Fast selection of miRNA candidates based on large-scale pre-computed MFE sets of randomized sequences

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Abstract

Background: Small RNAs are important regulators of genome function, yet their prediction in genomes is still a major computational challenge. Statistical analyses of pre-miRNA sequences indicated that their 2D structure tends to have a minimal free energy (MFE) significantly lower than MFE values of equivalently randomized sequences with the same nucleotide composition, in contrast to other classes of non-coding RNA. The computation of many MFEs is, however, too intensive to allow for genome-wide screenings. Results: Using a local grid infrastructure, MFE distributions of random sequences were pre-calculated on a large scale. These distributions follow a normal distribution and can be used to determine the MFE distribution for any given sequence composition by interpolation. It allows on-the-fly calculation of the normal distribution for any candidate sequence composition. Conclusion: The speedup achieved makes genome-wide screening with this characteristic of a pre-miRNA sequence practical. Although this particular property alone will not be able to distinguish miRNAs from other sequences sufficiently discriminative, the MFE-based P-value should be added to the parameters of choice to be included in the selection of potential miRNA candidates for experimental verification. © 2014 Warris et al.; licensee BioMed Central Ltd.

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Warris, S., Boymans, S., Muiser, I., Noback, M., Krijnen, W., & Nap, J. P. (2014). Fast selection of miRNA candidates based on large-scale pre-computed MFE sets of randomized sequences. BMC Research Notes, 7(1). https://doi.org/10.1186/1756-0500-7-34

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