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首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Mechanism of selectivity in aquaporins and aquaglyceroporins
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Mechanism of selectivity in aquaporins and aquaglyceroporins

机译:水通道蛋白和水甘油通道蛋白的选择性机理

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Aquaporins and aquaglyceroporins form a family of pore proteins that facilitate the efficient and selective flux of small solutes across biological membranes. We studied the selectivity of aquaporin-1 (AQP1) and the bacterial glycerol facilitator, GIpF, for O_2, CO_2, NH_3, glycerol, urea, and water. Using molecular dynamics simulations, we calculated potentials of mean force for solute permeation along the aquaporin channels and compared them with the alternative pathway across the lipid bilayer. For small solutes permeating through AQP1, a remarkable anticorrelation between permeability and solute hydrophobicity was observed, whereas the opposite trend was observed for permeation through the membrane. This finding renders AQP1 a selective filter for small polar solutes, whereas GIpF was found to be highly permeable for small solutes and permeable for larger solutes. Surprisingly, not solute-channel but water-channel interactions were found to be the key determinant underlying the selectivity mechanism of aquaporins. Hence, a hydrophobic effect, together with steric restraints, determines the selectivity of aquaporins.
机译:水孔蛋白和水甘油孔蛋白形成一类孔蛋白,可促进小溶质在生物膜上的高效选择性流动。我们研究了水通道蛋白1(AQP1)和细菌甘油促进剂GIpF对O_2,CO_2,NH_3,甘油,尿素和水的选择性。使用分子动力学模拟,我们计算了沿水通道蛋白通道溶质渗透的平均力潜力,并将其与跨脂质双层的替代途径进行了比较。对于通过AQP1渗透的小溶质,在渗透率和溶质疏水性之间观察到显着的反相关性,而在膜中渗透的趋势相反。这一发现使AQP1成为小极性溶质的选择性过滤器,而GIpF被发现对小溶质具有高渗透性,对大溶质具有渗透性。出人意料的是,不是溶质通道而是水通道相互作用被发现是水通道蛋白选择性机制的关键决定因素。因此,疏水作用以及空间限制决定了水通道蛋白的选择性。

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