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Retrieving high-resolution information from disordered 2D crystals by single-particle cryo-EM

机译:通过单粒子低温电磁波从无序2D晶体中检索高分辨率信息

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Electron crystallography can reveal the structure of membrane proteins within 2D crystals under close-to-native conditions. High-resolution structural information can only be reached if crystals are perfectly flat and highly ordered. In practice, such crystals are difficult to obtain. Available image unbending algorithms correct for disorder, but only perform well on images of non-tilted, flat crystals, while out-of-plane distortions are not addressed. Here, we present an approach that employs single-particle refinement procedures to locally unbend crystals in 3D. With this method, density maps of the MloK1 potassium channel with a resolution of 4 ? were obtained from images of 2D crystals that do not diffract beyond 10 ?. Furthermore, 3D classification allowed multiple structures to be resolved, revealing a series of MloK1 conformations within a single 2D crystal. This conformational heterogeneity explains the poor diffraction observed and is related to channel function. The approach is implemented in the FOCUS package.
机译:电子晶体学可以揭示在接近自然条件下二维晶体中膜蛋白的结构。仅当晶体完全平坦且高度有序时,才能获得高分辨率的结构信息。实际上,难以获得这种晶体。可用的图像非弯曲算法可纠正混乱,但仅在非倾斜,扁平晶体的图像上表现良好,而无法解决面外失真。在这里,我们提出一种采用单颗粒细化程序以3D方式局部弯曲晶体的方法。用这种方法,MloK1钾离子通道的密度图分辨率为4?。从衍射不超过10?的2D晶体的图像获得。此外,3D分类允许解析多个结构,从而揭示了单个2D晶体中的一系列MloK1构象。这种构象异质性解释了观察到的衍射差,并且与通道功能有关。该方法在FOCUS软件包中实现。

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