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Bayesian sampling of evolutionarily conserved RNA secondary structures with pseudoknots

机译:具有假结的进化保守RNA二级结构的贝叶斯采样

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Motivation: Today many non-coding RNAs are known to play an active role in various important biological processes. Since RNA's functionality is correlated with specific structural motifs that are often conserved in phylogenetically related molecules, computational prediction of RNA structure should ideally be based on a set of homologous primary structures. But many available RNA secondary structure prediction programs that use sequence alignments do not consider pseudoknots or their estimations consist on a single structure without information on uncertainty. Results: In this article we present a method that takes advantage of the evolutionary history of a group of aligned RNA sequences for sampling consensus secondary structures, including pseudoknots, according to their approximate posterior probability. We investigate the benefit of using evolutionary history and demonstrate the competitiveness of our method compared with similar methods based on RNase P RNA sequences and simulated data.
机译:动机:如今,许多非编码RNA在各种重要的生物学过程中均起着积极作用。由于RNA的功能性与特定的结构基序相关,这些基序通常在系统发生相关的分子中是保守的,因此理想情况下,RNA结构的计算预测应基于一组同源的一级结构。但是,许多使用序列比对的可用RNA二级结构预测程序都没有考虑假结,或者它们的估计仅包含单个结构而没有不确定性信息。结果:在本文中,我们提出了一种方法,该方法利用一组对齐的RNA序列的进化历史来对共有二级结构(包括假结)进行采样,以根据其近似后验概率。我们调查了使用进化史的好处,并证明了我们的方法与基于RNase P RNA序列和模拟数据的类似方法相比的竞争力。

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