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首页> 外文期刊>Journal of biosciences >Modulation of synaptic potentials and cell excitability by dendritic KIR and KAS channels in nucleus accumbens medium spiny neurons: A computational study
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Modulation of synaptic potentials and cell excitability by dendritic KIR and KAS channels in nucleus accumbens medium spiny neurons: A computational study

机译:树突状KIR和KAS通道对伏伏核棘中枢神经元突触电位和细胞兴奋性的调节:计算研究

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摘要

The nucleus accumbens (NAc), a critical structure of the brain reward circuit, is implicated in normal goal-directed behaviour and learning as well as pathological conditions like schizophrenia and addiction. Its major cellular substrates, the medium spiny (MS) neurons, possess a wide variety of dendritic active conductances that may modulate the excitatory post synaptic potentials (EPSPs) and cell excitability. We examine this issue using a biophysically detailed 189-compartment stylized model of the NAc MS neuron, incorporating all the known active conductances. We find that, of all the active channels, inward rectifying K+ (KIR) channels play the primary role in modulating the resting membrane potential (RMP) and EPSPs in the down-state of the neuron. Reduction in the conductance of KIR channels evokes facilitatory effects on EPSPs accompanied by rises in local input resistance and membrane time constant. At depolarized membrane potentials closer to up-state levels, the slowly inactivating A-type potassium channel (KAs) conductance also plays a strong role in determining synaptic potential parameters and cell excitability. We discuss the implications of our results for the regulation of accumbal MS neuron biophysics and synaptic integration by intrinsic factors and extrinsic agents such as dopamine.
机译:伏伏核(NAc)是大脑奖励回路的关键结构,与正常的目标定向行为和学习以及诸如精神分裂症和成瘾的病理状况有关。它的主要细胞底物,中棘(MS)神经元,具有各种各样的树突状活性电导,可以调节兴奋性突触后电位(EPSPs)和细胞兴奋性。我们使用NAc MS神经元的生物物理学详细的189室程式化模型,并结合了所有已知的主动电导,研究了这个问题。我们发现,在所有活动通道中,向内整流K +(KIR)通道在调节神经元下降状态下的静息膜电位(RMP)和EPSPs中起主要作用。 KIR通道电导的降低会引起对EPSP的促进作用,并伴有局部输入电阻和膜时间常数的增加。在去极化的膜电位接近上位状态时,缓慢失活的A型钾通道(KAs)电导在确定突触电位参数和细胞兴奋性方面也起着重要作用。我们讨论了我们的研究结果对内在因素和外在因素(如多巴胺)对MS型神经元生物物理调控和突触整合的影响。

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