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Pathways

Overview

This page provides information about how the programs in RNAstructure work together to provide sample pathways for solving common problems. In each pathway diagram, lines indicate files (annotated with file extensions) and programs are represented by boxes.



Secondary Structure Prediction

Secondary structure prediction can be accomplished in a number of ways. At this time, we recommend three approaches, free energy minimization, maximum expected accuracy, and ProbKnot. Often it would be best to try all three to provide alternative hypotheses for the secondary structure. Free energy minimization (Fold) predicts the lowest free energy structure (the single most probable structure) and a set of low free energy structures. Maximum expected accuracy (MaxExpect) assembles a structure composed of probably base pairs, and the pairs in these structures are slightly more likely to be correctly predicted than those in minimum free energy structures. ProbKnot is capable of predicting structures with pseudoknots. For each approach, we recommend color annotating the predicted secondary structures with base pairing probabilties. Highly probably pairs are more likely to be correctly predicted than less probable pairs.

mfe

mea

pseudoknot prediction



Predicting a Conserved RNA Structure Common to Multiple Homologs.

The accuracy of RNA secondary structure prediction can be dramatically improved by predicting a structure conserved by two or more homologs. RNAstructure has several programs that predict conserved structures. For two sequences, dynalign_ii or PARTS can be used for two sequences. For three or more sequences, TurboFold or multilign can be used. TurboFold is much faster and can predict base pairing probabilities. Multilign, however, is more suited if the set of sequences have low pairwise identity (roughly less than 60% identity).

dynalign_ii

PARTS

multilign

TurboFold


Bimolecular structure prediction

There are three major applications in RNAstructure for predicing the structure of two interacting RNA strands. The first, bifold, predicts the structure of two sequences, and allows for intermolecular and intramolecular base pairs. The second, DuplexFold, predicts the structure, but only allowing for intermolecular pairs. It is the fastest of the three applications. The third, AccessFold only alloes intermolecular pairs, but it accounts for the accessibility of each strand, given the competition with intramolecular pairs.

bifold

DuplexFold

AccessFold