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用于溶液小角散射的柔性膜结合生物分子复合物建模。

Modeling of flexible membrane-bound biomolecular complexes for solution small-angle scattering.

机构信息

Condensed Matter Physics, Niels Bohr Institute, University of Copenhagen, Universitetsparken 5, Copenhagen 2100, Denmark.

Structural Biology and NMR Laboratory, Department of Biology, University of Copenhagen, Ole Maaløes Vej 5, Copenhagen 2200, Denmark.

出版信息

J Colloid Interface Sci. 2023 Apr;635:611-621. doi: 10.1016/j.jcis.2022.12.024. Epub 2022 Dec 10.

DOI:10.1016/j.jcis.2022.12.024
PMID:36634513
Abstract

Recent advances in protein expression protocols, sample handling, and experimental set up of small-angle scattering experiments have allowed users of the technique to structurally investigate biomolecules of growing complexity and structural disorder. Notable examples include intrinsically disordered proteins, multi-domain proteins and membrane proteins in suitable carrier systems. Here, we outline a modeling scheme for calculating the scattering profiles from such complex samples. This kind of modeling is necessary for structural information to be refined from the corresponding data. The scheme bases itself on a hybrid of classical form factor based modeling and the well-known spherical harmonics-based formulation of small-angle scattering amplitudes. Our framework can account for flexible domains alongside other structurally elaborate components of the molecular system in question. We demonstrate the utility of this modeling scheme through a recent example of a structural model of the growth hormone receptor membrane protein in a phospholipid bilayer nanodisc which is refined against experimental SAXS data. Additionally we investigate how the scattering profiles from the complex would appear under different scattering contrasts. For each contrast situation we discuss what structural information is contained and the related consequences for modeling of the data.

摘要

近年来,蛋白质表达方案、样品处理和小角散射实验的实验设置方面的进展,使得该技术的使用者能够对越来越复杂和结构无序的生物分子进行结构研究。值得注意的例子包括固有无序的蛋白质、多结构域蛋白质和在合适的载体系统中的膜蛋白。在这里,我们概述了一种从这类复杂样品计算散射图谱的建模方案。对于从相应数据中提取结构信息来说,这种建模是必要的。该方案基于基于经典形态因子的建模和众所周知的基于球谐函数的小角散射幅度公式的混合。我们的框架可以考虑灵活的结构域以及所研究分子系统的其他精细结构组件。我们通过最近的一个例子证明了该建模方案的实用性,即生长激素受体膜蛋白在磷脂双层纳米盘中的结构模型,该模型是针对实验 SAXS 数据进行精修的。此外,我们还研究了在不同散射对比度下,复杂散射图谱的外观。对于每种对比情况,我们都讨论了包含的结构信息以及对数据建模的相关影响。

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