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QUAFIT:一种从小角度散射数据确定四级结构的新方法。

QUAFIT: a novel method for the quaternary structure determination from small-angle scattering data.

机构信息

Dipartimento di Scienze della Vita e dell'Ambiente, Università Politecnica delle Marche and Consorzio Nazionale Interuniversitario per le Scienze Fisiche della Materia, Ancona, Italy.

Dipartimento di Biologia, Università di Padova, Padova, Italy.

出版信息

Biophys J. 2012 Aug 8;103(3):511-521. doi: 10.1016/j.bpj.2012.06.037.

Abstract

The new QUAFIT method for determining the quaternary structure of biological macromolecular assemblies by analyzing x-ray or neutron small-angle scattering data is presented. The method is based on the idea that asymmetric monomers, formed by rigid domains of known atomic structure possibly connected by flexible linkers of known sequence, are assembled according to a point-group symmetry combined with a screw axis. Scattering amplitudes of domains and linkers are determined by means of a spherical harmonics expansion and combined to get the form factor of the assembly. To avoid any overlap among domains, the contact distance between two asymmetric domains is determined as a function of their orientation by a new algorithm, based on Stone's Invariants expansion. To account for continuity and compactness of the whole assembly, an anisotropic Lennard-Jones potential among domains, written in terms of the contact distances, is included in the merit function. QUAFIT allows for the simultaneous presence of oligomerization intermediates as well as of monomers distributed over multiple conformations. QUAFIT has been tested by studying the structure of a high molecular weight protein, the hemocyanin from Octopus vulgaris, under solution conditions that stabilize the decameric form or induce dissociation into monomers, respectively. Results are in very good agreement with the structural model derived from electron microscopy observations.

摘要

本文介绍了一种新的 QUAFIT 方法,用于通过分析 X 射线或中子小角散射数据来确定生物大分子组装体的四级结构。该方法基于这样的想法,即由具有已知原子结构的刚性结构域(可能通过已知序列的柔性接头连接)组成的不对称单体,根据点群对称性与螺旋轴组合进行组装。通过球谐展开确定结构域和接头的散射振幅,并将它们组合以得到组装体的形状因子。为了避免结构域之间的任何重叠,通过一种新算法,基于 Stone 的不变量展开,确定两个不对称结构域之间的接触距离作为它们取向的函数。为了考虑整个组装体的连续性和紧凑性,在优势函数中包含了以接触距离表示的结构域之间的各向异性 Lennard-Jones 势。QUAFIT 允许同时存在寡聚化中间体以及分布在多个构象上的单体。通过研究在分别稳定十聚体形式或诱导单体解离的溶液条件下的 Octopus vulgaris 血蓝蛋白的结构,对 QUAFIT 进行了测试。结果与电子显微镜观察得出的结构模型非常吻合。

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