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边缘叶反复癫痫发作后齿状回颗粒细胞的超微结构可塑性:I. 体细胞棘突增加。

Ultrastructural plasticity of the dentate gyrus granule cells following recurrent limbic seizures: I. Increase in somatic spines.

作者信息

Bundman M C, Pico R M, Gall C M

机构信息

Department of Anatomy and Neurobiology, University of California, Irvine 92717.

出版信息

Hippocampus. 1994 Oct;4(5):601-10. doi: 10.1002/hipo.450040510.

Abstract

Various paradigms have been used to assess the capacity of the adult brain to undergo activity-dependent morphological plasticity. In this report we have employed recurrent limbic seizures as a means of studying the effects of this form of enhanced neuronal activity on cellular morphology and, in particular, on the incidence of somatic spines on the dentate gyrus granule cells. Seizure activity was induced by the placement of focal, unilateral electrolytic lesions in the dentate gyrus hilus of adult rats. At various intervals postlesion, rats with behaviorally verified seizures were sacrificed, and the hippocampi contralateral to the lesions were removed and prepared for electron microscopy. Quantitative analysis showed that as early as 5 hours postlesion there was a dramatic increase in the density and morphological complexity of spines on the perikarya of the granule cells in rats that received seizure-producing hilus lesions when compared to granule cells from control rats. Many of the somatic spines received asymmetric synapses. The increase in somatic spines was dependent on seizure activity and persisted for at least 1 month following a single recurrent seizure episode. CA1 pyramidal neurons, which exhibit changes in gene expression in response to hilus lesion-induced seizures but do not normally possess somatic spines, did not exhibit an activity-dependent elaboration of somatic spines. Thus, the seizure-induced elaboration of somatic spines represents an amplification of an existing feature of the granule cells and not an effect occurring throughout hippocampus. These data provide evidence for very rapid and long-lasting structural plasticity in response to brief episodes of seizure activity in the adult brain.

摘要

已经采用了各种范式来评估成人大脑进行活动依赖性形态可塑性的能力。在本报告中,我们采用复发性边缘叶癫痫发作作为一种手段,来研究这种形式的增强神经元活动对细胞形态的影响,特别是对齿状回颗粒细胞体细胞棘突发生率的影响。通过在成年大鼠齿状回门处放置局灶性单侧电解损伤来诱导癫痫发作活动。在损伤后的不同时间间隔,对行为学上证实有癫痫发作的大鼠进行处死,并取出与损伤相对侧的海马,准备进行电子显微镜检查。定量分析表明,与对照大鼠的颗粒细胞相比,在接受产生癫痫发作的门损伤的大鼠中,早在损伤后5小时,颗粒细胞胞体上的棘突密度和形态复杂性就有显著增加。许多体细胞棘突接受不对称突触。体细胞棘突的增加依赖于癫痫发作活动,并且在单次复发性癫痫发作后至少持续1个月。CA1锥体神经元,其在基因表达上对门损伤诱导的癫痫发作有变化,但通常不具有体细胞棘突,并未表现出活动依赖性的体细胞棘突形成。因此,癫痫发作诱导的体细胞棘突形成代表了颗粒细胞现有特征的放大,而不是整个海马体中发生的效应。这些数据为成年大脑对短暂癫痫发作活动的非常快速和持久的结构可塑性提供了证据。

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