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Excitatory and inhibitory synaptic inputs are modulated by the spatial distribution of dendritic voltage-dependent channels: Modelling in realistic α-motoneuron

机译:兴奋性和抑制性突触输入受树突状电压依赖性通道的空间分布的调节:在真实的α-运动神经元中建模

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We simulated a reconstructed α-motoneuron by using realistic physiological and morphological parameters. In our simulations, we examined two distribution functions of the voltage-dependent sodium and potassium channels on the dendrites: (1) exponential decay (ED), illustrated by a high conductance density located proximal to the soma, exponentially decaying away from the soma; (2) exponential rise (ER), where the proximal low conductance density increases exponentially with the distance. We then tested the resulting excitatory postsynaptic potential (EPSP) and its inhibition by inhibitory postsynaptic potential (IPSP) under the above conditions and found that the introduction of a dendritic active conductance had prominent effects on the synaptic potentials. Our simulations lead to the following key observations: (1) the presence of the voltage-dependent channels in the dendrites is vital for obtaining EPSP_(peak) enhancement. (2) The EPSP_(peak) of the ED and ER models are similar, while the standard deviation (SD) of the EPSP_(peak) ED model compared to the ER model is larger. (3) Voltage dependent conductance, proximal to the soma, enhanced EPSP_(peak) inhibition significantly more than distally located active channels. (4) The EPSP_(peak) inhibition in the passive model is less efficient than in the ED model, but more than in the ER model.
机译:我们通过使用现实的生理和形态学参数模拟重建的α-运动神经元。在我们的模拟中,我们检查了树突上依赖电压的钠和钾通道的两个分布函数:(1)指数衰减(ED),以位于人体附近的高电导密度表示,远离人体成指数衰减。 (2)指数上升(ER),其中近端低电导密度随距离呈指数增长。然后,我们在上述条件下测试了所产生的兴奋性突触后电位(EPSP)及其被抑制性突触后电位(IPSP)的抑制作用,发现树突状活性电导的引入对突触电位具有显着影响。我们的仿真得出以下主要观察结果:(1)树突中存在电压依赖性通道对于获得EPSP_(peak)增强至关重要。 (2)ED模型和ER模型的EPSP_(peak)相似,而ER模型的EPSP_(peak)ED模型的标准差(SD)更大。 (3)与体表近端的电压依赖性电导相比,位于远端的活动通道增强了EPSP_(peak)抑制。 (4)被动模型中的EPSP_(peak)抑制比ED模型中的效率低,但比ER模型中的更高。

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