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二维中心-环绕反馈网络中癫痫传播的机制。

Mechanisms of seizure propagation in 2-dimensional centre-surround recurrent networks.

机构信息

Victoria Research Labs, National ICT Australia, Parkville, Victoria, Australia.

出版信息

PLoS One. 2013 Aug 13;8(8):e71369. doi: 10.1371/journal.pone.0071369. eCollection 2013.

Abstract

Understanding how seizures spread throughout the brain is an important problem in the treatment of epilepsy, especially for implantable devices that aim to avert focal seizures before they spread to, and overwhelm, the rest of the brain. This paper presents an analysis of the speed of propagation in a computational model of seizure-like activity in a 2-dimensional recurrent network of integrate-and-fire neurons containing both excitatory and inhibitory populations and having a difference of Gaussians connectivity structure, an approximation to that observed in cerebral cortex. In the same computational model network, alternative mechanisms are explored in order to simulate the range of seizure-like activity propagation speeds (0.1-100 mm/s) observed in two animal-slice-based models of epilepsy: (1) low extracellular [Formula: see text], which creates excess excitation and (2) introduction of gamma-aminobutyric acid (GABA) antagonists, which reduce inhibition. Moreover, two alternative connection topologies are considered: excitation broader than inhibition, and inhibition broader than excitation. It was found that the empirically observed range of propagation velocities can be obtained for both connection topologies. For the case of the GABA antagonist model simulation, consistent with other studies, it was found that there is an effective threshold in the degree of inhibition below which waves begin to propagate. For the case of the low extracellular [Formula: see text] model simulation, it was found that activity-dependent reductions in inhibition provide a potential explanation for the emergence of slowly propagating waves. This was simulated as a depression of inhibitory synapses, but it may also be achieved by other mechanisms. This work provides a localised network understanding of the propagation of seizures in 2-dimensional centre-surround networks that can be tested empirically.

摘要

了解癫痫发作如何在大脑中传播是治疗癫痫的一个重要问题,特别是对于旨在在局灶性癫痫发作扩散到大脑其他部位并使其不堪重负之前阻止其发作的植入式设备。本文对二维递归网络中癫痫样活动的计算模型中的传播速度进行了分析。该网络由整合-点火神经元组成,包含兴奋和抑制两种神经元群体,其连接结构为高斯差异,近似于大脑皮层中的观察结果。在同一个计算模型网络中,探索了替代机制,以模拟在两种基于动物切片的癫痫模型中观察到的癫痫样活动传播速度范围(0.1-100mm/s):(1)低细胞外[Formula: see text],可导致过度兴奋;(2)引入γ-氨基丁酸(GABA)拮抗剂,可减少抑制。此外,还考虑了两种替代连接拓扑结构:兴奋比抑制宽,抑制比兴奋宽。结果发现,对于这两种连接拓扑结构,都可以得到观察到的传播速度范围。对于 GABA 拮抗剂模型模拟的情况,与其他研究一致,发现抑制程度存在有效阈值,低于该阈值,波就会开始传播。对于低细胞外[Formula: see text]模型模拟的情况,发现抑制的活动依赖性降低为缓慢传播波的出现提供了一个潜在的解释。这被模拟为抑制性突触的抑制,但也可能通过其他机制实现。这项工作为二维中心-环绕网络中癫痫发作的传播提供了一个局部网络理解,可以通过实验进行检验。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8496/3742758/363314078068/pone.0071369.g001.jpg

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