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海马体中突触外谷氨酸的扩散:超微结构限制、摄取及受体激活

Extrasynaptic glutamate diffusion in the hippocampus: ultrastructural constraints, uptake, and receptor activation.

作者信息

Rusakov D A, Kullmann D M

机构信息

Department of Biology, The Open University, Milton Keynes MK7 6AA, United Kingdom.

出版信息

J Neurosci. 1998 May 1;18(9):3158-70. doi: 10.1523/JNEUROSCI.18-09-03158.1998.

Abstract

Fast excitatory synapses are generally thought to act as private communication channels between presynaptic and postsynaptic neurons. Some recent findings, however, suggest that glutamate may diffuse out of the synaptic cleft and bind to several subtypes of receptors, either in the perisynaptic membrane or at neighboring synapses. It is not known whether activation of these receptors can occur in response to the release of a single vesicle of glutamate. Here we estimate the spatiotemporal profile of glutamate in the extrasynaptic space after vesicle exocytosis, guided by detailed ultrastructural measurements of the CA1 neuropil in the adult rat. We argue that the vicinity of the synapse can be treated as an isotropic porous medium, in which diffusion is determined by the extracellular volume fraction and the tortuosity factor, and develop novel stereological methods to estimate these parameters. We also estimate the spatial separation between synapses, to ask whether glutamate released at one synapse can activate NMDA and other high-affinity receptors at a neighboring synapse. Kinetic simulations of extrasynaptic glutamate uptake show that transporters rapidly reduce the free concentration of transmitter. Exocytosis of a single vesicle is, however, sufficient to bind to high-affinity receptors situated in the immediate perisynaptic space. The distance separating a typical synapse from its nearest neighbor is approximately 465 nm. Whether glutamate can reach a sufficient concentration to activate NMDA receptors at this distance depends critically on the diffusion coefficient in the extracellular space. If diffusion is much slower than in free aqueous solution, NMDA receptors could mediate crosstalk between neighboring synapses.

摘要

快速兴奋性突触通常被认为是突触前神经元和突触后神经元之间的专用通信通道。然而,最近的一些研究结果表明,谷氨酸可能会扩散出突触间隙,并与突触周围膜或相邻突触处的几种受体亚型结合。尚不清楚这些受体的激活是否能响应单个谷氨酸囊泡的释放而发生。在这里,我们在对成年大鼠CA1神经纤维网进行详细的超微结构测量的指导下,估计了囊泡胞吐后突触外空间中谷氨酸的时空分布。我们认为突触附近可被视为各向同性多孔介质,其中扩散由细胞外体积分数和曲折因子决定,并开发了新的体视学方法来估计这些参数。我们还估计了突触之间的空间距离,以探讨在一个突触释放的谷氨酸是否能激活相邻突触处的NMDA和其他高亲和力受体。突触外谷氨酸摄取的动力学模拟表明,转运体迅速降低了递质的游离浓度。然而,单个囊泡的胞吐足以与紧邻突触周围空间中的高亲和力受体结合。一个典型突触与其最近邻突触之间的距离约为465纳米。谷氨酸在此距离能否达到足以激活NMDA受体的浓度,关键取决于细胞外空间中的扩散系数。如果扩散比在自由水溶液中慢得多,NMDA受体可能介导相邻突触之间的串扰。

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