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大鼠体感皮层抑制性中间神经元中宽带电导输入的整合:快速放电细胞中内在和输入驱动放电之间的抑制控制开关

Integration of broadband conductance input in rat somatosensory cortical inhibitory interneurons: an inhibition-controlled switch between intrinsic and input-driven spiking in fast-spiking cells.

作者信息

Tateno T, Robinson H P C

机构信息

Department of Physiology, Development, and Neuroscience, University of Cambridge, Cambridge, UK.

出版信息

J Neurophysiol. 2009 Feb;101(2):1056-72. doi: 10.1152/jn.91057.2008. Epub 2008 Dec 17.


DOI:10.1152/jn.91057.2008
PMID:19091918
Abstract

Quantitative understanding of the dynamics of particular cell types when responding to complex, natural inputs is an important prerequisite for understanding the operation of the cortical network. Different types of inhibitory neurons are connected by electrical synapses to nearby neurons of the same type, enabling the formation of synchronized assemblies of neurons with distinct dynamical behaviors. Under what conditions is spike timing in such cells determined by their intrinsic dynamics and when is it driven by the timing of external input? In this study, we have addressed this question using a systematic approach to characterizing the input-output relationships of three types of cortical interneurons (fast spiking [FS], low-threshold spiking [LTS], and nonpyramidal regular-spiking [NPRS] cells) in the rat somatosensory cortex, during fluctuating conductance input designed to mimic natural complex activity. We measured the shape of average conductance input trajectories preceding spikes and fitted a two-component linear model of neuronal responses, which included an autoregressive term from its own output, to gain insight into the input-output relationships of neurons. This clearly separated the contributions of stimulus and discharge history, in a cell-type dependent manner. Unlike LTS and NPRS cells, FS cells showed a remarkable switch in dynamics, from intrinsically driven spike timing to input-fluctuation-controlled spike timing, with the addition of even a small amount of inhibitory conductance. Such a switch could play a pivotal role in the function of FS cells in organizing coherent gamma oscillations in the local cortical network. Using both pharmacological perturbations and modeling, we show how this property is a consequence of the particular complement of voltage-dependent conductances in these cells.

摘要

定量理解特定细胞类型在对复杂自然输入做出反应时的动态变化,是理解皮层网络运作的重要前提。不同类型的抑制性神经元通过电突触与同类型的附近神经元相连,从而能够形成具有不同动态行为的神经元同步集合。在何种条件下,此类细胞的尖峰时间由其内在动态决定,又在何时由外部输入的时间驱动?在本研究中,我们采用系统方法来表征大鼠体感皮层中三种类型的皮层中间神经元(快速放电[FS]、低阈值放电[LTS]和非锥体常规放电[NPRS]细胞)的输入-输出关系,期间施加波动电导输入以模拟自然复杂活动。我们测量了尖峰之前平均电导输入轨迹的形状,并拟合了神经元反应的双组分线性模型,该模型包括来自其自身输出的自回归项,以深入了解神经元的输入-输出关系。这以细胞类型依赖的方式清晰地分离了刺激和放电历史的贡献。与LTS和NPRS细胞不同,FS细胞在动态变化上表现出显著的转变,从内在驱动的尖峰时间转变为输入波动控制的尖峰时间,即使添加少量抑制性电导也会如此。这种转变可能在FS细胞在组织局部皮层网络中相干伽马振荡的功能中起关键作用。通过药理学扰动和建模,我们展示了这种特性是这些细胞中电压依赖性电导特定组合的结果。

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[1]
Integration of broadband conductance input in rat somatosensory cortical inhibitory interneurons: an inhibition-controlled switch between intrinsic and input-driven spiking in fast-spiking cells.

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引用本文的文献

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J Neurosci. 2019-7-25

[2]
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IEEE Trans Biomed Eng. 2014-5

[3]
Toggling between gamma-frequency activity and suppression of cell assemblies.

Front Comput Neurosci. 2013-4-16

[4]
The Hodgkin-Huxley heritage: from channels to circuits.

J Neurosci. 2012-10-10

[5]
Impact of gamma-oscillatory inhibition on the signal transmission of a cortical pyramidal neuron.

Cogn Neurodyn. 2011-8-30

[6]
Mechanisms of gamma oscillations.

Annu Rev Neurosci. 2012-3-20

[7]
The ionic mechanism of gamma resonance in rat striatal fast-spiking neurons.

J Neurophysiol. 2011-8-31

[8]
Using computer simulations to determine the limitations of dynamic clamp stimuli applied at the soma in mimicking distributed conductance sources.

J Neurophysiol. 2011-2-16

[9]
Synchronization of firing in cortical fast-spiking interneurons at gamma frequencies: a phase-resetting analysis.

PLoS Comput Biol. 2010-9-30

[10]
Consistency and diversity of spike dynamics in the neurons of bed nucleus of stria terminalis of the rat: a dynamic clamp study.

PLoS One. 2010-8-3

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