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人类癫痫性硬化海马中吊灯细胞的组织病理学及重组

Histopathology and reorganization of chandelier cells in the human epileptic sclerotic hippocampus.

作者信息

Arellano J I, Muñoz A, Ballesteros-Yáñez I, Sola R G, DeFelipe J

机构信息

Departmento de Neuroanatomía y Biología Celular, Instituto Cajal, CSIC, Madrid, Spain.

出版信息

Brain. 2004 Jan;127(Pt 1):45-64. doi: 10.1093/brain/awh004. Epub 2003 Oct 8.

Abstract

Impairment of GABA-mediated inhibition is one of the main hypotheses invoked to explain seizure activity, both in experimental models and in human epilepsy. We have studied the distribution and the neurochemical characteristics of certain GABAergic circuits in the normal and epileptic human sclerotic hippocampal formation. We have focused our attention mainly on chandelier cells because, together with basket cells, they are considered to have powerful effects on spike generation. Chandelier cells represent a unique type of interneuron whose axon terminals (Ch-terminals) form synapses with the axon initial segments of cortical pyramidal cells and granular cells of the dentate gyrus. Different neurochemical subpopulations of chandelier cells have been identified by immunocytochemistry, mainly in the neocortex. Markers for Ch-terminals include the GABA transporter 1 (GAT-1), the polysialylated form of the cell-surface glycoprotein neural cell adhesion molecule (PSA-NCAM) and the calcium-binding proteins parvalbumin (PV) and calbindin D-28k (CB). In the normal hippocampal formation, GAT-1- and PV-immunoreactive (-ir) Ch-terminals were identified in the granular and polymorphic layers of the dentate gyrus, in the strata pyramidale and oriens of the CA fields, and in the pyramidal layer of the subicular complex. In addition, and in contrast to the hippocampus and dentate gyrus, subsets of Ch-terminals in the upper pyramidal layer of the normal subiculum express CB and PSA-NCAM. The sclerotic hippocampus of epileptic patients presented an impressive morphological and neurochemical reorganization of Ch-terminals and basket formations. This was apparent in the dentate gyrus and hippocampal formation, but not in the subiculum, which appeared to remain unaltered. Principally, numerous and more complex PV- and CB-ir Ch-terminals, as well as dense PV-ir basket formations, appeared in some hippocampal segments, whereas in other regions there was a lack of labelled elements. These changes varied considerably not only between different patients, but also within different hippocampal fields in a given patient. In general, the changes were not correlated with the clinical characteristics or degree of histopathological alterations observed in the patients, such as granular cell dispersion, neuron loss and proliferation of mossy fibres. However, some surviving neurons in the regions adjacent to the areas of neuron loss were consistently innervated by dense basket formations and complex Ch-terminals. These results indicate that, in the human epileptic hippocampus, GABAergic circuits are more highly modified than previously thought. When considered along with other extrahippocampal alterations, we suggest that these changes are important in the pathophysiology of temporal lobe epilepsy associated with hippocampal sclerosis.

摘要

γ-氨基丁酸(GABA)介导的抑制作用受损是用于解释实验模型和人类癫痫发作活动的主要假说之一。我们研究了正常和癫痫患者硬化海马结构中某些GABA能回路的分布及神经化学特征。我们主要关注了吊灯细胞,因为与篮状细胞一起,它们被认为对动作电位的产生有强大影响。吊灯细胞是一种独特类型的中间神经元,其轴突终末(Ch终末)与皮质锥体细胞和齿状回颗粒细胞的轴突起始段形成突触。通过免疫细胞化学已鉴定出吊灯细胞的不同神经化学亚群,主要在新皮质中。Ch终末的标志物包括GABA转运体1(GAT-1)、细胞表面糖蛋白神经细胞黏附分子的多唾液酸化形式(PSA-NCAM)以及钙结合蛋白小白蛋白(PV)和钙结合蛋白D-28k(CB)。在正常海马结构中,在齿状回的颗粒层和多形层、CA区的锥体层和始层以及下托复合体的锥体层中鉴定出了GAT-1免疫反应性(-ir)和PV-ir的Ch终末。此外,与海马和齿状回不同的是,正常下托上层锥体层中的Ch终末亚群表达CB和PSA-NCAM。癫痫患者的硬化海马呈现出Ch终末和篮状结构令人印象深刻的形态和神经化学重组。这在齿状回和海马结构中很明显,但在下托中未出现,下托似乎保持不变。主要的是,在一些海马节段出现了大量且更复杂的PV-ir和CB-ir Ch终末以及密集的PV-ir篮状结构,而在其他区域则缺乏标记元素。这些变化不仅在不同患者之间有很大差异,而且在给定患者的不同海马区域内也有差异。一般来说,这些变化与患者观察到的临床特征或组织病理学改变程度无关,如颗粒细胞分散、神经元丢失和苔藓纤维增生。然而,在神经元丢失区域相邻的一些存活神经元始终被密集的篮状结构和复杂的Ch终末支配。这些结果表明,在人类癫痫海马中,GABA能回路的改变比以前认为的更为显著。与其他海马外改变一起考虑时,我们认为这些变化在与海马硬化相关的颞叶癫痫的病理生理学中很重要。

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