Synergism between x-ray crystallography and NMR residual dipolar couplings in characterizing protein dynamics.

IF 2.3 2区物理与天体物理 Q3 CHEMISTRY, PHYSICAL Structural Dynamics-Us Pub Date : 2023-07-01 DOI:10.1063/4.0000192

Yang Shen, Ad Bax

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Abstract

The important role of structural dynamics in protein function is widely recognized. Thermal or B-factors and their anisotropy, seen in x-ray analysis of protein structures, report on the presence of atomic coordinate heterogeneity that can be attributed to motion. However, their quantitative evaluation in terms of protein dynamics by x-ray ensemble refinement remains challenging. NMR spectroscopy provides quantitative information on the amplitudes and time scales of motional processes. Unfortunately, with a few exceptions, the NMR data do not provide direct insights into the atomic details of dynamic trajectories. Residual dipolar couplings, measured by solution NMR, are very precise parameters reporting on the time-averaged bond-vector orientations and may offer the opportunity to derive correctly weighted dynamic ensembles of structures for cases where multiple high-resolution x-ray structures are available. Applications to the SARS-CoV-2 main protease, M^pro, and ubiquitin highlight this complementarity of NMR and crystallography for quantitative assessment of internal motions.

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x射线晶体学和核磁共振残余偶极偶联在蛋白质动力学表征中的协同作用。

结构动力学在蛋白质功能中的重要作用已被广泛认识。热因子或b因子及其各向异性，在蛋白质结构的x射线分析中可见，报告了可归因于运动的原子坐标异质性的存在。然而，它们在蛋白质动力学方面的定量评价通过x射线系综细化仍然具有挑战性。核磁共振光谱学提供了关于运动过程的振幅和时间尺度的定量信息。不幸的是，除了少数例外，核磁共振数据不能直接洞察动态轨迹的原子细节。通过溶液核磁共振测量的残余偶极耦合是报告时间平均键向量方向的非常精确的参数，可以为获得多个高分辨率x射线结构的情况提供正确加权的动态结构集合的机会。对SARS-CoV-2主要蛋白酶、Mpro和泛素的应用突出了核磁共振和晶体学在定量评估内部运动方面的互补性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Structural Dynamics-Us CHEMISTRY, PHYSICALPHYSICS, ATOMIC, MOLECU-PHYSICS, ATOMIC, MOLECULAR & CHEMICAL

CiteScore

5.50

自引率

3.60%

发文量

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.