DARS-RNP and QUASI-RNP: New statistical potentials for protein-RNA docking

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Abstract

Background: Protein-RNA interactions play fundamental roles in many biological processes. Understanding the molecular mechanism of protein-RNA recognition and formation of protein-RNA complexes is a major challenge in structural biology. Unfortunately, the experimental determination of protein-RNA complexes is tedious and difficult, both by X-ray crystallography and NMR. For many interacting proteins and RNAs the individual structures are available, enabling computational prediction of complex structures by computational docking. However, methods for protein-RNA docking remain scarce, in particular in comparison to the numerous methods for protein-protein docking.Results: We developed two medium-resolution, knowledge-based potentials for scoring protein-RNA models obtained by docking: the quasi-chemical potential (QUASI-RNP) and the Decoys As the Reference State potential (DARS-RNP). Both potentials use a coarse-grained representation for both RNA and protein molecules and are capable of dealing with RNA structures with posttranscriptionally modified residues. We compared the discriminative power of DARS-RNP and QUASI-RNP for selecting rigid-body docking poses with the potentials previously developed by the Varani and Fernandez groups.Conclusions: In both bound and unbound docking tests, DARS-RNP showed the highest ability to identify native-like structures. © 2011 Tuszynska and Bujnicki; licensee BioMed Central Ltd.

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Tuszynska, I., & Bujnicki, J. M. (2011). DARS-RNP and QUASI-RNP: New statistical potentials for protein-RNA docking. BMC Bioinformatics, 12. https://doi.org/10.1186/1471-2105-12-348

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