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Atomistic structure of monomolecular surface layer self-assemblies: Toward functionalized nanostructures

机译:单分子表面层自组装的原子结构:走向功能化的纳米结构。

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The concept of self-assembly is one of the most promising strategies for the creation of defined nanostructures and therefore became an essential part of nanotechnology for the controlled bottom-up design of nanoscale structures. Surface layers (S-layers), which represent the cell envelope of a great variety of prokaryotic cells, show outstanding self-assembly features in vitro and have been successfully used as the basic matrix for molecular construction kits. Here we present the three-dimensional structure of an S-layer lattice based on tetrameric unit cells, which will help to facilitate the directed binding of various molecules on the S-layer lattice, thereby creating functional nanoarrays for applications in nanobiotechnology. Our work demonstrates the successful combination of computer simulations, electron microscopy (TEM), and small-angle X-ray scattering (SAXS) as a tool for the investigation of the structure of self-assembling or aggregating proteins, which cannot be determined by X-ray crystallography. To the best of our knowledge, this is the first structural model at an amino acid level of an S-layer unit cell that exhibits p4 lattice symmetry.
机译:自组装的概念是创建定义的纳米结构的最有前途的策略之一,因此成为控制纳米级结构自下而上设计的纳米技术的重要组成部分。表面层(S层)代表了各种原核细胞的细胞膜,在体外显示出出色的自组装特征,并已成功用作分子构建试剂盒的基本基质。在这里,我们介绍基于四聚体晶胞的S层晶格的三维结构,这将有助于促进S层晶格上各种分子的定向结合,从而创建可用于纳米生物技术的功能纳米阵列。我们的工作证明了计算机模拟,电子显微镜(TEM)和小角度X射线散射(SAXS)的成功结合,可作为研究无法自行确定或聚集的蛋白质结构的工具射线晶体学。据我们所知,这是第一个显示p4晶格对称性的S层单位细胞氨基酸水平的结构模型。

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