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开放和关闭状态之间的人口转移改变了 Aquaporin Z 突变体的水通透性。

Population shift between the open and closed states changes the water permeability of an Aquaporin Z mutant.

机构信息

School of Civil and Environmental Engineering, Nanyang Technological University, Singapore.

出版信息

Biophys J. 2012 Jul 18;103(2):212-8. doi: 10.1016/j.bpj.2012.05.049. Epub 2012 Jul 17.

Abstract

Aquaporins are tetrameric transmembrane channels permeable to water and other small solutes. Wild-type (WT) and mutant Aquaporin Z (AqpZ) have been widely studied and multiple factors have been found to affect their water permeability. In this study, molecular dynamics simulations have been performed for the tetrameric AqpZ F43W/H174G/T183F mutant. It displayed ∼10% average water permeability compared to WT AqpZ, which had been attributed to the increased channel lumen hydrophobicity. Our simulations, however, show a ring stacking between W43 and F183 acting as a secondary steric gate in the triple mutant with R189 as the primary steric gate in both mutant and WT AqpZ. The double gates (R189 and W43-F183) result in a high population of the closed conformation in the mutant. Occasionally an open state, with diffusive water permeability very close to that of WT AqpZ, was observed. Taken together, our results show that the double-gate mechanism is sufficient to explain the reduced water permeability in the mutant without invoking effects arising from increased hydrophobicity of the channel lumen. Our findings provide insights into how aquaporin-mediated water transport can be modulated and may further point to how aquaporin function can be optimized for biomimetic membrane applications.

摘要

水通道蛋白是四聚体跨膜通道,可通透水和其他小溶质。野生型 (WT) 和突变型水通道蛋白 Z (AqpZ) 已被广泛研究,发现多种因素会影响其水通透性。在这项研究中,对四聚体 AqpZ F43W/H174G/T183F 突变体进行了分子动力学模拟。与 WT AqpZ 相比,其平均水通透性约为 10%,这归因于通道内腔疏水性增加。然而,我们的模拟显示,W43 和 F183 之间存在环堆叠,在三重突变体中充当次要的位阻门,而 R189 在突变体和 WT AqpZ 中充当主要的位阻门。双门(R189 和 W43-F183)导致突变体中封闭构象的高比例。偶尔会观察到开放状态,其扩散水通透性非常接近 WT AqpZ。总之,我们的结果表明,双门机制足以解释突变体中水通透性降低,而无需引入通道内腔疏水性增加所产生的影响。我们的发现提供了关于水通道蛋白介导的水运输如何被调节的见解,并可能进一步指出如何优化水通道蛋白的功能以用于仿生膜应用。

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