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大鼠脑部损伤通过多种启动子的差异使用诱导脑源性神经营养因子(BDNF)基因表达增加。

Brain insults in rats induce increased expression of the BDNF gene through differential use of multiple promoters.

作者信息

Kokaia Z, Metsis M, Kokaia M, Bengzon J, Elmér E, Smith M L, Timmusk T, Siesjö B K, Persson H, Lindvall O

机构信息

Department of Neurology, University Hospital, Lund, Sweden.

出版信息

Eur J Neurosci. 1994 Apr 1;6(4):587-96. doi: 10.1111/j.1460-9568.1994.tb00303.x.

Abstract

The rat brain-derived neurotrophic factor (BDNF) gene consists of four short 5'-exons linked to separate promoters and one 3'-exon encoding the mature BDNF protein. Using in situ hybridization we demonstrate here that kindling-induced seizures, cerebral ischaemia and insulin-induced hypoglycaemic coma increase BDNF mRNA levels through insult- and region-specific usage of three promoters within the BDNF gene. Both brief (2 min) and longer (10 min) periods of forebrain ischaemia induced significant and major increases only of exon III mRNA in the dentate gyrus. Following hypoglycaemic coma (1 and 30 min), exon III mRNA was markedly elevated in the dentate gyrus and, in addition, exon I mRNA showed a moderate increase. Single and recurrent (n = 40) hippocampal seizures significantly increased expression of exon I, II and III mRNAs in the dentate gyrus granule cells. After recurrent seizures, including generalized convulsions, there were also major increases of both exon I and III mRNAs in the CA3 region, amygdala, piriform cortex and neocortex, whereas in the hippocampal CA1 sector marked elevations were detected only for exon III mRNA. The insults had no effect on the level of exon IV mRNA in the brain. The region- and insult-specific pattern of promoter activation might be of importance for the effectiveness of protective responses as well as for the regulation of plastic changes following brain insults.

摘要

大鼠脑源性神经营养因子(BDNF)基因由与不同启动子相连的四个短5'外显子和一个编码成熟BDNF蛋白的3'外显子组成。我们在此通过原位杂交证明,点燃诱导的癫痫发作、脑缺血和胰岛素诱导的低血糖昏迷通过BDNF基因内三个启动子的损伤和区域特异性使用来增加BDNF mRNA水平。短暂(2分钟)和较长(10分钟)的前脑缺血期仅在齿状回中诱导外显子III mRNA显著且大幅增加。低血糖昏迷(1分钟和30分钟)后,齿状回中外显子III mRNA明显升高,此外,外显子I mRNA有中度增加。单次和反复(n = 40)海马癫痫发作显著增加齿状回颗粒细胞中外显子I、II和III mRNA的表达。反复癫痫发作后,包括全身性惊厥,CA3区、杏仁核、梨状皮质和新皮质中外显子I和III mRNA也大幅增加,而在海马CA1区仅检测到外显子III mRNA有明显升高。这些损伤对脑中的外显子IV mRNA水平没有影响。启动子激活的区域和损伤特异性模式可能对保护反应的有效性以及脑损伤后可塑性变化的调节具有重要意义。

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