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Template-based prediction of ribosomal RNA secondary structure

机译:基于模板的核糖体RNA二级结构预测

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Determining the structure of ribosomal RNAs (rRNAs) is one of the crucial steps in understanding the process of protein synthesis, for which rRNAs are one of the basic components. Nevertheless, due to extreme technical difficulties, spatial (3D) structures have been resolved experimentally for only 14 organisms. Also, computational prediction of 3D rRNA structure is almost impossible, and prediction of secondary structure (the list of base pairs in the folded RNA), an important intermediate step between sequence and 3D structure that is used broadly in modeling of RNA structures, is in the case of rRNAs hindered by both extreme sequence length and high structure complexity. Here we present a proof-of-concept for an rRNA secondary structure prediction method that utilizes known structures as structural templates. Our template-based prediction algorithm determines those regions of the sequence for which structure is being predicted that are conserved well enough so that their secondary structure can be copied over from the template. The structure of the remaining, unconserved regions is predicted using a thermodynamic folding model. Applying a baseline implementation of our algorithm to the E. coli 16S rRNA, we have achieved state-of-the-art recall and precision using the structure of T. thermophilus 16S rRNA as a template.
机译:确定核糖体RNA(rRNA)的结构是理解蛋白质合成过程的关键步骤之一,为此,rRNA是基本成分之一。然而,由于极端的技术困难,仅对14种生物进行了实验上的空间(3D)结构解析。同样,对3D rRNA结构的计算预测几乎是不可能的,而二级结构(折叠后的RNA中的碱基对列表)的预测则是不可能的,这是广泛用于RNA结构建模的序列和3D结构之间的重要中间步骤。极端序列长度和高结构复杂性都阻碍了rRNA的案例。在这里,我们介绍了利用已知结构作为结构模板的rRNA二级结构预测方法的概念验证。我们基于模板的预测算法可确定序列中要对其结构进行充分保守的那些区域,以便可以从模板复制其二级结构。使用热力学折叠模型预测剩余的非保守区域的结构。将我们的算法的基线实现应用于大肠杆菌16S rRNA,我们以嗜热链球菌16S rRNA的结构为模板,实现了最新的召回率和精确度。

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