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Microsecond simulation of human aquaporin 2 reveals structural determinants of water permeability and selectivity

机译:人类水上素2的微秒模拟显示水渗透性和选择性的结构决定因素

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摘要

Human aquaporin 2 (AQP2) from the family of aquaporins assumes great physiological importance, owing to its association with nephrogenic diabetes insipidus (NDI). The present study provides detailed insights into the transport properties of AQP2 with the use of microsecond-scale molecular dynamics simulations, and explains how these channels conduct water molecules while at the same time excluding other molecules. Water transport is seen to be diffusion-limited, with a barrier of only 1.6 kcal mol(-1), and the channel is more water-permeable than other known aquaporins. A constriction site with a pore-facing phenylalanine and arginine is proposed to serve as a selectivity filter as well as a gate modulating the conductance state of the channel. Water molecules form a continuous single-file in the pore lumen, and the orientation of water molecules in this chain is governed by water-protein interactions. A mutant is designed that exhibits different orientation of water molecules, leading to altered permeability. The study complements experimental studies by revealing details of the transport mechanism, energetics, and kinetics. Furthermore, insights obtained into the regulation of permeability in the channel offer the promise of devising new strategies for altering the permeability of the channel under diseased conditions. (C) 2016 Elsevier B.V. All rights reserved.
机译:由于其与肾病糖尿病患者(NDI)的关联,来自Aquaporins系列的人类水疗法2(AQP2)具有很大的生理重要性。本研究提供了通过使用微秒级分子动力学模拟的AQP2的传输特性的详细见解,并解释了这些通道如何在不包括其他分子的同时进行水分子。看到水运被视为扩散限制,仅具有1.6千卡摩尔(-1)的屏障,并且该通道比其他已知的水蛋白蛋白更加透水。提出具有面向孔和精氨酸的收缩部位和精氨酸用作选择性滤波器以及调制通道的电导状态的栅极。水分子在孔腔中形成连续单一文件,该链中水分子的取向受水蛋白质相互作用的控制。设计突变体,其表现出水分子的不同取向,导致渗透性改变。该研究通过揭示运输机制,能量和动力学的细节来补充实验研究。此外,在渠道中渗透性调节中获得的见解提供了制定改变疾病条件下渠道渗透性的新策略的承诺。 (c)2016年Elsevier B.v.保留所有权利。

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