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小胶质细胞通过 GLT-1 和谷胱甘肽实现自我防御。

Microglial self-defence mediated through GLT-1 and glutathione.

机构信息

Department of Clinical Neuroscience and Rehabilitation, Institute of Neuroscience and Physiology, The Sahlgrenska Academy, University of Gothenburg, Per Dubbsgatan 14, 1tr, 41345, Gothenburg, Sweden.

出版信息

Amino Acids. 2012 Jan;42(1):207-19. doi: 10.1007/s00726-011-0865-7. Epub 2011 Mar 5.

DOI:10.1007/s00726-011-0865-7
PMID:21373770
Abstract

Glutamate is stored in synaptic vesicles in presynaptic neurons. It is released into the synaptic cleft to provide signalling to postsynaptic neurons. Normally, the astroglial glutamate transporters GLT-1 and GLAST take up glutamate to mediate a high signal-to-noise ratio in the synaptic signalling, and also to prevent excitotoxic effects by glutamate. In astrocytes, glutamate is transformed into glutamine, which is safely transported back to neurons. However, in pathological conditions, such as an ischemia or virus infection, astroglial transporters are down-regulated which could lead to excitotoxicity. Lately, it was shown that even microglia can express glutamate transporters during pathological events. Microglia have two systems for glutamate transport: GLT-1 for transport into the cells and the x (c) (-) system for transport out of the cells. We here review results from our work and others, which demonstrate that microglia in culture express GLT-1, but not GLAST, and transport glutamate from the extracellular space. We also show that TNF-α can induce increased microglial GLT-1 expression, possibly associating the expression with inflammatory systems. Furthermore, glutamate taken up through GLT-1 may be used for direct incorporation into glutathione and to fuel the intracellular glutamate pool to allow cystine uptake through the x (c) (-) system. This can lead to a defence against oxidative stress and have an antiviral function.

摘要

谷氨酸储存在突触前神经元的突触小泡中。它被释放到突触间隙中,为突触后神经元提供信号。通常,星形胶质细胞谷氨酸转运体 GLT-1 和 GLAST 摄取谷氨酸,以介导突触信号中的高信噪比,并防止谷氨酸的兴奋毒性作用。在星形胶质细胞中,谷氨酸被转化为谷氨酰胺,然后被安全地运输回神经元。然而,在病理条件下,如缺血或病毒感染,星形胶质细胞转运体下调,可能导致兴奋毒性。最近的研究表明,即使在病理事件中,小胶质细胞也可以表达谷氨酸转运体。小胶质细胞有两种谷氨酸转运系统:GLT-1 用于向细胞内转运,x(c)(-)系统用于从细胞外向细胞内转运。我们在这里回顾了我们和其他人的工作结果,这些结果表明,培养中的小胶质细胞表达 GLT-1,但不表达 GLAST,并从细胞外空间转运谷氨酸。我们还表明,TNF-α可以诱导小胶质细胞 GLT-1 的表达增加,这可能与炎症系统有关。此外,通过 GLT-1 摄取的谷氨酸可能被直接用于掺入谷胱甘肽中,并为细胞内谷氨酸池提供燃料,以允许通过 x(c)(-)系统摄取胱氨酸。这可以对抗氧化应激并具有抗病毒功能。

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