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Hydrophobin Film Structure for HFBI and HFBII and Mechanism for Accelerated Film Formation

机译:HFBI和HFBII的疏水蛋白膜结构及其加速成膜的机理

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Hydrophobins represent an important group of proteins from both a biological and nanotechnological standpoint. They are the means through which filamentous fungi affect their environment to promote growth, and their properties at interfaces have resulted in numerous applications. In our study we have combined protein docking, molecular dynamics simulation, and electron cryo-microscopy to gain atomistic level insight into the surface structure of films composed of two class II hydrophobins: HFBI and HFBII produced by Trichoderma reesei. Together our results suggest a unit cell composed of six proteins; however, our computational results suggest P6 symmetry, while our experimental results show P3 symmetry with a unit cell size of 56 ?. Our computational results indicate the possibility of an alternate ordering with a three protein unit cell with P3 symmetry and a smaller unit cell size, and we have used a Monte Carlo simulation of a spin model representing the hydrophobin film to show how this alternate metastable structure may play a role in increasing the rate of surface coverage by hydrophobin films, possibly indicating a mechanism of more general significance to both biology and nanotechnology.
机译:从生物学和纳米技术的观点来看,疏水蛋白代表重要的蛋白质组。它们是丝状真菌影响其环境以促进生长的手段,并且它们在界面处的特性已导致了许多应用。在我们的研究中,我们结合了蛋白质对接,分子动力学模拟和电子冷冻显微镜技术,以原子级的眼光洞察了由里氏木霉(Trichoderma reesei)生产的两种II类疏水蛋白:HFBI和HFBII组成的薄膜的表面结构。我们的研究结果共同表明一个由六种蛋白质组成的单位细胞。然而,我们的计算结果表明P6对称,而我们的实验结果表明P3对称具有56?的晶胞大小。我们的计算结果表明,具有三个具有P3对称性且单位细胞尺寸较小的蛋白质单位细胞的替代排序的可能性,并且我们已经使用了代表疏水蛋白膜的自旋模型的蒙特卡罗模拟来显示这种替代的亚稳态结构如何疏水蛋白膜在增加表面覆盖率方面起着重要作用,这可能表明该机制对生物学和纳米技术都具有更普遍的意义。

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