多蛋白复合物的中等分辨率冷冻电镜图谱解读。

Interpretation of medium resolution cryoEM maps of multi-protein complexes.

机构信息

MRC Laboratory of Molecular Biology, Cambridge CB2 0QH, United Kingdom.

出版信息

Curr Opin Struct Biol. 2019 Oct;58:166-174. doi: 10.1016/j.sbi.2019.06.009. Epub 2019 Jul 27.

DOI:10.1016/j.sbi.2019.06.009

PMID:31362190

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6863432/

Abstract

Electron cryo-microscopy (cryoEM) is used to determine structures of biological molecules, including multi-protein complexes. Maps at better than 3.0Å resolution are relatively straightforward to interpret since atomic models of proteins and nucleic acids can be built directly. Still, these resolutions are often difficult to achieve, and map quality frequently varies within a structure. This results in data that are challenging to interpret, especially when crystal structures or suitable homology models are not available. Recent advances in mass spectrometry techniques, computational methods and model building tools facilitate subunit/domain fitting into maps, elucidation of protein contacts, and de novo generation of atomic models. Here, we review techniques for map interpretation and provide examples from recent studies of multi-protein complexes.

摘要

电子冷冻显微镜（cryoEM）用于确定生物分子的结构，包括多蛋白复合物。分辨率优于 3.0Å 的图谱相对容易解释，因为可以直接构建蛋白质和核酸的原子模型。尽管如此，这些分辨率通常很难达到，而且结构内的图谱质量经常变化。这导致数据难以解释，尤其是在没有晶体结构或合适的同源模型的情况下。质谱技术、计算方法和模型构建工具的最新进展有助于将亚基/结构域拟合到图谱中，阐明蛋白质接触，并从头生成原子模型。在这里，我们回顾了图谱解释技术，并提供了来自多蛋白复合物的最新研究的示例。

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多蛋白复合物的中等分辨率冷冻电镜图谱解读。

Interpretation of medium resolution cryoEM maps of multi-protein complexes.

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