RIsearch: fast RNA-RNA interaction search using a simplified nearest-neighbor energy model

被引:67
|
作者
Wenzel, Anne [1 ,2 ]
Akbasli, Erdinc [3 ]
Gorodkin, Jan [1 ,2 ]
机构
[1] Univ Copenhagen, Ctr Noncoding RNA Technol & Hlth, DK-1870 Frederiksberg, Denmark
[2] Univ Copenhagen, Dept Vet Clin & Anim Sci, DK-1870 Frederiksberg, Denmark
[3] Univ Copenhagen, Software Dev Grp, DK-2300 Copenhagen S, Denmark
关键词
SECONDARY STRUCTURE PREDICTION; BASE-PAIRING PROBABILITIES; NONCODING RNAS; COMPARATIVE GENOMICS; TARGETS; IDENTIFICATION; ALGORITHM; ACCESSIBILITY; ALIGNMENTS; STABILITY;
D O I
10.1093/bioinformatics/bts519
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
Motivation: Regulatory, non-coding RNAs often function by forming a duplex with other RNAs. It is therefore of interest to predict putative RNA-RNA duplexes in silico on a genome-wide scale. Current computational methods for predicting these interactions range from fast complementary-based searches to those that take intramolecular binding into account. Together these methods constitute a trade-off between speed and accuracy, while leaving room for improvement within the context of genome-wide screens. A fast pre-filtering of putative duplexes would therefore be desirable. Results: We present RIsearch, an implementation of a simplified Turner energy model for fast computation of hybridization, which significantly reduces runtime while maintaining accuracy. Its time complexity for sequences of lengths m and n is O(m.n) with a much smaller pre-factor than other tools. We show that this energy model is an accurate approximation of the full energy model for near-complementary RNA-RNA duplexes. RIsearch uses a Smith-Waterman-like algorithm using a dinucleotide scoring matrix which approximates the Turner nearest-neighbor energies. We show in benchmarks that we achieve a speed improvement of at least 2.4x compared with RNAplex, the currently fastest method for searching near-complementary regions. RIsearch shows a prediction accuracy similar to RNAplex on two datasets of known bacterial short RNA (sRNA)-messenger RNA (mRNA) and eukaryotic microRNA (miRNA)-mRNA interactions. Using RIsearch as a pre-filter in genome-wide screens reduces the number of binding site candidates reported by miRNA target prediction programs, such as TargetScanS and miRanda, by up to 70%. Likewise, substantial filtering was performed on bacterial RNA-RNA interaction data.
引用
收藏
页码:2738 / 2746
页数:9
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