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脑源性神经营养因子可恢复大鼠反复电惊厥发作后脑内Jun和Fos诱导型转录因子的表达。

BDNF restores the expression of Jun and Fos inducible transcription factors in the rat brain following repetitive electroconvulsive seizures.

作者信息

Hsieh T F, Simler S, Vergnes M, Gass P, Marescaux C, Wiegand S J, Zimmermann M, Herdegen T

机构信息

II. Institute of Physiology, University of Heidelberg, Germany.

出版信息

Exp Neurol. 1998 Jan;149(1):161-74. doi: 10.1006/exnr.1997.6686.

Abstract

The expression of inducible transcription factors was studied following repetitive electroconvulsive seizures (ECS), c-Fos, c-Jun, JunB, and JunD immunoreactivities were investigated following a single (1 x ECS) or repetitive ECS evoked once per day for 4, 5, or 10 days (4 x ECS, 5 x ECS, or 10 x ECS). Animals were killed 3 or 12 h following the last ECS. Three hours after 1 x ECS, c-Fos was expressed throughout the cortex and hippocampus. After 5 x ECS and 10 x ECS, c-Fos was reexpressed in the CA4 area, but was completely absent in the other hippocampal areas and cortex. In these areas, c-Fos became only reinducible when the time lag between two ECS stimuli was 5 days. In contrast to c-Fos, intense JunB expression was inducible in the cortex and hippocampus, but not CA4 subfield, after 1 x ECS, 5 x ECS, and 10 x ECS. Repetitive ECS did not effect c-Jun and JunD expression. In a second model of systemic excitation of the brain, repetitive daily injection of kainic acid for 4 days completely failed to express c-Fos, c-Jun, and JunB after the last application whereas injection of kainic acid once per week did not alter the strong expressions compared to a single application of kainic acid. In order to study the maintenance of c-Fos expression during repetitive seizures, brain-derived neurotrophic factor (BDNF) was applied in parallel for 5 or 10 days via miniosmotic pumps and permanent cannula targeted at the hippocampus or the parietal cortex. Infusion of BDNF completely reinduced c-Fos expression during 5 x ECS or 10 x ECS in the cortex ipsilaterally to the cannula and, to a less extent, also increased the expression of c-Jun and JunB when compared to saline-treated controls. BDNF had no effect on the expression patterns in the hippocampus. ECS with or without BDNF infusion did not change the expression patterns of the constitutive transcription factors ATF-2, CREB, and SRF. These data demonstrate that various transcription factors substantially differ in their response to acute and chronic neural stimulation. Repetitive pathophysiological excitation decreases the transcriptional actions of neurons over days in the adult brain, and this decrement can be prevented by BDNF restoring the neuroplasticity at the level of gene transcription.

摘要

研究了重复电惊厥发作(ECS)后诱导型转录因子的表达,在单次(1×ECS)或每天诱发一次、持续4、5或10天(4×ECS、5×ECS或10×ECS)的重复ECS后,研究了c-Fos、c-Jun、JunB和JunD的免疫反应性。在最后一次ECS后3或12小时处死动物。1×ECS后3小时,c-Fos在整个皮质和海马中表达。5×ECS和10×ECS后,c-Fos在CA4区重新表达,但在其他海马区和皮质中完全缺失。在这些区域,只有当两次ECS刺激之间的时间间隔为5天时,c-Fos才会再次被诱导。与c-Fos不同,在1×ECS、5×ECS和10×ECS后,皮质和海马中可诱导强烈的JunB表达,但CA4亚区除外。重复ECS对c-Jun和JunD的表达没有影响。在第二个脑全身兴奋模型中,连续4天每天重复注射海人酸,在最后一次注射后完全未能表达c-Fos、c-Jun和JunB,而与单次注射海人酸相比,每周注射一次海人酸并没有改变其强烈的表达。为了研究重复发作期间c-Fos表达的维持情况,通过微型渗透泵和靶向海马或顶叶皮质的永久套管并行应用脑源性神经营养因子(BDNF)5或10天。与生理盐水处理的对照组相比,输注BDNF在5×ECS或10×ECS期间完全重新诱导了套管同侧皮质中c-Fos的表达,并且在较小程度上也增加了c-Jun和JunB的表达。BDNF对海马中的表达模式没有影响。有无BDNF输注的ECS均未改变组成型转录因子ATF-2、CREB和SRF的表达模式。这些数据表明,各种转录因子对急性和慢性神经刺激的反应存在显著差异。重复的病理生理兴奋在数天内会降低成人大脑中神经元的转录作用,而BDNF可以通过在基因转录水平恢复神经可塑性来预防这种下降。

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