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视觉体验和随后的睡眠会诱导皮质神经元中假定的抑制性和兴奋性神经元的顺序发生可塑性变化。

Visual experience and subsequent sleep induce sequential plastic changes in putative inhibitory and excitatory cortical neurons.

机构信息

Department of Neuroscience, University of Pennsylvania, Philadelphia, PA 19104, USA.

出版信息

Proc Natl Acad Sci U S A. 2013 Feb 19;110(8):3101-6. doi: 10.1073/pnas.1208093110. Epub 2013 Jan 8.

Abstract

Ocular dominance plasticity in the developing primary visual cortex is initiated by monocular deprivation (MD) and consolidated during subsequent sleep. To clarify how visual experience and sleep affect neuronal activity and plasticity, we continuously recorded extragranular visual cortex fast-spiking (FS) interneurons and putative principal (i.e., excitatory) neurons in freely behaving cats across periods of waking MD and post-MD sleep. Consistent with previous reports in mice, MD induces two related changes in FS interneurons: a response shift in favor of the closed eye and depression of firing. Spike-timing-dependent depression of open-eye-biased principal neuron inputs to FS interneurons may mediate these effects. During post-MD nonrapid eye movement sleep, principal neuron firing increases and becomes more phase-locked to slow wave and spindle oscillations. Ocular dominance (OD) shifts in favor of open-eye stimulation--evident only after post-MD sleep--are proportional to MD-induced changes in FS interneuron activity and to subsequent sleep-associated changes in principal neuron activity. OD shifts are greatest in principal neurons that fire 40-300 ms after neighboring FS interneurons during post-MD slow waves. Based on these data, we propose that MD-induced changes in FS interneurons play an instructive role in ocular dominance plasticity, causing disinhibition among open-eye-biased principal neurons, which drive plasticity throughout the visual cortex during subsequent sleep.

摘要

在发育中的初级视觉皮层中,眼优势可塑性是由单眼剥夺 (MD) 引发的,并在随后的睡眠中得到巩固。为了阐明视觉经验和睡眠如何影响神经元活动和可塑性,我们在自由活动的猫中连续记录了颗粒外视觉皮层快速放电 (FS) 中间神经元和推定的主 (即兴奋性) 神经元,跨越清醒 MD 和 MD 后睡眠期。与之前在小鼠中的报告一致,MD 诱导 FS 中间神经元发生两种相关变化:对闭眼的反应转移和放电抑制。对 FS 中间神经元的睁眼优势主神经元输入的时依赖抑制可能介导这些效应。在 MD 后非快速眼动睡眠期间,主神经元放电增加,并与慢波和纺锤波振荡更加同步。仅在 MD 后睡眠后才明显的眼优势 (OD) 向睁眼刺激转移与 FS 中间神经元活动的 MD 诱导变化以及随后与睡眠相关的主神经元活动变化成正比。在 MD 后慢波期间,与相邻 FS 中间神经元后 40-300 毫秒放电的主神经元的 OD 转移最大。基于这些数据,我们提出 MD 诱导的 FS 中间神经元变化在眼优势可塑性中起着指导作用,导致睁眼优势主神经元之间的去抑制,从而在随后的睡眠期间驱动整个视觉皮层的可塑性。

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