用分子置换法测定分辨率降低的X射线和电子衍射数据中的小分子晶体结构。

IF 1.9 4区 材料科学 Q3 CHEMISTRY, MULTIDISCIPLINARY
Tatiana E Gorelik, Peer Lukat, Christian Kleeberg, Wulf Blankenfeldt, Rolf Mueller
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引用次数: 0

摘要

小分子晶体的3D电子衍射(ED)数据的分辨率通常相对较差,这是由于数据收集过程中的电子束辐射损伤或材料的结晶度较差。当数据分辨率低于1.2的公认极限时,用作晶体结构测定标准的直接方法不适用 Å。因此,对分子置换(MR)程序的性能进行了评估,该程序通常用于蛋白质结构测定,用于从3D ED数据中分析小分子晶体结构。在本研究过程中,确定了致癌转录因子BCL6的高效抑制剂Bi-3812的两种晶体结构:α-Bi-38112的结构由单晶X射线数据确定,β-Bi-3812的结构由3D ED数据确定,在这两种情况下均使用直接方法。这些数据随后用于具有不同数据类型的MR,改变数据分辨率限制(1、1.5和2 Å),并通过使用由BI-3812的连接或断开的片段组成的搜索模型。MR在2时成功获得3D ED数据 Å分辨率,使用代表74%完整分子的搜索模型。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Molecular replacement for small-molecule crystal structure determination from X-ray and electron diffraction data with reduced resolution.

Molecular replacement for small-molecule crystal structure determination from X-ray and electron diffraction data with reduced resolution.

Molecular replacement for small-molecule crystal structure determination from X-ray and electron diffraction data with reduced resolution.

Molecular replacement for small-molecule crystal structure determination from X-ray and electron diffraction data with reduced resolution.

The resolution of 3D electron diffraction (ED) data of small-molecule crystals is often relatively poor, due to either electron-beam radiation damage during data collection or poor crystallinity of the material. Direct methods, used as standard for crystal structure determination, are not applicable when the data resolution falls below the commonly accepted limit of 1.2 Å. Therefore an evaluation was carried out of the performance of molecular replacement (MR) procedures, regularly used for protein structure determination, for structure analysis of small-molecule crystal structures from 3D ED data. In the course of this study, two crystal structures of Bi-3812, a highly potent inhibitor of the oncogenic transcription factor BCL6, were determined: the structure of α-Bi-3812 was determined from single-crystal X-ray data, the structure of β-Bi-3812 from 3D ED data, using direct methods in both cases. These data were subsequently used for MR with different data types, varying the data resolution limit (1, 1.5 and 2 Å) and by using search models consisting of connected or disconnected fragments of BI-3812. MR was successful with 3D ED data at 2 Å resolution using a search model that represented 74% of the complete molecule.

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来源期刊
Acta Crystallographica Section A: Foundations and Advances
Acta Crystallographica Section A: Foundations and Advances CHEMISTRY, MULTIDISCIPLINARYCRYSTALLOGRAPH-CRYSTALLOGRAPHY
CiteScore
2.60
自引率
11.10%
发文量
419
期刊介绍: Acta Crystallographica Section A: Foundations and Advances publishes articles reporting advances in the theory and practice of all areas of crystallography in the broadest sense. As well as traditional crystallography, this includes nanocrystals, metacrystals, amorphous materials, quasicrystals, synchrotron and XFEL studies, coherent scattering, diffraction imaging, time-resolved studies and the structure of strain and defects in materials. The journal has two parts, a rapid-publication Advances section and the traditional Foundations section. Articles for the Advances section are of particularly high value and impact. They receive expedited treatment and may be highlighted by an accompanying scientific commentary article and a press release. Further details are given in the November 2013 Editorial. The central themes of the journal are, on the one hand, experimental and theoretical studies of the properties and arrangements of atoms, ions and molecules in condensed matter, periodic, quasiperiodic or amorphous, ideal or real, and, on the other, the theoretical and experimental aspects of the various methods to determine these properties and arrangements.
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