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大鼠中枢神经系统中GLT-1两种剪接变体的克隆、转运特性及差异定位:对中枢神经系统谷氨酸稳态的影响

Cloning, transport properties, and differential localization of two splice variants of GLT-1 in the rat CNS: implications for CNS glutamate homeostasis.

作者信息

Sullivan Robert, Rauen Thomas, Fischer Frauke, Wiessner Michael, Grewer Christof, Bicho Ana, Pow David V

机构信息

School of Biomedical Sciences, Department of Physiology and Pharmacology, University of Queensland, Brisbane 4072, Australia.

出版信息

Glia. 2004 Jan 15;45(2):155-69. doi: 10.1002/glia.10317.

DOI:10.1002/glia.10317
PMID:14730709
Abstract

At least two splice variants of GLT-1 are expressed by rat brain astrocytes, albeit in different membrane domains. There is at present only limited data available as to the spatial relationship of such variants relative to the location of synapses and their functional properties. We have characterized the transport properties of GLT-1v in a heterologous expression system and conclude that its transport properties are similar to those of the originally described form of GLT-1, namely GLT-1alpha. We demonstrate that GLT-1alpha is localized to glial processes, some of which are interposed between multiple synapse types, including GABAergic synapses, whereas GLT-1v is expressed by astrocytic processes, at sites not interposed between synapses. Both splice variants can be expressed by a single astrocyte, but such expression is not uniform over the surface of the astrocytes. Neither splice variant of GLT-1 is evident in brain neurons, but both are abundantly expressed in some retinal neurons. We conclude that GLT-1v may not be involved in shaping the kinetics of synaptic signaling in the brain, but may be critical in preventing spillover of glutamate between adjacent synapses, thereby regulating intersynaptic glutamatergic and GABAergic transmission. Furthermore, GLT-1v may be crucial in ensuring that low levels of glutamate are maintained at extrasynaptic locations, especially in pathological conditions such as ischemia, motor neurone disease, and epilepsy.

摘要

大鼠脑星形胶质细胞表达至少两种GLT-1剪接变体,尽管它们位于不同的膜结构域。目前,关于这些变体相对于突触位置及其功能特性的空间关系,仅有有限的数据。我们在异源表达系统中对GLT-1v的转运特性进行了表征,并得出结论,其转运特性与最初描述的GLT-1形式(即GLT-1α)相似。我们证明GLT-1α定位于胶质细胞突起,其中一些位于多种突触类型之间,包括GABA能突触,而GLT-1v由星形胶质细胞突起在不位于突触之间的位点表达。两种剪接变体均可由单个星形胶质细胞表达,但这种表达在星形胶质细胞表面并不均匀。GLT-1的两种剪接变体在脑神经元中均不明显,但在一些视网膜神经元中均大量表达。我们得出结论,GLT-1v可能不参与塑造大脑中突触信号传导的动力学,但可能在防止谷氨酸在相邻突触之间溢出从而调节突触间谷氨酸能和GABA能传递方面至关重要。此外,GLT-1v对于确保突触外位置维持低水平的谷氨酸可能至关重要,尤其是在诸如缺血、运动神经元疾病和癫痫等病理状况下。

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