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Identifying novel sequence variants of RNA 3D motifs

机译:识别RNA 3D基序的新型序列变体

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摘要

Predicting RNA 3D structure from sequence is a major challenge in biophysics. An important sub-goal is accurately identifying recurrent 3D motifs from RNA internal and hairpin loop sequences extracted from secondary structure (2D) diagrams. We have developed and validated new probabilistic models for 3D motif sequences based on hybrid Stochastic Context-Free Grammars and Markov Random Fields (SCFG/MRF). The SCFG/MRF models are constructed using atomic-resolution RNA 3D structures. To parameterize each model, we use all instances of each motif found in the RNA 3D Motif Atlas and annotations of pairwise nucleotide interactions generated by the FR3D software. Isostericity relations between non-Watson–Crick basepairs are used in scoring sequence variants. SCFG techniques model nested pairs and insertions, while MRF ideas handle crossing interactions and base triples. We use test sets of randomly-generated sequences to set acceptance and rejection thresholds for each motif group and thus control the false positive rate. Validation was carried out by comparing results for four motif groups to RMDetect. The software developed for sequence scoring (JAR3D) is structured to automatically incorporate new motifs as they accumulate in the RNA 3D Motif Atlas when new structures are solved and is available free for download.
机译:从序列预测RNA 3D结构是生物物理学中的主要挑战。一个重要的子目标是从从二级结构(2D)图中提取的RNA内部序列和发夹环序列中准确识别重复的3D主题。我们已经开发并验证了基于混合随机上下文无关文法和马尔可夫随机场(SCFG / MRF)的3D主题序列的新概率模型。 SCFG / MRF模型是使用原子分辨率RNA 3D结构构建的。为了参数化每个模型,我们使用在RNA 3D Motif Atlas中发现的每个基序的所有实例,以及由FR3D软件生成的成对核苷酸相互作用的注释。非沃森-克里克碱基对之间的等距关系用于评分序列变体。 SCFG技术为嵌套对和插入建模,而MRF想法处理交叉交互和基础三元组。我们使用随机生成序列的测试集为每个基序组设置接受和拒绝阈值,从而控制假阳性率。通过将四个基序组的结果与RMDetect进行比较来进行验证。开发用于序列评分的软件(JAR3D)的结构是,在解决新结构后,新的基序在RNA 3D Motif Atlas中累积时会自动合并,并且可以免费下载。

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