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Evaluating native-like structures of RNA-protein complexes through the deep learning method

Author

Listed:
  • Chengwei Zeng

    (Central China Normal University)

  • Yiren Jian

    (Dartmouth College)

  • Soroush Vosoughi

    (Dartmouth College)

  • Chen Zeng

    (The George Washington University)

  • Yunjie Zhao

    (Central China Normal University)

Abstract

RNA-protein complexes underlie numerous cellular processes, including basic translation and gene regulation. The high-resolution structure determination of the RNA-protein complexes is essential for elucidating their functions. Therefore, computational methods capable of identifying the native-like RNA-protein structures are needed. To address this challenge, we thus develop DRPScore, a deep-learning-based approach for identifying native-like RNA-protein structures. DRPScore is tested on representative sets of RNA-protein complexes with various degrees of binding-induced conformation change ranging from fully rigid docking (bound-bound) to fully flexible docking (unbound-unbound). Out of the top 20 predictions, DRPScore selects native-like structures with a success rate of 91.67% on the testing set of bound RNA-protein complexes and 56.14% on the unbound complexes. DRPScore consistently outperforms existing methods with a roughly 10.53–15.79% improvement, even for the most difficult unbound cases. Furthermore, DRPScore significantly improves the accuracy of the native interface interaction predictions. DRPScore should be broadly useful for modeling and designing RNA-protein complexes.

Suggested Citation

  • Chengwei Zeng & Yiren Jian & Soroush Vosoughi & Chen Zeng & Yunjie Zhao, 2023. "Evaluating native-like structures of RNA-protein complexes through the deep learning method," Nature Communications, Nature, vol. 14(1), pages 1-9, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-36720-9
    DOI: 10.1038/s41467-023-36720-9
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    References listed on IDEAS

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