Combining NMR relaxation with chemical shift perturbation data to drive protein-protein docking

van Dijk ADJ; Kaptein R; Boelens R; Bonvin AMJJ

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Combining NMR relaxation with chemical shift perturbation data to drive protein-protein docking

机译：将NMR弛豫与化学位移扰动数据结合起来以驱动蛋白质-蛋白质对接

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The modeling of biomolecular complexes by computational docking using the known structures of their constituents is developing rapidly to become a powerful tool in structural biology. It is especially useful in combination with even limited experimental information describing the interface. Here we demonstrate for the first time the use of diffusion anisotropy in combination with chemical shift perturbation data to drive protein-protein docking. For validation purposes we make use of simulated diffusion anisotropy data. Inclusion of this information, which can be derived from NMR relaxation rates and reports on the orientation of the components of a complex with respect to the rotational diffusion tensor, substantially improves the docking results.

机译：通过分子对接的已知结构利用计算对接对生物分子复合物进行建模正在迅速发展，已成为结构生物学的强大工具。与描述接口的有限实验信息结合使用时，它特别有用。在这里，我们首次证明了将扩散各向异性与化学位移扰动数据结合使用来驱动蛋白质-蛋白质对接。为了进行验证，我们使用了模拟的扩散各向异性数据。包含此信息（可以从NMR弛豫率得出并报告复合物的各组分相对于旋转扩散张量的取向）可大大改善对接结果。

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来源
《Journal of Biomolecular NMR》 |2006年第4期|共8页
作者
van Dijk ADJ; Kaptein R; Boelens R; Bonvin AMJJ;
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正文语种 eng
中图分类分子生物学;
关键词
computational docking; NMR relaxation; protein complex; structure calculation; RESIDUAL DIPOLAR COUPLINGS; PHOSPHOTRANSFERASE SYSTEM; HYDRODYNAMIC CALCULATIONS; ROTATIONAL DIFFUSION; DOMAIN ORIENTATION; DYNAMICS; HPR; DEPENDENCE; ANISOTROPY; COMPLEXES;

机译：计算对接;核磁共振弛豫;蛋白质复合物;结构计算;残双链偶联;磷酸转移酶体系;水力计算;旋转扩散;域取向;动力学;HPR;依赖性;各向异性;复杂性;

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专利

1. Combining NMR relaxation with chemical shift perturbation data to drive protein-protein docking [J] . van Dijk ADJ, Kaptein R, Boelens R, Journal of Biomolecular NMR . 2006,第4期

机译：将NMR弛豫与化学位移扰动数据结合起来以驱动蛋白质-蛋白质对接
2. An NMR study of the origin of dioxygen-induced spin-lattice relaxation enhancement and chemical shift perturbation [J] . Prosser RS, Luchette PA Journal of magnetic resonance . 2004,第2期

机译：NMR研究双氧引起的自旋晶格弛豫增强和化学位移扰动的起源
3. Combining Free Energy Simulations and NMR Chemical-Shift Perturbation To Identify Transient Cation-pi Contacts in Proteins [J] . Reis Andre A. O., Sayegh Raphael S. R., Marana Sandro R., Journal of chemical information and modeling . 2020,第2期

机译：结合自由能量模拟和NMR化学频移扰动，以鉴定蛋白质中的瞬时阳离子PI触点
4. GWIDD: A genome-wide protein-protein docking database [C] . Zhengwei Zhu, Tovchigrechko, A., Bioengineering Conference, 2007 IEEE 33rd Annual Northeast . 2007

机译：GWIDD：全基因组的蛋白质-蛋白质对接数据库
5. Protein Dynamics, Loop Motions and Protein-Protein Interactions Combining Nuclear Magnetic Resonance (NMR) Spectroscopy with Molecular Dynamics (MD) Simulations. [D] . Gu, Yina. 2016

机译：结合核磁共振（NMR）光谱和分子动力学（MD）模拟的蛋白质动力学，循环运动和蛋白质相互作用。
6. Atomic Structures of Excited State A-T Hoogsteen Base Pairs in Duplex DNA by Combining NMR Relaxation Dispersion Mutagenesis and Chemical Shift Calculations [O] . Honglue Shi, Mary C. Clay, Atul Rangadurai, -1

机译：核磁共振弛豫诱变和化学位移计算相结合的双链DNA中激发态A-T Hoogsteen碱基对的原子结构。
7. Combining NMR relaxation with chemical shift perturbation data to drive protein–protein docking [O] . van Dijk, A.D.J., Kaptein, R., Boelens, R., 2006

机译：将NmR弛豫与化学位移扰动数据相结合，以驱动蛋白质 - 蛋白质对接

Combining NMR relaxation with chemical shift perturbation data to drive protein-protein docking

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