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人源钠/肌醇转运蛋白 2(SMIT2/SGLT6)的转运机制,该蛋白属于 LeuT 结构家族成员。

The transport mechanism of the human sodium/myo-inositol transporter 2 (SMIT2/SGLT6), a member of the LeuT structural family.

机构信息

Groupe d'étude des protéines membranaires (GÉPROM) and Département de Physique, Université de Montréal, Montreal, Quebec, Canada.

Groupe d'étude des protéines membranaires (GÉPROM) and Département de Physique, Université de Montréal, Montreal, Quebec, Canada

出版信息

Am J Physiol Cell Physiol. 2014 Sep 1;307(5):C431-41. doi: 10.1152/ajpcell.00054.2014. Epub 2014 Jun 18.

Abstract

The sodium/myo-inositol transporter 2 (SMIT2) is a member of the SLC5A gene family, which is believed to share the five-transmembrane segment inverted repeat of the LeuT structural family. The two-electrode voltage-clamp (TEVC) technique was used to measure the steady-state and the pre-steady-state currents mediated by human SMIT2 after expression in Xenopus laevis oocytes. Phlorizin is first shown to be a poor inhibitor of pre-steady-state currents for depolarizing voltage pulse. From an up to threefold difference between the apparent ON and OFF transferred charges during a voltage pulse, we also show that a fraction of the transient current recorded for very negative potentials is not a true pre-steady-state current coming from the cotransporter conformational changes. We suggest that this transient current comes from a time-dependent leak current that can reach large amplitudes when external Na(+) concentration is reduced. A kinetic model was generated through a simulated annealing algorithm. This algorithm was used to identify the optimal connectivity among 19 different kinetic models and obtain the numerical values of the associated parameters. The proposed 5-state model includes cooperative binding of Na(+) ions, strong apparent asymmetry of the energy barriers, a rate-limiting step that is likely associated with the translocation of the empty transporter, and a turnover rate of 21 s(-1). The proposed model is a proof of concept for a novel approach to kinetic modeling of electrogenic transporters and allows insight into the transport mechanism of members of the LeuT structural family at the millisecond timescale.

摘要

钠/肌醇转运蛋白 2(SMIT2)是 SLC5A 基因家族的成员,据信该家族共享 LeuT 结构家族的五个跨膜片段反向重复。双电极电压钳(TEVC)技术用于测量人 SMIT2 在非洲爪蟾卵母细胞表达后的稳态和预稳态电流。首先表明根皮苷是去极化电压脉冲的预稳态电流的不良抑制剂。从电压脉冲期间表观 ON 和 OFF 转移电荷之间高达三倍的差异,我们还表明,记录的非常负电位的瞬态电流的一部分不是来自协同转运体构象变化的真正预稳态电流。我们建议,这种瞬态电流来自时变漏电流,当外部 Na(+)浓度降低时,该漏电流可以达到很大的幅度。通过模拟退火算法生成了一个动力学模型。该算法用于识别 19 个不同动力学模型之间的最佳连接,并获得相关参数的数值。所提出的 5 状态模型包括 Na(+)离子的协同结合,能量势垒的明显强不对称性,可能与空载体易位相关的限速步骤,以及 21 s(-1)的周转率。所提出的模型是一种新颖的电致转运体动力学建模方法的概念证明,并允许在毫秒时间尺度上深入了解 LeuT 结构家族成员的运输机制。

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