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细胞外ATP对大鼠原代皮质神经元早期生长反应转录因子表达的调控

Regulation of expression of early growth response transcription factors in rat primary cortical neurons by extracellular ATP.

作者信息

McKee Sarah C, Thompson Charlie S, Sabourin Luc A, Hakim Antoine M

机构信息

Department of Cellular and Molecular Medicine, University of Ottawa, 451 Smyth Road, Ottawa, Ontario, Canada.

出版信息

Brain Res. 2006 May 9;1088(1):1-11. doi: 10.1016/j.brainres.2006.02.133. Epub 2006 May 2.

DOI:10.1016/j.brainres.2006.02.133
PMID:16647694
Abstract

The zinc finger transcription factor early growth response-1 (Egr-1, NGFI-A, zif268, Krox 24, TIS8, ZENK) is upregulated immediately in the brain by cortical spreading depression (CSD) and other preconditioning stimuli and thus might participate in regulation of the overall genomic response to preconditioning. In the present study, the induction of expression of Egr-1 and other early growth response family members was characterized in rat primary cortical neuronal cultures. In neuronal cultures in vitro, depolarization or exposure to extracellular glutamate caused a 4-fold increase in egr-1 mRNA while exposure to extracellular ATP caused a 10-fold increase. The presence of mRNA encoding for multiple types of purinergic receptors was confirmed by RT-PCR. A number of nucleotide agonists proved effective in eliciting an increase in egr-1 mRNA. Over a limited range of concentration, the most effective agonists were ATP > ADP > alpha, beta-methylene ATP > UTP > cAMP > UDP > AMP > adenosine. Pertussis toxin, suramin, reactive blue 2, PPADS, DPCPX and inhibitors of Protein Kinase C, Protein Kinase A and PI3 kinase significantly reduced the upregulation of egr-1 by exposure to extracellular ATP. These findings suggest that neuronal metabotropic purinergic receptor activation contributes to the induction of early growth response transcription factors and may provide a target that can be manipulated to increase ischemic tolerance of the brain in vivo.

摘要

锌指转录因子早期生长反应因子-1(Egr-1,NGFI-A,zif268,Krox 24,TIS8,ZENK)在大脑中会因皮层扩散性抑制(CSD)和其他预处理刺激而立即上调,因此可能参与对预处理的整体基因组反应的调节。在本研究中,对大鼠原代皮层神经元培养物中Egr-1和其他早期生长反应家族成员的表达诱导进行了表征。在体外神经元培养物中,去极化或暴露于细胞外谷氨酸会使egr-1 mRNA增加4倍,而暴露于细胞外ATP会使其增加10倍。通过RT-PCR证实了编码多种嘌呤能受体的mRNA的存在。许多核苷酸激动剂被证明能有效引起egr-1 mRNA的增加。在有限的浓度范围内,最有效的激动剂是ATP > ADP > α,β-亚甲基ATP > UTP > cAMP > UDP > AMP > 腺苷。百日咳毒素、苏拉明、活性蓝2、PPADS、DPCPX以及蛋白激酶C、蛋白激酶A和PI3激酶的抑制剂显著降低了暴露于细胞外ATP时egr-1的上调。这些发现表明,神经元代谢型嘌呤能受体激活有助于早期生长反应转录因子的诱导,并且可能提供一个可被操控以提高体内大脑缺血耐受性的靶点。

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