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CREB在中脑边缘多巴胺奖赏通路中的差异分布。

Differential distribution of CREB in the mesolimbic dopamine reward pathway.

作者信息

Walters Carrie L, Kuo Yuo-Chen, Blendy Julie A

机构信息

Department of Pharmacology, University of Pennsylvania, 3620 Hamilton Walk, Philadelphia, PA 19104-6084, USA.

出版信息

J Neurochem. 2003 Dec;87(5):1237-44. doi: 10.1046/j.1471-4159.2003.02090.x.

DOI:10.1046/j.1471-4159.2003.02090.x
PMID:14622103
Abstract

The transcription factor cAMP response element binding protein (CREB) has been implicated in the long-term neuronal plasticity associated with addiction. While CREB is expressed in many cells throughout the brain, very little is known about the relative concentrations of CREB protein in various brain regions. Studies in which CREB levels have been altered, either constitutively throughout the brain via gene targeting or transiently in specific brain regions, demonstrate variable roles for this protein in mediating reinforcing properties of drugs of abuse. To investigate the complex nature of CREB function in addiction, we examined the distribution of CREB protein in the nucleus accumbens (NAc) and ventral tegmental area (VTA), two brain regions that are part of the well-defined mesolimbic dopamine pathway involved in reward processing. Our data demonstrate significantly more CRE binding activity and CREB protein in the NAc compared to levels present in the VTA of wild-type mice. Phospho-CREB levels are increased in the NAc of both wild-type and CREBalphaDelta mutant animals after cocaine. However, morphine-induced increases of phospho-CREB levels are seen in the VTA of wild-type mice but not CREBalphaDelta mutant mice. Consequently, the 90% reduction of CREB in CREBalphaDelta mutant mice differentially affects CREB phosphorylation and induction of downstream targets of CREB in the NAc and VTA.

摘要

转录因子环磷腺苷效应元件结合蛋白(CREB)与成瘾相关的长期神经元可塑性有关。虽然CREB在大脑中的许多细胞中都有表达,但对于CREB蛋白在各个脑区的相对浓度却知之甚少。通过基因靶向在全脑组成性改变CREB水平或在特定脑区短暂改变CREB水平的研究表明,该蛋白在介导滥用药物的强化特性中具有多种作用。为了研究CREB在成瘾中功能的复杂性,我们检测了伏隔核(NAc)和腹侧被盖区(VTA)中CREB蛋白的分布,这两个脑区是参与奖赏处理的明确中脑边缘多巴胺通路的一部分。我们的数据表明,与野生型小鼠VTA中的水平相比,NAc中的CRE结合活性和CREB蛋白明显更多。可卡因处理后,野生型和CREBαΔ突变动物的NAc中磷酸化CREB水平均升高。然而,吗啡诱导的磷酸化CREB水平升高在野生型小鼠的VTA中可见,而在CREBαΔ突变小鼠中则未见。因此,CREBαΔ突变小鼠中90%的CREB减少对NAc和VTA中CREB磷酸化及CREB下游靶点的诱导有不同影响。

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