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A novel molecular dynamics study of CO2 permeation through aquaporin-5

机译:Aquaporin-5的二氧化碳渗透的新型分子动力学研究

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Aquaporins (AQPs) are protein channels which facilitate rapid water permeation across cell membrane. The AQPs are very vital for biological organs, as their malfunction causes severe diseases in human body. A particular family of AQPs, that is AQP5, has a significant role in lung fluid transport due to submucosal glands structure. However, it has not been yet well understood whether these protein channels can conduct gas molecules. Here, Molecular Dynamics (MD) simulations are used to investigate the CO2 permeability and diffusion in AQP5 during a 40-nanosecond period. For the first time, equilibrium and Steered MD (SMD) are used to simulate self and force-induced diffusion of CO2 molecules across AQP5 and POPE lipid bilayer. According to PMFs profile associated to CO2 permeation, the hydrophobic central pore provides a more suitable pathway for gas molecules compared to other AQP5 channels. Although CO2 molecules can also permeate across AQP5 water channels, the rate of CO2 permeation through four channels of the AQP5 monomers is much lower than the central pore. The rate of CO2 permeation through four AQP5 water channels is even lower than CO2 diffusion through POPE lipid membrane. The results reported in this investigation demonstrate that MD simulations of human AQP5 provide valuable insights into the gas permeation mechanism for both the equilibrium self-diffusion, and quasi-equilibrium condition.
机译:Aquaporins(AQP)是蛋白质通道,其促进穿越细胞膜的快速渗透。 AQP对生物器官非常重要,因为它们的故障导致人体的严重疾病。一个特定的AQP系列,即AQP5,由于粘膜腺结构,在肺部流体运输中具有重要作用。然而,尚未清楚这些蛋白质通道是否可以进行气体分子。这里,在40纳秒期间,使用分子动力学(MD)模拟来研究AQP5中的CO 2渗透率和扩散。首次,平衡和转向MD(SMD)用于模拟AQP5和POPE脂质双层在AQP5和POPE脂质双层之间的自我和力诱导的CO 2分子扩散。根据与CO2渗透相关的PMFS谱,与其他AQP5通道相比,疏水性中央孔提供了更合适的气体分子途径。尽管CO 2分子也可以穿过AQP5水通道渗透,但是通过四个通道的AQP5单体渗透的速率远低于中央孔。通过四个AQP5水通道的CO2渗透速率甚至低于通过教材脂膜的二氧化碳扩散。本研究报告的结果表明,人类AQP5的MD模拟为均衡自扩散和准平衡条件的气体渗透机制提供了有价值的见解。

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