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控制哺乳动物血清素转运体中与转运相关电流的pH调节的氨基酸残基。

Amino acid residues that control pH modulation of transport-associated current in mammalian serotonin transporters.

作者信息

Cao Y, Li M, Mager S, Lester H A

机构信息

Division of Biology, California Institute of Technology, Pasadena, California 91125, USA.

出版信息

J Neurosci. 1998 Oct 1;18(19):7739-49. doi: 10.1523/JNEUROSCI.18-19-07739.1998.

Abstract

The rat and human serotonin transporters (rSERT and hSERT, respectively) were expressed in Xenopus oocytes and studied using site-directed mutagenesis, electrophysiological recordings, and [3H]5-HT uptake measurements. rSERT, but not hSERT, displayed increased transport-associated current at low pH. Chimeras and point mutations showed that, of the 52 nonidentical residues, a single residue at position 490 (threonine in rSERT and lysine in hSERT) governs this difference. Furthermore, potentiation required the glutamate residue at position 493. Cysteine substitution and alkylation experiments showed that residue 493 is extracellular. Cysteine at 493 increased, whereas aspartate decreased, the net charge movement per transported 5-HT molecule. The mutations at this region did not significantly affect other aspects of SERT function, including agonist-independent leakage current, voltage-dependent transient current, and H+ current. This region may therefore be part of an external gate required for rSERT function. The data and analyses show that, in the absence of detailed structural information, a gate-lumen-gate scheme is useful for interpreting results from mutations that alter functional properties of neurotransmitter transporters.

摘要

大鼠和人类血清素转运体(分别为rSERT和hSERT)在非洲爪蟾卵母细胞中表达,并通过定点诱变、电生理记录和[3H]5-HT摄取测量进行研究。rSERT而非hSERT在低pH值下显示出与转运相关的电流增加。嵌合体和点突变表明,在52个不同的残基中,第490位的单个残基(rSERT中的苏氨酸和hSERT中的赖氨酸)决定了这种差异。此外,增强作用需要第493位的谷氨酸残基。半胱氨酸取代和烷基化实验表明,第493位残基位于细胞外。493位的半胱氨酸增加了每个转运的5-HT分子的净电荷移动,而天冬氨酸则使其减少。该区域的突变并未显著影响SERT功能的其他方面,包括非激动剂依赖性泄漏电流、电压依赖性瞬态电流和H+电流。因此,该区域可能是rSERT功能所需的外部门控的一部分。数据和分析表明,在缺乏详细结构信息的情况下,门控-内腔-门控方案有助于解释改变神经递质转运体功能特性的突变结果。

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