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调控神经元细胞中 xCT 表达和系统 x(c)(-)功能。

Regulation of xCT expression and system x (c) (-) function in neuronal cells.

机构信息

Department of Neurology, University Medical Center Hamburg-Eppendorf, Martinistraße 52, 20241, Hamburg, Germany.

出版信息

Amino Acids. 2012 Jan;42(1):171-9. doi: 10.1007/s00726-011-0862-x. Epub 2011 Mar 3.

DOI:10.1007/s00726-011-0862-x
PMID:21369940
Abstract

The glutamate/cystine antiporter system x(c)(-) transports cystine into cells in exchange for glutamate at a ratio of 1:1. It is composed of a specific light chain, xCT, and a heavy chain, 4F2, linked by a disulfide bridge. Intracellularly, cystine is reduced into cysteine, the rate-limiting precursor of glutathione (GSH), an important small molecule antioxidant. Several lines of evidence suggest that the expression of xCT and thereby the presence system x(c)(-) activity plays an important role in the brain. First, it regulates extracellular glutamate concentrations. Second, as brain is prone to oxidative stress due to its high oxygen consumption and lipid content, system x(c)(-) by favoring GSH synthesis, may prevent oxidative damage. Thus, to understand how xCT expression and system x(c)(-) activity are regulated in the central nervous system is of utmost importance. In this review, we will summarize the current knowledge about the molecular basis by which xCT expression and system x(c)(-) activity are regulated in neuronal cell lines, especially the hippocampal cell line, HT22. In addition, we will relate these pathways to findings in other cell types, especially those found in the central nervous system. We will focus on the signaling pathways that modulate the transcription of the xCT gene. Furthermore, we describe possible pathways that modify system x(c)(-) activity beyond the level of xCT transcription, including regulation on the level of membrane trafficking and substrate availability, especially the regulation by glutamate transport through excitatory amino acid transporters.

摘要

谷氨酸/胱氨酸反向转运蛋白系统 x(c)(-)以 1:1 的比例将胱氨酸转运到细胞内,交换谷氨酸。它由一个特定的轻链 xCT 和一个重链 4F2 通过二硫键连接组成。在细胞内,胱氨酸被还原成半胱氨酸,半胱氨酸是谷胱甘肽 (GSH) 的限速前体,GSH 是一种重要的小分子抗氧化剂。有几条证据表明,xCT 的表达及其系统 x(c)(-)活性的存在在大脑中起着重要作用。首先,它调节细胞外谷氨酸浓度。其次,由于大脑的耗氧量和脂质含量高,容易受到氧化应激的影响,系统 x(c)(-)通过促进 GSH 的合成,可能预防氧化损伤。因此,了解 xCT 表达和系统 x(c)(-)活性在中枢神经系统中的调节方式至关重要。在这篇综述中,我们将总结目前关于神经元细胞系(特别是海马细胞系 HT22)中 xCT 表达和系统 x(c)(-)活性调节的分子基础的知识。此外,我们将这些途径与其他细胞类型(特别是中枢神经系统中的细胞类型)的发现联系起来。我们将重点介绍调节 xCT 基因转录的信号通路。此外,我们还描述了可能调节系统 x(c)(-)活性的途径,这些途径超出了 xCT 转录的水平,包括通过兴奋性氨基酸转运蛋白调节膜转运和底物可用性的调节,特别是谷氨酸转运的调节。

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