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Neutron Crystallography for the Study of Hydrogen Bonds in Macromolecules

机译:中子晶体学研究大分子中的氢键

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摘要

The hydrogen bond (H bond) is one of the most important interactions that form the foundation of secondary and tertiary protein structure. Beyond holding protein structures together, H bonds are also intimately involved in solvent coordination, ligand binding, and enzyme catalysis. The H bond by definition involves the light atom, H, and it is very difficult to study directly, especially with X-ray crystallographic techniques, due to the poor scattering power of H atoms. Neutron protein crystallography provides a powerful, complementary tool that can give unambiguous information to structural biologists on solvent organization and coordination, the electrostatics of ligand binding, the protonation states of amino acid side chains and catalytic water species. The method is complementary to X-ray crystallography and the dynamic data obtainable with NMR spectroscopy. Also, as it gives explicit H atom positions, it can be very valuable to computational chemistry where exact knowledge of protonation and solvent orientation can make a large difference in modeling. This article gives general information about neutron crystallography and shows specific examples of how the method has contributed to structural biology, structure-based drug design; and the understanding of fundamental questions of reaction mechanisms.
机译:氢键(H键)是形成二级和三级蛋白质结构基础的最重要的相互作用之一。除了将蛋白质结构保持在一起之外,H键还与溶剂配位,配体结合和酶催化密切相关。根据定义,氢键涉及轻原子H,由于H原子的散射能力差,因此很难直接研究,尤其是使用X射线晶体学技术。中子蛋白质晶体学提供了功能强大的互补工具,可以为结构生物学家提供有关溶剂组织和配位,配体结合的静电,氨基酸侧链的质子化状态和催化水物种的明确信息。该方法是X射线晶体学和NMR光谱学可获得的动态数据的补充。另外,由于它给出了明确的H原子位置,因此对于计算化学非常有价值,因为在该化学中,对质子化和溶剂取向的确切了解会对建模产生很大的影响。本文提供了有关中子晶体学的一般信息,并显示了该方法如何有助于结构生物学,基于结构的药物设计的具体实例;以及对反应机制基本问题的理解。

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