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Old Dog, New Tricks: Exact Seeding Strategy Improves RNA Design Performances

  • Théo Boury
  • , Leonhard Sidl
  • , Ivo L. Hofacker
  • , Yann Ponty
  • , Hua Ting Yao
  • Laboratoire d'Informatique (LIX)
  • University of Vienna

Research output: Chapter in Book/Report/Conference proceedingConference contributionpeer-review

Abstract

The Inverse Folding problem involves identifying RNA sequences that adopt a target structure with respect to free-energy minimization, i.e., preferential to all alternative structures. The problem has historically been regarded as challenging, largely due to its proven NP-completeness of an extended version where the base pair maximization energy model is used. In contrast, it has recently been shown that a large subset called m-separable structures, notably including those comprising helices of length 3+, can be solved in linear time within the same energy model. This permits not only the identification of a single solution but also the characterization of a language of solutions. In this work, we seek to describe the “hardness” of Inverse Folding, bridging (at least heuristically) the gap between a simplified energy model and a more realistic Turner energy model. We used LinearBPDesign to generate seed sequences for RNAinverse, thereby improving the design process in a Turner energy model. To this end, we extended LinearBPDesign to accommodate biseparability and to handle non- or high modulo separable structures by minimalist addition of base pairs. Our study suggests that seeds generated by LinearBPDesign capture long-range interactions, thereby improving the performance of RNAinverse compared to seed focusing on refining the energy model itself. Most surprisingly, a significant number of LinearBPDesign seeds uniquely fold into the target structure in the Turner model, especially when helices are at least of length 2. This observation suggests that the “hardness” of design may arise from the intrinsic properties of the structures themselves.

Original languageEnglish
Title of host publicationResearch in Computational Molecular Biology - 29th International Conference, RECOMB 2025, Proceedings
EditorsSriram Sankararaman
PublisherSpringer Science and Business Media Deutschland GmbH
Pages134-152
Number of pages19
ISBN (Print)9783031902512
DOIs
Publication statusPublished - 1 Jan 2025
Event29th International Conference on Research in Computational Molecular Biology, RECOMB 2025 - Seoul, Korea, Republic of
Duration: 26 Apr 202529 Apr 2025

Publication series

NameLecture Notes in Computer Science
Volume15647 LNBI
ISSN (Print)0302-9743
ISSN (Electronic)1611-3349

Conference

Conference29th International Conference on Research in Computational Molecular Biology, RECOMB 2025
Country/TerritoryKorea, Republic of
CitySeoul
Period26/04/2529/04/25

Keywords

  • Dynamic programming
  • RNA design
  • RNA secondary structure
  • Sampling

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