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首页> 外文期刊>The biochemical journal >Non-essential roles of cysteine residues in functional expression and redox regulatory pathways for canine glutamate/aspartate transporter based on mutagenic analysis
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Non-essential roles of cysteine residues in functional expression and redox regulatory pathways for canine glutamate/aspartate transporter based on mutagenic analysis

机译:基于诱变分析的半胱氨酸残基在犬谷氨酸/天冬氨酸转运蛋白的功能性表达和氧化还原调节途径中的非必需作用

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pA redox regulatory mechanism and a molecular link between oxidative and excitotoxic neurodegeneration have been postulated for high-affinity Nasup+/sup-dependent glutamate transporters. In the present study, mutations were introduced at three cysteine residues in canine glutamate/aspartate transporter (GLAST) to investigate the functional significance of thiol groups in response to oxidation. Cys(-) GLAST, in which all cysteines were replaced by other amino acids, as well as other mutants with disruption of one of three cysteine residues, showed insoluble oligomer formation, which was considered to be due to spontaneous and excessive oxidation as observed in wild-type GLAST. The mutant transporters also showed plasma-membrane localization and glutamate-transport kinetics that were very similar to those of wild-type GLAST. Glutamate-transport activities in COS-7 cells transfected with wild-type and Cys(-) GLAST were inhibited to the same degree when cells were exposed to Hgsup2+/sup and were recovered by the addition of thiol-specific reductant dithiothreitol. These findings suggest that cysteine residues are not critical in functional expression of GLAST and the redox-sensing pathway via glutamate transporters./p
机译:>高亲和力的Na + 依赖型谷氨酸转运体被认为具有氧化还原调节机制和氧化与兴奋性神经变性之间的分子联系。在本研究中,在犬谷氨酸/天冬氨酸转运蛋白(GLAST)的三个半胱氨酸残基处引入了突变,以研究巯基在氧化反应中的功能意义。 Cys(-)GLAST(其中所有半胱氨酸均被其他氨基酸取代,以及其他破坏了三个半胱氨酸残基之一的突变体)显示出不溶性低聚物的形成,这被认为是由于自发性和过度氧化所致。野生型GLAST。突变转运蛋白还显示出与野生型GLAST非常相似的血浆膜定位和谷氨酸转运动力学。当野生型和Cys(-)GLAST转染的COS-7细胞中的谷氨酸转运活性在暴露于Hg 2 + 时受到相同程度的抑制,并通过添加硫醇特定还原剂二硫苏糖醇。这些发现表明,半胱氨酸残基在谷氨酸转运蛋白的功能性表达和通过谷氨酸转运蛋白的氧化还原传感途径中并不关键。

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