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</script>pmid: 23088372
pmc: PMC3549849
Background: We study the sparsification of dynamic programming folding algorithms of RNA structures. Sparsification applies to the mfe-folding of RNA structures and can lead to a significant reduction of time complexity. Results: We analyze the sparsification of a particular decomposition rule, $��^*$, that splits an interval for RNA secondary and pseudoknot structures of fixed topological genus. Essential for quantifying the sparsification is the size of its so called candidate set. We present a combinatorial framework which allows by means of probabilities of irreducible substructures to obtain the expected size of the set of $��^*$-candidates. We compute these expectations for arc-based energy models via energy-filtered generating functions (GF) for RNA secondary structures as well as RNA pseudoknot structures. For RNA secondary structures we also consider a simplified loop-energy model. This combinatorial analysis is then compared to the expected number of $��^*$-candidates obtained from folding mfe-structures. In case of the mfe-folding of RNA secondary structures with a simplified loop energy model our results imply that sparsification provides a reduction of time complexity by a constant factor of 91% (theory) versus a 96% reduction (experiment). For the "full" loop-energy model there is a reduction of 98% (experiment).
27 pages, 12 figures
QH301-705.5, Sparsification, Applied Mathematics, Research, QH426-470, Dynamic programming, Computational Theory and Mathematics, Structural Biology, Genetics, FOS: Mathematics, Mathematics - Combinatorics, Combinatorics (math.CO), math.CO, Biology (General), Molecular Biology, 32Q55, Generating function
QH301-705.5, Sparsification, Applied Mathematics, Research, QH426-470, Dynamic programming, Computational Theory and Mathematics, Structural Biology, Genetics, FOS: Mathematics, Mathematics - Combinatorics, Combinatorics (math.CO), math.CO, Biology (General), Molecular Biology, 32Q55, Generating function
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