RNAsnoop: efficient target prediction for H/ACA snoRNAs
Open Access
- 16 December 2009
- journal article
- research article
- Published by Oxford University Press (OUP) in Bioinformatics
- Vol. 26 (5) , 610-616
- https://doi.org/10.1093/bioinformatics/btp680
Abstract
Motivation: Small nucleolar RNAs are an abundant class of non-coding RNAs that guide chemical modifications of rRNAs, snRNAs and some mRNAs. In the case of many ‘orphan’ snoRNAs, the targeted nucleotides remain unknown, however. The box H/ACA subclass determines uridine residues that are to be converted into pseudouridines via specific complementary binding in a well-defined secondary structure configuration that is outside the scope of common RNA (co-)folding algorithms. Results:RNAsnoop implements a dynamic programming algorithm that computes thermodynamically optimal H/ACA-RNA interactions in an efficient scanning variant. Complemented by an support vector machine (SVM)-based machine learning approach to distinguish true binding sites from spurious solutions and a system to evaluate comparative information, it presents an efficient and reliable tool for the prediction of H/ACA snoRNA target sites. We apply RNAsnoop to identify the snoRNAs that are responsible for several of the remaining ‘orphan’ pseudouridine modifications in human rRNAs, and we assign a target to one of the five orphan H/ACA snoRNAs in Drosophila. Availability: The C source code of RNAsnoop is freely available at http://www.tbi.univie.ac.at/∼htafer/RNAsnoop Contact:htafer@tbi.univie.ac.at Supplementary information: Supplementary data are available at Bioinformatics online.Keywords
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