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L-脯氨酸和L-哌可酸在转染了高亲和力哺乳动物脑L-脯氨酸转运体的人胚肾293细胞中诱导脑啡肽敏感电流。

L-proline and L-pipecolate induce enkephalin-sensitive currents in human embryonic kidney 293 cells transfected with the high-affinity mammalian brain L-proline transporter.

作者信息

Galli A, Jayanthi L D, Ramsey I S, Miller J W, Fremeau R T, DeFelice L J

机构信息

Department of Pharmacology, University of Texas, Health Science Center, San Antonio, Texas 78284-7764, USA.

出版信息

J Neurosci. 1999 Aug 1;19(15):6290-7. doi: 10.1523/JNEUROSCI.19-15-06290.1999.

Abstract

The high-affinity mammalian brain L-proline transporter (PROT) belongs to the GAT1 gene family, which includes Na- and Cl-dependent plasma membrane carriers for neurotransmitters, osmolites, and metabolites. These transporters couple substrate flux to transmembrane electrochemical gradients, particularly the Na gradient. In the nervous system, transporters clear synapses and help to replenish transmitters in nerve terminals. The localization of PROT to specific excitatory terminals in rat forebrain suggests a role for this carrier in excitatory transmission (). We investigated the voltage regulation and electrogenicity of this novel transporter, using human embryonic kidney (HEK) 293 cells stably transfected with rat PROT cDNA. In physiological solutions between -140 and -40 mV, L-proline (PRO) and its six-member ring congener L-pipecolate (PIP) induced inward current. The current-voltage relationship and the variance of current fluctuations were similar for PRO- and PIP-induced current, and the ratio of induced variance to the mean current ranged from 20 to 60 fA. Des-Tyr-Leu-enkephalin (GGFL), a competitive peptide inhibitor of PROT, reduced the rat PROT-associated current to control levels. GGFL alone did not elicit currents, and the GGFL-sensitive substrate-induced current was absent in nontransfected cells. Finally, GGFL inhibited PROT-mediated transport only when applied to the extracellular face of PROT. These data suggest that (1) PROT uptake is electrogenic, (2) individual transporter currents are voltage-independent, and (3) GGFL is a nonsubstrate inhibitor that interacts either with an extracellular domain of PROT or in an externally accessible pore.

摘要

高亲和力的哺乳动物脑L-脯氨酸转运体(PROT)属于GAT1基因家族,该家族包括依赖钠和氯的质膜载体,用于转运神经递质、渗透溶质和代谢物。这些转运体将底物通量与跨膜电化学梯度,特别是钠梯度相偶联。在神经系统中,转运体清除突触并有助于在神经末梢补充递质。PROT在大鼠前脑特定兴奋性终末的定位表明该载体在兴奋性传递中发挥作用()。我们使用稳定转染大鼠PROT cDNA的人胚肾(HEK)293细胞,研究了这种新型转运体的电压调节和电生性。在-140至-40 mV的生理溶液中,L-脯氨酸(PRO)及其六元环同系物L-哌啶酸(PIP)诱导内向电流。PRO和PIP诱导电流的电流-电压关系以及电流波动的方差相似,诱导方差与平均电流的比值范围为20至60 fA。PROT的竞争性肽抑制剂去酪氨酸-亮氨酸-脑啡肽(GGFL)将大鼠PROT相关电流降低至对照水平。单独的GGFL不引发电流,未转染的细胞中不存在GGFL敏感的底物诱导电流。最后,GGFL仅在应用于PROT的细胞外表面时才抑制PROT介导的转运。这些数据表明:(1)PROT摄取是电生性的;(2)单个转运体电流与电压无关;(3)GGFL是一种非底物抑制剂,它与PROT的细胞外结构域或外部可及的孔相互作用。

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