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海马中间神经元网络介导的4-氨基吡啶诱导的、GABA(A)依赖性自发同步活动的成像。

Imaging of 4-AP-induced, GABA(A)-dependent spontaneous synchronized activity mediated by the hippocampal interneuron network.

作者信息

Sinha S R, Saggau P

机构信息

Division of Neuroscience, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

J Neurophysiol. 2001 Jul;86(1):381-91. doi: 10.1152/jn.2001.86.1.381.

Abstract

Under conditions of increased excitability, such as application of the K(+) channel blocker 4-aminopyridine (4-AP, 100 microM), interneurons in the hippocampal slice show an additional form of synchronized activity that is distinct from the ictal and interictal epileptiform activity induced by these manipulations. In principal neurons, i.e., pyramidal and granule cells, this synchronized interneuron activity (SIA) generates large, multi-component synaptic potentials, which have been termed long-lasting depolarizations (LLDs). These LLDs are dependent on GABA(A) receptor-mediated synaptic transmission but not on excitatory amino acid (EAA) receptors. Intracellular recordings from hilar interneurons have shown that depolarizing GABA(A) receptor-mediated synaptic potentials are also largely responsible for the synchronization of interneurons. The spatiotemporal characteristics of this interneuron activity have not been investigated previously. Using a voltage-sensitive dye and optical techniques that are capable of recording spontaneous synchronized activity, we have characterized the spatiotemporal pattern of SIA (in the presence of 4-AP + EAA receptor antagonists) and compared it with interictal epileptiform activity (in 4-AP only). Like interictal activity, SIA could be observed throughout the hippocampal slice. Unlike interictal activity, which originated in area CA2/CA3 and spread from there, SIA was most prominent in area CA1 and originated either there or in the subiculum. In CA1, interictal activity was largest in and near stratum pyramidale, while SIA was mainly located in s. lacunosum moleculare. Furthermore SIA was equally likely to propagate in either direction, and multiple patterns of propagation could be observed within a single brain slice. These studies suggest that hippocampal area CA1 has the highest propensity for SIA, that multiple locations can serve as the site of origin, and that interneurons located in s. lacunosum moleculare or interneurons that specifically project to this region may be particularly important for synchronized interneuron activity.

摘要

在兴奋性增加的条件下,如应用钾离子通道阻滞剂4-氨基吡啶(4-AP,100微摩尔),海马切片中的中间神经元会表现出一种额外的同步活动形式,这种活动不同于由这些操作诱导的发作期和发作间期癫痫样活动。在主要神经元,即锥体细胞和颗粒细胞中,这种同步中间神经元活动(SIA)会产生大的、多成分的突触电位,这些电位被称为长时程去极化(LLD)。这些LLD依赖于GABA(A)受体介导的突触传递,而不依赖于兴奋性氨基酸(EAA)受体。来自海马门区中间神经元的细胞内记录表明,去极化的GABA(A)受体介导的突触电位在很大程度上也负责中间神经元的同步化。这种中间神经元活动的时空特征此前尚未被研究过。我们使用电压敏感染料和能够记录自发同步活动的光学技术,对SIA的时空模式(在存在4-AP + EAA受体拮抗剂的情况下)进行了表征,并将其与发作间期癫痫样活动(仅在4-AP中)进行了比较。与发作间期活动一样,SIA在整个海马切片中都能观察到。与起源于CA2/CA3区并从那里扩散的发作间期活动不同,SIA在CA1区最为显著,起源于该区或海马下托。在CA1区,发作间期活动在锥体层及其附近最大,而SIA主要位于分子层的腔隙层。此外,SIA向两个方向传播的可能性相同,并且在单个脑切片中可以观察到多种传播模式。这些研究表明,海马CA1区具有最高的SIA倾向,多个位置可作为起源部位,并且位于分子层腔隙层的中间神经元或专门投射到该区域的中间神经元对于同步中间神经元活动可能特别重要。

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