High-confidence placement of low-occupancy fragments into electron density using the anomalous signal of sulfur and halogen atoms.

IF 2.6 4区 生物学 Q2 BIOCHEMICAL RESEARCH METHODS
Shumeng Ma, Shymaa Damfo, Matthew W Bowler, Vitaliy Mykhaylyk, Frank Kozielski
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引用次数: 0

Abstract

Fragment-based drug design using X-ray crystallography is a powerful technique to enable the development of new lead compounds, or probe molecules, against biological targets. This study addresses the need to determine fragment binding orientations for low-occupancy fragments with incomplete electron density, an essential step before further development of the molecule. Halogen atoms play multiple roles in drug discovery due to their unique combination of electronegativity, steric effects and hydrophobic properties. Fragments incorporating halogen atoms serve as promising starting points in hit-to-lead development as they often establish halogen bonds with target proteins, potentially enhancing binding affinity and selectivity, as well as counteracting drug resistance. Here, the aim was to unambiguously identify the binding orientations of fragment hits for SARS-CoV-2 nonstructural protein 1 (nsp1) which contain a combination of sulfur and/or chlorine, bromine and iodine substituents. The binding orientations of carefully selected nsp1 analogue hits were focused on by employing their anomalous scattering combined with Pan-Dataset Density Analysis (PanDDA). Anomalous difference Fourier maps derived from the diffraction data collected at both standard and long-wavelength X-rays were compared. The discrepancies observed in the maps of iodine-containing fragments collected at different energies were attributed to site-specific radiation-damage stemming from the strong X-ray absorption of I atoms, which is likely to cause cleavage of the C-I bond. A reliable and effective data-collection strategy to unambiguously determine the binding orientations of low-occupancy fragments containing sulfur and/or halogen atoms while mitigating radiation damage is presented.

利用硫原子和卤素原子的异常信号,高置信度地将低占位碎片置于电子密度中。
利用 X 射线晶体学技术进行基于片段的药物设计是一项强大的技术,可以针对生物靶标开发新的先导化合物或探针分子。这项研究解决了确定电子密度不完全的低占位片段结合方向的需求,这是进一步开发分子前的重要步骤。卤素原子具有独特的电负性、立体效应和疏水特性,因此在药物研发中发挥着多重作用。含有卤素原子的片段在 "先导-命中 "研发过程中是很有希望的起点,因为它们通常会与靶蛋白建立卤素键,从而有可能增强结合亲和力和选择性,并抵消耐药性。本研究的目的是明确确定含有硫和/或氯、溴和碘取代基组合的 SARS-CoV-2 非结构蛋白 1(nsp1)片段的结合方向。通过采用异常散射和泛数据集密度分析(PanDDA)技术,重点研究了精心挑选的 nsp1 类似物的结合方向。比较了从标准 X 射线和长波长 X 射线收集的衍射数据中得出的异常差分傅立叶图。在不同能量下采集的含碘片段图谱中观察到的差异被归因于特定位点的辐射损伤,这种辐射损伤源于 I 原子对 X 射线的强烈吸收,很可能导致 C-I 键的裂解。本文介绍了一种可靠有效的数据收集策略,既能明确确定含硫和/或卤原子的低占位片段的结合方向,又能减轻辐射损伤。
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来源期刊
Acta Crystallographica. Section D, Structural Biology
Acta Crystallographica. Section D, Structural Biology BIOCHEMICAL RESEARCH METHODSBIOCHEMISTRY &-BIOCHEMISTRY & MOLECULAR BIOLOGY
CiteScore
4.50
自引率
13.60%
发文量
216
期刊介绍: Acta Crystallographica Section D welcomes the submission of articles covering any aspect of structural biology, with a particular emphasis on the structures of biological macromolecules or the methods used to determine them. Reports on new structures of biological importance may address the smallest macromolecules to the largest complex molecular machines. These structures may have been determined using any structural biology technique including crystallography, NMR, cryoEM and/or other techniques. The key criterion is that such articles must present significant new insights into biological, chemical or medical sciences. The inclusion of complementary data that support the conclusions drawn from the structural studies (such as binding studies, mass spectrometry, enzyme assays, or analysis of mutants or other modified forms of biological macromolecule) is encouraged. Methods articles may include new approaches to any aspect of biological structure determination or structure analysis but will only be accepted where they focus on new methods that are demonstrated to be of general applicability and importance to structural biology. Articles describing particularly difficult problems in structural biology are also welcomed, if the analysis would provide useful insights to others facing similar problems.
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