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首页> 外文期刊>The European Journal of Neuroscience >Model of very fast (> 75 Hz) network oscillations generated by electrical coupling between the proximal axons of cerebellar Purkinje cells.
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Model of very fast (> 75 Hz) network oscillations generated by electrical coupling between the proximal axons of cerebellar Purkinje cells.

机译:小脑浦肯野细胞近端轴突之间的电耦合产生的非常快的(> 75 Hz)网络振荡模型。

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Very fast oscillations (VFO; > 75 Hz) occur transiently in vivo, in the cerebellum of mice genetically modified to model Angelman syndrome, and in a mouse model of fetal alcohol syndrome. We recently reported VFO in slices of mouse cerebellar cortex (Crus I and II of ansiform and paramedian lobules), either in association with gamma oscillations ( approximately 40 Hz, evoked by nicotine) or in isolation [evoked by nicotine in combination with gamma-aminobutyric acid (GABA)(A) receptor blockade]. The experimental data suggest a role for electrical coupling between Purkinje cells (blockade of VFO by drugs reducing gap junction conductance and spikelets in some Purkinje cells); and the data suggest the specific involvement of Purkinje cell axons (because of field oscillation maxima in the granular layer). We show here that a detailed network model (1000 multicompartment Purkinje cells) replicates the experimental data when gap junctions are located on the proximal axons of Purkinje cells, provided sufficient spontaneous firing is present. Unlike other VFO models, most somatic spikelets do not correspond to axonal spikes in the parent axon, but reflect spikes in electrically coupled axons. The model predicts gating of VFO frequency by g(Na) inactivation, and experiments prolonging this inactivation time constant, with beta-pompilidotoxin, are consistent with this prediction. The model also predicts that cerebellar VFO can be explained as an electrically coupled system of axons that are not intrinsic oscillators: the electrically uncoupled cells do not individually oscillate (in the model) and axonal firing rates are much lower in the uncoupled state than in the coupled state.
机译:在体内,在转基因为Angelman综合征模型的小鼠小脑和胎儿酒精综合征的小鼠模型中,体内会短暂发生非常快速的振荡(VFO;> 75 Hz)。我们最近报道了与小脑振荡(大约40 Hz,由尼古丁引起)或分离[由尼古丁与γ-氨基丁酸联合引起]的小鼠小脑皮质切片(甲状旁腺和旁中小叶的克鲁斯I和II)中的VFO (GABA)(A)受体阻滞剂]。实验数据表明,Purkinje细胞之间的电耦合具有一定的作用(药物可降低间隙连接电导和某些Purkinje细胞中的小尖峰对VFO的阻断作用)。和数据表明浦肯野细胞轴突的具体参与(由于在颗粒层中的最大场振荡)。我们在这里显示出详细的网络模型(1000个多隔室的Purkinje细胞)复制了当缝隙连接位于Purkinje细胞的近轴突上的实验数据,条件是存在足够的自发放电。与其他VFO模型不同,大多数体细胞小穗并不对应于父轴突中的轴突突峰,而是反映了电耦合轴突中的突突。该模型通过g(Na)失活预测了VFO频率的门控,并且使用β-绒毛膜毒素延长该失活时间常数的实验与该预测一致。该模型还预测,小脑VFO可以解释为不是本征振荡器的轴突的电耦合系统:在模型中,未电耦合的细胞不会单独振荡,并且在未耦合状态时,轴突的发射率要比在耦合状态下低。耦合状态。

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