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Sequence–structure relationships in RNA loops: establishing the basis for loop homology modeling

机译:RNA环中的序列-结构关系:建立环同源性建模的基础

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The specific function of RNA molecules frequently resides in their seemingly unstructured loop regions. We performed a systematic analysis of RNA loops extracted from experimentally determined three-dimensional structures of RNA molecules. A comprehensive loop-structure data set was created and organized into distinct clusters based on structural and sequence similarity. We detected clear evidence of the hallmark of homology present in the sequence–structure relationships in loops. Loops differing by 25% in sequence identity fold into very similar structures. Thus, our results support the application of homology modeling for RNA loop model building. We established a threshold that may guide the sequence divergence-based selection of template structures for RNA loop homology modeling. Of all possible sequences that are, under the assumption of isosteric relationships, theoretically compatible with actual sequences observed in RNA structures, only a small fraction is contained in the Rfam database of RNA sequences and classes implying that the actual RNA loop space may consist of a limited number of unique loop structures and conserved sequences. The loop-structure data sets are made available via an online database, RLooM. RLooM also offers functionalities for the modeling of RNA loop structures in support of RNA engineering and design efforts.
机译:RNA分子的特定功能通常位于它们看似无结构的环区域。我们对从实验确定的RNA分子三维结构提取的RNA环进行了系统的分析。基于结构和序列相似性,创建了一个完整的回路结构数据集并将其组织为不同的簇。我们检测到循环中序列-结构关系中存在同源标记的清晰证据。序列同一性相差小于25%的环折叠成非常相似的结构。因此,我们的结果支持同源性建模在RNA环模型构建中的应用。我们建立了一个阈值,可以指导基于序列差异的RNA环同源性建模模板结构的选择。在等构关系的假设下,所有可能的序列在理论上都与RNA结构中观察到的实际序列相容,在Rfam RNA序列和类别数据库中仅包含一小部分,这意味着实际的RNA环空间可能包含一个有限数量的独特环结构和保守序列。回路结构数据集可通过在线数据库RLooM获得。 RLooM还提供了用于RNA环结构建模的功能,以支持RNA工程和设计工作。

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