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由细胞类型选择性光遗传学驱动的不同新皮层振荡的计算模型:由低阈值发放和快速发放中间神经元控制的可分离共振回路。

Computational modeling of distinct neocortical oscillations driven by cell-type selective optogenetic drive: separable resonant circuits controlled by low-threshold spiking and fast-spiking interneurons.

作者信息

Vierling-Claassen Dorea, Cardin Jessica A, Moore Christopher I, Jones Stephanie R

机构信息

McGovern Institute of Brain Research, Massachusetts Institute of Technology Cambridge, MA, USA.

出版信息

Front Hum Neurosci. 2010 Nov 22;4:198. doi: 10.3389/fnhum.2010.00198. eCollection 2010.

Abstract

Selective optogenetic drive of fast-spiking (FS) interneurons (INs) leads to enhanced local field potential (LFP) power across the traditional "gamma" frequency band (20-80 Hz; Cardin et al., 2009). In contrast, drive to regular-spiking (RS) pyramidal cells enhances power at lower frequencies, with a peak at 8 Hz. The first result is consistent with previous computational studies emphasizing the role of FS and the time constant of GABA(A) synaptic inhibition in gamma rhythmicity. However, the same theoretical models do not typically predict low-frequency LFP enhancement with RS drive. To develop hypotheses as to how the same network can support these contrasting behaviors, we constructed a biophysically principled network model of primary somatosensory neocortex containing FS, RS, and low-threshold spiking (LTS) INs. Cells were modeled with detailed cell anatomy and physiology, multiple dendritic compartments, and included active somatic and dendritic ionic currents. Consistent with prior studies, the model demonstrated gamma resonance during FS drive, dependent on the time constant of GABA(A) inhibition induced by synchronous FS activity. Lower-frequency enhancement during RS drive was replicated only on inclusion of an inhibitory LTS population, whose activation was critically dependent on RS synchrony and evoked longer-lasting inhibition. Our results predict that differential recruitment of FS and LTS inhibitory populations is essential to the observed cortical dynamics and may provide a means for amplifying the natural expression of distinct oscillations in normal cortical processing.

摘要

对快速发放(FS)中间神经元(INs)进行选择性光遗传学驱动会导致传统“γ”频段(20 - 80赫兹;Cardin等人,2009年)的局部场电位(LFP)功率增强。相比之下,对规则发放(RS)锥体细胞的驱动会增强较低频率的功率,峰值在8赫兹。第一个结果与之前强调FS作用以及GABA(A)突触抑制时间常数在γ节律性中的作用的计算研究一致。然而,相同的理论模型通常并不预测RS驱动会增强低频LFP。为了就同一网络如何支持这些不同行为提出假设,我们构建了一个包含FS、RS和低阈值发放(LTS)INs的初级体感新皮层的生物物理原理网络模型。细胞通过详细的细胞解剖结构和生理学、多个树突隔室进行建模,并包括活跃的体细胞和树突离子电流。与先前的研究一致,该模型在FS驱动期间表现出γ共振,这取决于同步FS活动诱导的GABA(A)抑制的时间常数。仅在纳入一个抑制性LTS群体后才重现了RS驱动期间的低频增强,其激活关键取决于RS同步性并诱发更持久的抑制。我们的结果预测,FS和LTS抑制性群体的差异募集对于观察到的皮层动力学至关重要,并且可能为放大正常皮层处理中不同振荡的自然表达提供一种手段。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/655b/2996257/7d7abcf7e98c/fnhum-04-00198-g001.jpg

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