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培养的人成纤维细胞中L-谷氨酸转运的结构选择性和分子性质

Structural selectivity and molecular nature of L-glutamate transport in cultured human fibroblasts.

作者信息

Cooper B, Chebib M, Shen J, King N J, Darvey I G, Kuchel P W, Rothstein J D, Balcar V J

机构信息

Department of Anatomy and Histology, University of Sydney, NSW, Australia.

出版信息

Arch Biochem Biophys. 1998 May 15;353(2):356-64. doi: 10.1006/abbi.1998.0626.

DOI:10.1006/abbi.1998.0626
PMID:9606970
Abstract

Uptake of L-[3H]glutamate by monolayers of fibroblasts cultured from human embryonic skin has been studied in the presence of several nonradioactive structural analogs of glutamate and aspartate. Results have suggested that the structural specificites of glutamate transporters in cultured human fibroblasts are similar to those of glutamate transporters in the mammalian brain. Only subtle differences have been detected: in the mammalian cerebral cortex, enantiomers of threo-3-hydroxyaspartate are almost equipotent as inhibitors of L-[3H]glutamate uptake while, in human fibroblasts, the D-isomer has been found to be an order of magnitude less potent than the corresponding L-isomer. Kinetic analysis of a model in which substrates are recognized by the glutamate transporter binding site(s) as both alpha- and beta-amino acids indicated that such a mechanism cannot explain the apparent negative cooperativity characterizing the effects of D- and L-aspartate. Molecular modeling has been used to estimate the optimum conformation of L-glutamate as it interacts with the transporter(s). Flow cytometry has indicated that all fibroblasts in culture express at least moderate levels of four glutamate transporters cloned from human brain. Small subpopulations (< 3%) of cells, however, were strongly labeled with antibodies against EAAT1 (GLAST) and EAAT2 (GLT-1) transporters. We conclude that these two transporters--known to be strongly expressed in brain tissue--can be principally responsible for the "high affinity" transport of glutamate also in nonneural cells.

摘要

在几种谷氨酸和天冬氨酸的非放射性结构类似物存在的情况下,对从人胚胎皮肤培养的成纤维细胞单层摄取L-[3H]谷氨酸进行了研究。结果表明,培养的人成纤维细胞中谷氨酸转运体的结构特异性与哺乳动物脑中的谷氨酸转运体相似。仅检测到细微差异:在哺乳动物大脑皮层中,苏型-3-羟基天冬氨酸的对映体作为L-[3H]谷氨酸摄取的抑制剂几乎具有同等效力,而在人成纤维细胞中,发现D-异构体的效力比相应的L-异构体低一个数量级。对一种模型的动力学分析表明,底物被谷氨酸转运体结合位点识别为α-和β-氨基酸,这种机制无法解释D-和L-天冬氨酸作用所具有的明显负协同性。分子建模已用于估计L-谷氨酸与转运体相互作用时的最佳构象。流式细胞术表明,培养中的所有成纤维细胞至少中等水平表达从人脑中克隆的四种谷氨酸转运体。然而,一小部分细胞亚群(<3%)被抗EAAT1(GLAST)和EAAT2(GLT-1)转运体的抗体强烈标记。我们得出结论,这两种已知在脑组织中强烈表达的转运体,也可能是成纤维细胞中谷氨酸“高亲和力”转运的主要原因。

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