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Integrating Diverse Data for Structure Determination of Macromolecular Assemblies.

机译:整合各种数据来确定大分子组装体的结构。

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摘要

To understand the cell, we need to determine the macromolecular assembly structures, which may consist of tens to hundreds of components. First, we review the varied experimental data that characterize the assemblies at several levels of resolution. We then describe computational methods for generating the structures using these data. To maximize completeness, resolution, accuracy, precision, and efficiency of the structure determination, a computational approach is required that uses spatial information from a variety of experimental methods. We propose such an approach, defined by its three main components: a hierarchical representation of the assembly, a scoring function consisting of spatial restraints derived from experimental data, and an optimization method that generates structures consistent with the data. This approach is illustrated by determining the configuration of the 456 proteins in the nuclear pore complex (NPC) from baker's yeast. With these tools, we are poised to integrate structural information gathered at multiple levels of the biological hierarchy-from atoms to cells-into a common framework.
机译:要了解细胞,我们需要确定大分子组装结构,该结构可能包含数十到数百个组件。首先,我们回顾各种分辨率的实验数据,这些数据表征了装配体。然后,我们描述使用这些数据生成结构的计算方法。为了使结构确定的完整性,分辨率,准确性,精确性和效率最大化,需要一种使用来自各种实验方法的空间信息的计算方法。我们提出了这样一种方法,该方法由其三个主要组成部分定义:装配体的层次表示形式,由实验数据派生的空间约束组成的评分函数以及生成与数据一致的结构的优化方法。通过确定来自面包酵母的核孔复合物(NPC)中456种蛋白质的构型,可以说明这种方法。使用这些工具,我们准备将在生物层次结构的各个层次(从原子到细胞)收集的结构信息整合到一个通用框架中。

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