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Development of a motif-based topology-independent structure comparison method to identify evolutionarily related folds

机译:开发基于图案的拓扑独立结构比较方法以识别进化相关的折叠

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摘要

Structure conservation, functional similarities and homologous relationships that exist across diverse protein topologies suggest that some regions of the protein fold universe are continuous. However, the current structure classification systems are based on hierarchical organizations, which cannot accommodate structural relationships that span fold definitions. Here we describe a novel, supersecondary-structure motif-based, topology-independent structure comparison method (SmotifCOMP) that is able to quantitatively identify structural relationships between disparate topologies. The basis of SmotifCOMP is a systematically defined supersecondary-structure motif library whose representative geometries are shown to be saturated in the Protein Data Bank and exhibit a unique distribution within the known folds. SmotifCOMP offers a robust and quantitative technique to compare domains that adopt different topologies since the method does not rely on a global superposition. SmotifCOMP is used to perform an exhaustive comparison of the known folds and the identified relationships are used to produce a non-hierarchical representation of the fold space that reflects the notion of a continuous and connected fold universe. The current work offers insight into previously hypothesized evolutionary relationships between disparate folds and provides a resource for exploring novel ones.
机译:跨多种蛋白质拓扑结构存在的结构保守性,功能相似性和同源关系表明,蛋白质折叠世界的某些区域是连续的。但是,当前的结构分类系统基于层次结构的组织,不能适应跨越折叠定义的结构关系。在这里,我们描述了一种新颖的,基于超二级结构的基于基元的,独立于拓扑的结构比较方法(SmotifCOMP),该方法能够定量识别不同拓扑之间的结构关系。 SmotifCOMP的基础是系统定义的超二级结构基序库,该库的代表性几何结构在蛋白质数据库中显示为饱和,并且在已知折叠范围内表现出独特的分布。由于该方法不依赖于全局叠加,因此SmotifCOMP提供了一种健壮且定量的技术来比较采用不同拓扑的域。 SmotifCOMP用于对已知折痕进行详尽的比较,识别出的关系用于产生折痕空间的非分层表示,反映了连续且相连的折痕宇宙的概念。当前的工作提供了对不同折叠之间先前假设的进化关系的见解,并提供了探索新颖折叠的资源。

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