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Main Authors: Weber, Mirko, Erichson, Felix, Antczak, Maciej, Zok, Tomasz, Steffen, Fabio D., Szachniuk, Marta, Börner, Richard
Format: Preprint
Published: 2025
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Online Access:https://arxiv.org/abs/2509.18301
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author Weber, Mirko
Erichson, Felix
Antczak, Maciej
Zok, Tomasz
Steffen, Fabio D.
Szachniuk, Marta
Börner, Richard
author_facet Weber, Mirko
Erichson, Felix
Antczak, Maciej
Zok, Tomasz
Steffen, Fabio D.
Szachniuk, Marta
Börner, Richard
contents Integrative biomolecular modeling of RNA relies on structural refined collections and accurate experimental data that reflect binding and folding behavior. However, the prediction of such collections remains challenging due to the rugged energy landscape and extensive conformational heterogeneity of large RNAs. To overcome these limitations, we applied a FRET-guided strategy to identify RNA conformational states consistent with single-molecule FRET (smFRET) experiments. We predicted 3D structures of a ribosomal RNA tertiary contact comprising a GAAA tetraloop and a kissing loop using three popular RNA 3D modeling tools namely RNAComposer, FARFAR2, and AlphaFold3, yielding a collection of candidate conformations. These models were structurally validated based on Watson-Crick base-pairing patterns and filtered using an eRMSD threshold. For each retained structure, we computed the accessible contact volume (ACV) of the sCy3/sCy5 dye pair using FRETraj to predict FRET distributions. These distributions were then compared and weighted against experimental smFRET data to identify conformational states compatible with the observed FRET states. Our results demonstrate that experimental transfer efficiencies can be reproduced using \textit{in silico} predicted RNA 3D structures. This FRET-guided workflow, combined with structural validation, lays the foundation for capturing the highly diverse conformational states characteristic of flexible RNA motifs.
format Preprint
id arxiv_https___arxiv_org_abs_2509_18301
institution arXiv
publishDate 2025
record_format arxiv
spellingShingle FRET-guided selection of RNA 3D structures
Weber, Mirko
Erichson, Felix
Antczak, Maciej
Zok, Tomasz
Steffen, Fabio D.
Szachniuk, Marta
Börner, Richard
Biological Physics
Integrative biomolecular modeling of RNA relies on structural refined collections and accurate experimental data that reflect binding and folding behavior. However, the prediction of such collections remains challenging due to the rugged energy landscape and extensive conformational heterogeneity of large RNAs. To overcome these limitations, we applied a FRET-guided strategy to identify RNA conformational states consistent with single-molecule FRET (smFRET) experiments. We predicted 3D structures of a ribosomal RNA tertiary contact comprising a GAAA tetraloop and a kissing loop using three popular RNA 3D modeling tools namely RNAComposer, FARFAR2, and AlphaFold3, yielding a collection of candidate conformations. These models were structurally validated based on Watson-Crick base-pairing patterns and filtered using an eRMSD threshold. For each retained structure, we computed the accessible contact volume (ACV) of the sCy3/sCy5 dye pair using FRETraj to predict FRET distributions. These distributions were then compared and weighted against experimental smFRET data to identify conformational states compatible with the observed FRET states. Our results demonstrate that experimental transfer efficiencies can be reproduced using \textit{in silico} predicted RNA 3D structures. This FRET-guided workflow, combined with structural validation, lays the foundation for capturing the highly diverse conformational states characteristic of flexible RNA motifs.
title FRET-guided selection of RNA 3D structures
topic Biological Physics
url https://arxiv.org/abs/2509.18301