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转运系统xc(-)的底物和非底物抑制剂的区分:L-谷氨酸和L-胱氨酸的专一性交换体

Differentiation of substrate and non-substrate inhibitors of transport system xc(-): an obligate exchanger of L-glutamate and L-cystine.

作者信息

Patel Sarjubhai A, Warren Brady A, Rhoderick Joseph F, Bridges Richard J

机构信息

Department of Biomedical and Pharmaceutical Sciences, University of Montana, Missoula, MT 59812, USA.

出版信息

Neuropharmacology. 2004 Feb;46(2):273-84. doi: 10.1016/j.neuropharm.2003.08.006.

DOI:10.1016/j.neuropharm.2003.08.006
PMID:14680765
Abstract

In addition to the well-characterized sodium-dependent excitatory amino acid transporters (EAATs) present in the mammalian CNS, a chloride-dependent, sodium-independent transporter has also been identified that is capable of mediating the uptake of L-glutamate. Named system x(c)(-), this transporter is an obligate exchanger that normally couples the export of intracellular L-glutamate with the import of extracellular L-cystine. Two cell lines that express high levels of system x(c)(-) are used to delineate the pharmacology of the transporter and demonstrate that it is distinct from both the EAATs and EAA ionotropic receptors. Potent competitive inhibitors of system x(c)(-) include: L-homocysteate, ibotenate, L-serine-O-sulphate, (RS)-4-bromohomoibotenate, quisqualate, and (S)-4-carboxyphenylglycine. A fluorescent-based assay that allows system x(c)(-)-mediated exchange of L-glutamate and L-cystine to be followed in real time is used to assess substrate activity. Interestingly, those compounds that proved to be the most potent competitive inhibitors (e.g. L-quisqualate and 4-S-CPG) also proved to be the least active as substrates, suggesting that distinct structural features may control binding and translocation. Lastly, the finding that a number of system x(c)(-) inhibitors are also commonly used as probes of excitotoxic pathology (e.g., L-quisqualate, ibotenate and L-homocysteate) raises some interesting questions regarding the mechanisms through which these analogues produce CNS damage.

摘要

除了哺乳动物中枢神经系统中特征明确的钠依赖性兴奋性氨基酸转运体(EAATs)外,还鉴定出一种氯依赖性、钠非依赖性转运体,它能够介导L-谷氨酸的摄取。这种转运体被命名为系统x(c)(-),是一种专一性交换体,通常将细胞内L-谷氨酸的输出与细胞外L-胱氨酸的输入偶联起来。两种高表达系统x(c)(-)的细胞系被用于描绘该转运体的药理学特性,并证明它与EAATs和离子otropic型兴奋性氨基酸受体都不同。系统x(c)(-)的强效竞争性抑制剂包括:L-高半胱氨酸、鹅膏蕈氨酸、L-丝氨酸-O-硫酸盐、(RS)-4-溴高鹅膏蕈氨酸、quisqualate和(S)-4-羧基苯甘氨酸。一种基于荧光的检测方法可实时跟踪系统x(c)(-)介导的L-谷氨酸和L-胱氨酸交换,用于评估底物活性。有趣的是,那些被证明是最有效的竞争性抑制剂的化合物(如L-quisqualate和4-S-CPG)也被证明是活性最低的底物,这表明不同的结构特征可能控制结合和转运。最后,一些系统x(c)(-)抑制剂也常用作兴奋性毒性病理学的探针(如L-quisqualate、鹅膏蕈氨酸和L-高半胱氨酸)这一发现,引发了一些关于这些类似物产生中枢神经系统损伤机制的有趣问题。

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