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赖氨酸300对于 NhaA钠/氢逆向转运蛋白的稳定性至关重要,但对于其电致转运并非必需。

Lysine 300 is essential for stability but not for electrogenic transport of the NhaA Na/H antiporter.

作者信息

Călinescu Octavian, Dwivedi Manish, Patiño-Ruiz Miyer, Padan Etana, Fendler Klaus

机构信息

From the Max-Planck Institute of Biophysics, 60438 Frankfurt am Main, Germany.

the "Carol Davila" University of Medicine and Pharmacy, 050474 Bucharest, Romania, and.

出版信息

J Biol Chem. 2017 May 12;292(19):7932-7941. doi: 10.1074/jbc.M117.778175. Epub 2017 Mar 22.

DOI:10.1074/jbc.M117.778175
PMID:28330875
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5427271/
Abstract

Na/H antiporters are located in the cytoplasmic and intracellular membranes and play crucial roles in regulating intracellular pH, Na, and volume. The NhaA antiporter of is the best studied member of the Na/H exchanger family and a model system for all related Na/H exchangers, including eukaryotic representatives. Several amino acid residues are important for the transport activity of NhaA, including Lys-300, a residue that has recently been proposed to carry one of the two H ions that NhaA exchanges for one Na ion during one transport cycle. Here, we sought to characterize the effects of mutating Lys-300 of NhaA to amino acid residues containing side chains of different polarity and length ( Ala, Arg, Cys, His, Glu, and Leu) on transporter stability and function. Salt resistance assays, acridine-orange fluorescence dequenching, solid supported membrane-based electrophysiology, and differential scanning fluorometry were used to characterize Na and H transport, charge translocation, and thermal stability of the different variants. These studies revealed that NhaA could still perform electrogenic Na/H exchange even in the absence of a protonatable residue at the Lys-300 position. However, all mutants displayed lower thermal stability and reduced ion transport activity compared with the wild-type enzyme, indicating the critical importance of Lys-300 for optimal NhaA structural stability and function. On the basis of these experimental data, we propose a tentative mechanism integrating the functional and structural role of Lys-300.

摘要

钠/氢反向转运蛋白位于细胞质膜和细胞内膜中,在调节细胞内pH值、钠离子浓度和细胞体积方面发挥着关键作用。嗜盐碱芽孢杆菌的NhaA反向转运蛋白是钠/氢交换蛋白家族中研究最深入的成员,也是所有相关钠/氢交换蛋白(包括真核生物代表)的模型系统。几个氨基酸残基对NhaA的转运活性很重要,包括赖氨酸-300,最近有人提出该残基在一次转运循环中携带NhaA用于交换一个钠离子的两个氢离子中的一个。在这里,我们试图研究将NhaA的赖氨酸-300突变为含有不同极性和长度侧链的氨基酸残基(丙氨酸、精氨酸、半胱氨酸、组氨酸、谷氨酸和亮氨酸)对转运蛋白稳定性和功能的影响。采用耐盐性测定、吖啶橙荧光猝灭、基于固体支持膜的电生理学和差示扫描荧光法来表征不同变体的钠和氢转运、电荷转运和热稳定性。这些研究表明,即使在赖氨酸-300位置没有可质子化残基的情况下,NhaA仍然可以进行电致钠/氢交换。然而,与野生型酶相比,所有突变体的热稳定性较低,离子转运活性降低,这表明赖氨酸-300对NhaA的最佳结构稳定性和功能至关重要。基于这些实验数据,我们提出了一种整合赖氨酸-300功能和结构作用的初步机制。

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