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由单个星形胶质细胞区域所界定的突触岛。

Synaptic islands defined by the territory of a single astrocyte.

作者信息

Halassa Michael M, Fellin Tommaso, Takano Hajime, Dong Jing-Hui, Haydon Philip G

机构信息

Silvio Conte Center for Integration at the Tripartite Synapse, Department of Neuroscience, University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Neurosci. 2007 Jun 13;27(24):6473-7. doi: 10.1523/JNEUROSCI.1419-07.2007.

Abstract

In the mammalian brain, astrocytes modulate neuronal function, in part, by synchronizing neuronal firing and coordinating synaptic networks. Little, however, is known about how this is accomplished from a structural standpoint. To investigate the structural basis of astrocyte-mediated neuronal synchrony and synaptic coordination, the three-dimensional relationships between cortical astrocytes and neurons was investigated. Using a transgenic and viral approach to label astrocytes with enhanced green fluorescent protein, we performed a three-dimensional reconstruction of astrocytes from tissue sections or live animals in vivo. We found that cortical astrocytes occupy nonoverlapping territories similar to those described in the hippocampus. Using immunofluorescence labeling of neuronal somata, a single astrocyte enwraps on average four neuronal somata with an upper limit of eight. Single-neuron dye-fills allowed us to estimate that one astrocyte contacts 300-600 neuronal dendrites. Together with the recent findings showing that glial Ca2+ signaling is restricted to individual astrocytes in vivo, and that Ca2+ signaling leads to gliotransmission, we propose the concept of functional islands of synapses in which groups of synapses confined within the boundaries of an individual astrocyte are modulated by the gliotransmitter environment controlled by that astrocyte. Our description offers a new structurally based conceptual framework to evaluate functional data involving interactions between neurons and astrocytes in the mammalian brain.

摘要

在哺乳动物大脑中,星形胶质细胞部分地通过同步神经元放电和协调突触网络来调节神经元功能。然而,从结构角度来看,对于这一过程是如何实现的却知之甚少。为了研究星形胶质细胞介导的神经元同步性和突触协调的结构基础,我们研究了皮质星形胶质细胞与神经元之间的三维关系。利用转基因和病毒方法用增强型绿色荧光蛋白标记星形胶质细胞,我们对组织切片或活体动物体内的星形胶质细胞进行了三维重建。我们发现皮质星形胶质细胞占据着与海马体中所描述的类似的非重叠区域。通过对神经元胞体进行免疫荧光标记,单个星形胶质细胞平均包裹四个神经元胞体,上限为八个。对单个神经元进行染料填充使我们能够估计一个星形胶质细胞与300 - 600个神经元树突相接触。结合最近的研究结果表明,胶质细胞Ca2+信号在体内局限于单个星形胶质细胞,并且Ca2+信号导致胶质递质释放,我们提出了突触功能岛的概念,即局限于单个星形胶质细胞边界内的突触群受到该星形胶质细胞控制的胶质递质环境的调节。我们的描述提供了一个基于结构的新的概念框架,用于评估涉及哺乳动物大脑中神经元与星形胶质细胞相互作用的功能数据。

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