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电击诱发癫痫后大鼠脑中转录因子mRNA的快速上升。

Rapid rise in transcription factor mRNAs in rat brain after electroshock-induced seizures.

作者信息

Cole A J, Abu-Shakra S, Saffen D W, Baraban J M, Worley P F

机构信息

Department of Neuroscience, Johns Hopkins University School of Medicine, Baltimore, Maryland 21205.

出版信息

J Neurochem. 1990 Dec;55(6):1920-7. doi: 10.1111/j.1471-4159.1990.tb05777.x.

Abstract

Recent studies have demonstrated that several transcription factor genes are rapidly activated by neuronal stimulation. For example, we have found that prolonged and repeated seizure activity produced by administration of chemical convulsants induces a rapid and transient increase in mRNA levels of four immediate early genes in rat brain. These genes, zif/268, c-fos, c-jun, and jun-B, encode sequence specific DNA binding proteins thought to act as transcription regulatory factors. To ascertain whether a brief electrically induced seizure discharge of the type utilized in clinical electroconvulsive treatment is sufficient to induce a similar genomic response, we have examined the response of these mRNAs in rat brain following single and repeated electroshock-induced seizures. After electroshock, mRNA levels of each of these genes increase within 15 min, and all except c-jun return to near baseline levels within 4 h. Although this response is most prominent in granule cell neurons of the hippocampus, increases are also apparent in neocortex and pyriform cortex. The rapid mRNA response persists in animals receiving a chronic electroshock protocol similar to that used in clinical electroconvulsive therapy. Intrahippocampal infusion of the sodium channel antagonist tetrodotoxin blocks hippocampal mRNA responses without blocking seizures, indicating a role for electrical excitation in the electroshock-induced mRNA response. By contrast, pretreatment with anticonvulsants or selective NMDA antagonists, which reduce seizure intensity and block hindlimb extension, fails to alter mRNA responses, suggesting that seizure induction, rather than spread, is linked to these mRNA responses. Because electroshock induces robust, highly reproducible mRNA responses, it may be useful to study the neuronal genomic response to stimulation.

摘要

最近的研究表明,几种转录因子基因可被神经元刺激迅速激活。例如,我们发现,通过给予化学惊厥剂产生的长时间反复癫痫活动会诱导大鼠脑中四个即刻早期基因的mRNA水平迅速短暂升高。这些基因,即zif/268、c-fos、c-jun和jun-B,编码被认为作为转录调节因子起作用的序列特异性DNA结合蛋白。为了确定临床电休克治疗中使用的那种短暂电诱导癫痫放电是否足以诱导类似的基因组反应,我们研究了单次和反复电休克诱导癫痫发作后大鼠脑中这些mRNA的反应。电休克后,这些基因中的每一个的mRNA水平在15分钟内升高,除c-jun外,所有基因在4小时内恢复到接近基线水平。尽管这种反应在海马颗粒细胞神经元中最为明显,但在新皮层和梨状皮层中也明显增加。在接受类似于临床电休克治疗的慢性电休克方案的动物中,快速的mRNA反应持续存在。海马内注入钠通道拮抗剂河豚毒素可阻断海马mRNA反应而不阻断癫痫发作,表明电刺激在电休克诱导的mRNA反应中起作用。相比之下,用抗惊厥药或选择性NMDA拮抗剂预处理可降低癫痫发作强度并阻断后肢伸展,但未能改变mRNA反应,这表明癫痫发作的诱导而非传播与这些mRNA反应有关。由于电休克可诱导强烈的、高度可重复的mRNA反应,因此研究神经元对刺激的基因组反应可能会有所帮助。

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