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Structure determination of membrane proteins in five easy pieces

机译:五个简单片段中膜蛋白的结构测定

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Rotational Alignment (RA) solid-state NMR provides the basis for a general method for determining the structures of membrane proteins in phospholipid bilayers under physiological conditions. Membrane proteins are high priority targets for structure determination, and are challenging for existing experimental methods. Because membrane proteins reside in liquid crystalline phospholipid bilayer membranes it is important to study them in this type of environment. The RA solid-state NMR approach we have developed can be summarized in five steps, and incorporates methods of molecular biology, biochemistry, sample preparation, the implementation of NMR experiments, and structure calculations. It relies on solid-state NMR spectroscopy to obtain high-resolution spectra and residue-specific structural restraints for membrane proteins that undergo rotational diffusion around the membrane normal, but whose mobility is otherwise restricted by interactions with the membrane phospholipids. High resolution spectra of membrane proteins alone and in complex with other proteins and ligands set the stage for structure determination and functional studies of these proteins in their native, functional environment.
机译:旋转比对(RA)固态NMR为确定在生理条件下磷脂双层中的膜蛋白结构的一般方法提供了基础。膜蛋白是结构确定的高度优先目标,并且对现有的实验方法具有挑战性。因为膜蛋白驻留在液晶磷脂双层膜中,所以在这种类型的环境中研究它们很重要。我们开发的RA固态NMR方法可以分为五个步骤,其中包括分子生物学,生物化学,样品制备,NMR实验的实施和结构计算的方法。它依靠固态NMR光谱学来获得高分辨率的光谱和膜蛋白的残基特异性结构限制,这些蛋白在膜法线周围进行旋转扩散,但其迁移率受到与膜磷脂相互作用的限制。单独和与其他蛋白质及配体配合使用的膜蛋白的高分辨率光谱为这些蛋白质在其天然功能环境中的结构确定和功能研究奠定了基础。

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