Department of Chemistry, National Tsing Hua University, Hsinchu, Taiwan.
Nucleic Acids Res. 2010 Aug;38(14):e150. doi: 10.1093/nar/gkq478. Epub 2010 Jun 4.
Proteins with insignificant sequence and overall structure similarity may still share locally conserved contiguous structural segments; i.e. structural/3D motifs. Most methods for finding 3D motifs require a known motif to search for other similar structures or functionally/structurally crucial residues. Here, without requiring a query motif or essential residues, a fully automated method for discovering 3D motifs of various sizes across protein families with different folds based on a 16-letter structural alphabet is presented. It was applied to structurally non-redundant proteins bound to DNA, RNA, obligate/non-obligate proteins as well as free DNA-binding proteins (DBPs) and proteins with known structures but unknown function. Its usefulness was illustrated by analyzing the 3D motifs found in DBPs. A non-specific motif was found with a 'corner' architecture that confers a stable scaffold and enables diverse interactions, making it suitable for binding not only DNA but also RNA and proteins. Furthermore, DNA-specific motifs present 'only' in DBPs were discovered. The motifs found can provide useful guidelines in detecting binding sites and computational protein redesign.
尽管蛋白质的序列和整体结构相似度不高,但它们可能仍然具有局部保守的连续结构片段,即结构/3D 基序。大多数寻找 3D 基序的方法都需要一个已知的基序来搜索其他类似的结构或功能/结构关键残基。在这里,我们提出了一种无需查询基序或必需残基的方法,该方法可以基于 16 字母结构字母表,在具有不同折叠的蛋白质家族中发现各种大小的 3D 基序。该方法应用于与 DNA、RNA 结合的结构非冗余蛋白、必需/非必需蛋白以及具有已知结构但未知功能的游离 DNA 结合蛋白 (DBP) 和蛋白。通过分析 DBP 中发现的 3D 基序,说明了该方法的有用性。发现了一种具有“角”结构的非特异性基序,它提供了一个稳定的支架,并允许多样化的相互作用,使其不仅适合与 DNA 结合,还适合与 RNA 和蛋白质结合。此外,还发现了仅存在于 DBP 中的 DNA 特异性基序。所发现的基序可以为检测结合位点和计算蛋白质重新设计提供有用的指导。
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