Appraising protein conformational changes by resampling time-resolved serial x-ray crystallography data.

IF 2.3 2区 物理与天体物理 Q3 CHEMISTRY, PHYSICAL Structural Dynamics-Us Pub Date : 2024-07-24 eCollection Date: 2024-07-01 DOI:10.1063/4.0000258
Adams Vallejos, Gergely Katona, Richard Neutze
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Abstract

With the development of serial crystallography at both x-ray free electron laser and synchrotron radiation sources, time-resolved x-ray crystallography is increasingly being applied to study conformational changes in macromolecules. A successful time-resolved serial crystallography study requires the growth of microcrystals, a mechanism for synchronized and homogeneous excitation of the reaction of interest within microcrystals, and tools for structural interpretation. Here, we utilize time-resolved serial femtosecond crystallography data collected from microcrystals of bacteriorhodopsin to compare results from partial occupancy structural refinement and refinement against extrapolated data. We illustrate the domain wherein the amplitude of refined conformational changes is inversely proportional to the activated state occupancy. We illustrate how resampling strategies allow coordinate uncertainty to be estimated and demonstrate that these two approaches to structural refinement agree within coordinate errors. We illustrate how singular value decomposition of a set of difference Fourier electron density maps calculated from resampled data can minimize phase bias in these maps, and we quantify residual densities for transient water molecules by analyzing difference Fourier and Polder omit maps from resampled data. We suggest that these tools may assist others in judging the confidence with which observed electron density differences may be interpreted as functionally important conformational changes.

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通过重采样时间分辨序列 X 射线晶体学数据评估蛋白质构象变化
随着 X 射线自由电子激光和同步辐射源系列晶体学的发展,时间分辨 X 射线晶体学正越来越多地应用于研究大分子的构象变化。成功的时间分辨序列晶体学研究需要微晶体的生长、微晶体内相关反应的同步和均匀激发机制以及结构解释工具。在这里,我们利用从细菌眼色素微晶体中收集到的时间分辨串行飞秒晶体学数据,比较了部分占位结构细化和根据外推数据细化的结果。我们说明了细化构象变化的幅度与激活状态占位成反比的领域。我们说明了重采样策略如何允许估计坐标不确定性,并证明这两种结构细化方法在坐标误差范围内是一致的。我们说明了通过重采样数据计算出的一组差分傅立叶电子密度图的奇异值分解如何最大限度地减少这些图中的相位偏差,我们还通过分析重采样数据中的差分傅立叶图和波德省略图量化了瞬态水分子的残余密度。我们认为这些工具可以帮助他人判断观察到的电子密度差异是否可以解释为具有重要功能的构象变化。
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来源期刊
Structural Dynamics-Us
Structural Dynamics-Us CHEMISTRY, PHYSICALPHYSICS, ATOMIC, MOLECU-PHYSICS, ATOMIC, MOLECULAR & CHEMICAL
CiteScore
5.50
自引率
3.60%
发文量
24
审稿时长
16 weeks
期刊介绍: Structural Dynamics focuses on the recent developments in experimental and theoretical methods and techniques that allow a visualization of the electronic and geometric structural changes in real time of chemical, biological, and condensed-matter systems. The community of scientists and engineers working on structural dynamics in such diverse systems often use similar instrumentation and methods. The journal welcomes articles dealing with fundamental problems of electronic and structural dynamics that are tackled by new methods, such as: Time-resolved X-ray and electron diffraction and scattering, Coherent diffractive imaging, Time-resolved X-ray spectroscopies (absorption, emission, resonant inelastic scattering, etc.), Time-resolved electron energy loss spectroscopy (EELS) and electron microscopy, Time-resolved photoelectron spectroscopies (UPS, XPS, ARPES, etc.), Multidimensional spectroscopies in the infrared, the visible and the ultraviolet, Nonlinear spectroscopies in the VUV, the soft and the hard X-ray domains, Theory and computational methods and algorithms for the analysis and description of structuraldynamics and their associated experimental signals. These new methods are enabled by new instrumentation, such as: X-ray free electron lasers, which provide flux, coherence, and time resolution, New sources of ultrashort electron pulses, New sources of ultrashort vacuum ultraviolet (VUV) to hard X-ray pulses, such as high-harmonic generation (HHG) sources or plasma-based sources, New sources of ultrashort infrared and terahertz (THz) radiation, New detectors for X-rays and electrons, New sample handling and delivery schemes, New computational capabilities.
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