诱导。Fos表达被5-羟色胺能神经毒素对氯苯丙胺阻断。用D1-多巴胺受体拮抗剂SCH 23390预处理导致尾壳核中Fos/Jun B表达显著降低,但在皮质中没有,而用非选择性5-羟色胺5-HT1受体拮抗剂甲硫哒嗪预处理则完全阻断了皮质中的Fos表达,而在尾壳核中仅部分阻断。纹状体中Fos/Jun B的表达主要发生在含强啡肽的神经元和表现出NADPH-黄递酶活性的纹状体中间神经元亚群中。纹状体中大多数含脑啡肽的神经元没有显示Fos/Jun B染色。这些结果表明,d-芬氟拉明在大鼠尾壳核中诱导c-fos和jun B表达的机制至少部分取决于5-羟色胺对多巴胺能系统的激活。

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