predictAlternativeSecondaryStructures: Predicts alternative secondary structures of a given RNA...
In ncRNAtools: An R toolkit for non-coding RNA

Description Usage Arguments Value References Examples

View source: R/ncRNAtools_secondaryStructurePredictionFunctions.R

Attempts to identify potential alternative secondary structures of the provided RNA sequence using the RintW method, based on the decomposition of the base-pairing probability matrix over the Hamming distance to a reference secondary structure. It should be noted that RintW runs can take considerable amounts of time.

1	predictAlternativeSecondaryStructures(sequence, gammaWeight=4, inferenceEngine="BL")

`sequence`	string with an RNA sequence whose secondary structure should be predicted. Should contain only standard RNA symbols (i.e., "A", "U", "G" and "C").
`gammaWeight`	weight factor for predicted base pairs. It directly affects the number of predicted base pairs. A higher value leads to a higher number of base pairs predicted. It should be a positive number. In the default behavior, a value of 4 is used.
`inferenceEngine`	engine used to identify the optimal canonical secondary structure. Possible values are "BL", "Turner" and "CONTRAfold". In the first two cases, a McCaskill partition function is applied, using respectively the Boltzmann likelihood model or Turner's energy model. In the third case, the CONTRAfold engine, based on conditional log-linear models, is applied. In the default behavior, a McCaskill partition function with a Boltzmann likelihood model is used.

A list of two-element lists, where each element of the upper level list represents a potential secondary structure. The first top-level element always represents the canonical secondary structure. If no alternative secondary structures are found, simply a list of two elements is returned, comprising the query sequence and the canonical secondary structure.

When alternative secondary structure elements are found, each top-level element comprises the following two elements:

`sequence`	Query RNA sequence
`secondaryStructure`	Predicted secondary structure

Andronescu M, Condon A, Hoos HH, Mathews DH, Murphy KP. Computational approaches for RNA energy parameter estimation. RNA. 2010;16(12):2304-2318. doi:10.1261/rna.1950510

Do CB, Woods DA, Batzoglou S. CONTRAfold: RNA secondary structure prediction without physics-based models. Bioinformatics. 2006;22(14):e90-e98. doi:10.1093/bioinformatics/btl246

Hagio T, Sakuraba S, Iwakiri J, Mori R, Asai K. Capturing alternative secondary structures of RNA by decomposition of base-pairing probabilities. BMC Bioinformatics. 2018;19(Suppl 1):38. Published 2018 Feb 19. doi:10.1186/s12859-018-2018-4

Hamada M, Ono Y, Kiryu H, et al. Rtools: a web server for various secondary structural analyses on single RNA sequences. Nucleic Acids Res. 2016;44(W1):W302-W307. doi:10.1093/nar/gkw337

Mathews DH, Sabina J, Zuker M, Turner DH. Expanded sequence dependence of thermodynamic parameters improves prediction of RNA secondary structure. J Mol Biol. 1999;288(5):911-940. doi:10.1006/jmbi.1999.2700

http://rtools.cbrc.jp/

# Predict alternative secondary structures of an RNA sequence:

alternativeStructures <- predictAlternativeSecondaryStructures("AAAGGGGUUUCCC")

# Count the number of potential alternative structures identified:

length(alternativeStructures)