MOTIVATION: Regulatory RNAs often unfold their action via RNA-RNA interaction. Transcriptional gene silencing by means of siRNAs and miRNA as well as snoRNA directed RNA editing rely on this mechanism. Additionally ncRNA regulation in bacteria is mainly based upon RNA duplex formation. Finding putative target sites for newly discovered ncRNAs is a lengthy task as tools for cofolding RNA molecules like RNAcofold and RNAup are too slow for genome-wide search. Tools like RNAhybrid that neglects intramolecular interactions have runtimes proportional to O(m x n), albeit with a large prefactor. Still in many cases the need for even faster methods exists. RESULTS: We present a new program, RNAplex, especially designed to quickly find possible hybridization sites for a query RNA in large RNA databases. RNAplex uses a slightly different energy model which reduces the computational time by a factor 10-27 compared to RNAhybrid. In addition a length penalty allows to focus the target search on short highly stable interactions. AVAILABILITY: RNAplex can be downloaded at http://www.tbi.univie.ac.at/~htafer/ SUPPLEMENTARY INFORMATION: Supplementary data are available at Bioinformatics online.
展开▼
机译:动机:调节性RNA通常通过RNA-RNA相互作用发挥作用。通过siRNA和miRNA以及snoRNA指导的RNA编辑实现转录基因沉默依赖于这种机制。另外,细菌中的ncRNA调节主要基于RNA双链体的形成。为新发现的ncRNA寻找假定的靶位点是一项艰巨的任务,因为共折叠RNA分子(如RNAcofold和RNAup)的工具对于全基因组搜索而言太慢了。诸如RNAhybrid之类的忽略分子内相互作用的工具,其运行时间与O(m x n)成正比,尽管它的前置因子很大。在许多情况下,仍然需要更快的方法。结果:我们提出了一个新程序RNAplex,该程序专门用于在大型RNA数据库中快速找到查询RNA的可能杂交位点。 RNAplex使用略有不同的能量模型,与RNAhybrid相比,该模型将计算时间减少了10-27倍。另外,长度损失允许将目标搜索集中在短暂的高度稳定的交互上。可用性:RNAplex可以从http://www.tbi.univie.ac.at/~htafer/下载。补充信息:补充数据可从在线生物信息学获得。
展开▼
