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盘状结构域家族再探讨:来自原核生物的新成员及基于同源性的折叠预测

The discoidin domain family revisited: new members from prokaryotes and a homology-based fold prediction.

作者信息

Baumgartner S, Hofmann K, Chiquet-Ehrismann R, Bucher P

机构信息

Lund University, Department of Cell & Molecular Biology, Sweden.

出版信息

Protein Sci. 1998 Jul;7(7):1626-31. doi: 10.1002/pro.5560070717.

Abstract

Members of the discoidin (DS) domain family, which includes the C1 and C2 repeats of blood coagulation factors V and VIII, occur in a great variety of eukaryotic proteins, most of which have been implicated in cell-adhesion or developmental processes. So far, no three-dimensional structure of a known example of this extracellular module has been determined, limiting the usefulness of identifying a new sequence as member of this family. Here, we present results of a recent search of the protein sequence database for new DS domains using generalized profiles, a sensitive multiple alignment-based search technique. Several previously unrecognized DS domains could be identified by this method, including the first examples from prokaryotic species. More importantly, we present statistical, structural, and functional evidence that the D1 domain of galactose oxidase whose three-dimensional structure has been determined at 1.7 A resolution, is a distant member of this family. Taken together, these findings significantly expand the concept of the DS domain, by extending its taxonomic range and by implying a fold prediction for all its members. The proposed alignment with the galactose oxidase sequence makes it possible to construct homology-based three-dimensional models for the most interesting examples, as illustrated by an accompanying paper on the C1 and C2 domains of factor V.

摘要

盘状结构域(DS)家族成员包括凝血因子V和VIII的C1和C2重复序列,存在于多种真核生物蛋白质中,其中大多数与细胞黏附或发育过程有关。到目前为止,尚未确定该细胞外模块已知实例的三维结构,这限制了将新序列鉴定为该家族成员的实用性。在此,我们展示了最近使用广义谱(一种基于敏感多重比对的搜索技术)在蛋白质序列数据库中搜索新DS结构域的结果。通过这种方法可以鉴定出几个以前未被识别的DS结构域,包括来自原核生物物种的首个实例。更重要的是,我们提供了统计、结构和功能证据,表明已以1.7埃分辨率确定三维结构的半乳糖氧化酶的D1结构域是该家族的远亲成员。综上所述,这些发现通过扩展其分类范围并暗示其所有成员的折叠预测,显著扩展了DS结构域的概念。与半乳糖氧化酶序列的拟议比对使得能够为最有趣的实例构建基于同源性的三维模型,如随附的一篇关于因子V的C1和C2结构域的论文所示。

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