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视觉皮层表观遗传的细胞类似物。I. 方向选择性的可塑性。

Cellular analogs of visual cortical epigenesis. I. Plasticity of orientation selectivity.

作者信息

Frégnac Y, Shulz D, Thorpe S, Bienenstock E

机构信息

Laboratoire de Neurobiologie et Neuropharmacologie du Développement, Université Paris XI, Orsay, France.

出版信息

J Neurosci. 1992 Apr;12(4):1280-300. doi: 10.1523/JNEUROSCI.12-04-01280.1992.

Abstract

A differential pairing procedure was applied in vivo to individual neurons in the primary visual cortex of anesthetized paralyzed cats, in order to produce changes in their relative orientation preference. While we recorded from a single cell, its visual response to a light bar was driven iontophoretically to a "high" level when stimulating with an initially nonpreferred orientation (S+), and alternately reduced to a "low" level when stimulating with the preferred orientation (S). This associative procedure was devised to test the possible role of neuronal coactivity in controlling the plasticity of orientation selectivity. Among 87 cells tested, 35 (40%) showed significant long-lasting changes, either in the relative orientation preference for the two "paired" stimuli S+ and S-, in the global orientation tuning profile, or in both. Measurements of relative orientation preference demonstrated significant effects in 27 cells (31%), all in favor of the positively reinforced orientation (S+). Modifications of orientation selectivity (studied over the entire orientation spectrum in 45 of the conditioned cells) usually consisted (21 out of 25 modified cells) of a competitive reorganization of the orientation tuning curve: the preferred orientation shifted toward S+, and a loss of relative visual responsiveness was observed for orientations close to the negatively reinforced orientation (S-). The largest changes were found in deprived kittens at the peak of the critical period, although the probability of inducing a significant change studied during the first year of postnatal life was independent of age. These functional modifications demonstrated at the cellular level are analogous to those induced by a global manipulation of the visual environment, when only a restricted spectrum of orientations is experienced during the critical period. Our results support the hypothesis that covariance levels between pre- and postsynaptic activity determine the sign and the amplitude of the modification of efficacy of cortical synapses.

摘要

在麻醉瘫痪的猫的初级视觉皮层中,对单个神经元应用了差异配对程序,以改变它们的相对方向偏好。在记录单个细胞时,当用最初非偏好的方向(S+)刺激时,其对光条的视觉反应通过离子电泳驱动到“高”水平,而当用偏好的方向(S)刺激时,反应交替降低到“低”水平。设计这种关联程序是为了测试神经元共同活动在控制方向选择性可塑性方面的可能作用。在测试的87个细胞中,35个(40%)在两个“配对”刺激S+和S-的相对方向偏好、全局方向调谐曲线或两者中都显示出显著的长期变化。相对方向偏好的测量在27个细胞(31%)中显示出显著影响,所有这些都有利于正向增强的方向(S+)。对45个条件细胞在整个方向谱上进行研究的方向选择性改变(25个改变的细胞中有21个)通常包括方向调谐曲线的竞争性重组:偏好方向向S+移动,并且观察到接近负向增强方向(S-)的方向的相对视觉反应性丧失。在关键期高峰的剥夺小猫中发现了最大的变化,尽管在出生后第一年研究诱导显著变化的概率与年龄无关。在细胞水平上证明的这些功能改变类似于在关键期仅经历有限方向谱时通过对视觉环境的全局操纵所诱导的改变。我们的结果支持这样的假设,即突触前和突触后活动之间的协方差水平决定了皮质突触效能改变的符号和幅度。

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