RNA-binding protein recognition based on multi-view deep feature and multi-label learning

Haitao Yang; Zhaohong Deng; Xiaoyong Pan; Hong-Bin Shen; Kup-Sze Choi; Lei Wang; Shitong Wang; Jing Wu

doi:10.1093/bib/bbaa174

RNA-binding protein recognition based on multi-view deep feature and multi-label learning

Brief Bioinform. 2021 May 20;22(3):bbaa174. doi: 10.1093/bib/bbaa174.

Authors

Haitao Yang¹, Zhaohong Deng², Xiaoyong Pan³, Hong-Bin Shen⁴, Kup-Sze Choi⁵, Lei Wang⁶, Shitong Wang⁷, Jing Wu⁶

Affiliations

¹ Jiangnan University.
² School of Artificial Intelligence and Computer Science of Jiangnan University, Key Laboratory of Computational Neuroscience and Brain-Inspired Intelligence (LCNBI) and ZJLab.
³ Department of Automation of Shanghai Jiao Tong University.
⁴ Shanghai Jiao Tong University.
⁵ Hong Kong Polytechnic University.
⁶ School of Biotechnology and Key Laboratory of Industrial Biotechnology Ministry in Jiangnan University.
⁷ School of Artificial Intelligence and Computer Science of Jiangnan University.

PMID: 32808039
DOI: 10.1093/bib/bbaa174

Abstract

RNA-binding protein (RBP) is a class of proteins that bind to and accompany RNAs in regulating biological processes. An RBP may have multiple target RNAs, and its aberrant expression can cause multiple diseases. Methods have been designed to predict whether a specific RBP can bind to an RNA and the position of the binding site using binary classification model. However, most of the existing methods do not take into account the binding similarity and correlation between different RBPs. While methods employing multiple labels and Long Short Term Memory Network (LSTM) are proposed to consider binding similarity between different RBPs, the accuracy remains low due to insufficient feature learning and multi-label learning on RNA sequences. In response to this challenge, the concept of RNA-RBP Binding Network (RRBN) is proposed in this paper to provide theoretical support for multi-label learning to identify RBPs that can bind to RNAs. It is experimentally shown that the RRBN information can significantly improve the prediction of unknown RNA-RBP interactions. To further improve the prediction accuracy, we present the novel computational method iDeepMV which integrates multi-view deep learning technology under the multi-label learning framework. iDeepMV first extracts data from the views of amino acid sequence and dipeptide component based on the RNA sequences as the original view. Deep neural network models are then designed for the respective views to perform deep feature learning. The extracted deep features are fed into multi-label classifiers which are trained with the RNA-RBP interaction information for the three views. Finally, a voting mechanism is designed to make comprehensive decision on the results of the multi-label classifiers. Our experimental results show that the prediction performance of iDeepMV, which combines multi-view deep feature learning models with RNA-RBP interaction information, is significantly better than that of the state-of-the-art methods. iDeepMV is freely available at http://www.csbio.sjtu.edu.cn/bioinf/iDeepMV for academic use. The code is freely available at http://github.com/uchihayht/iDeepMV.

Keywords: multi RNA-binding proteins recognition; multi-label learning; multi-view deep feature learning.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Computational Biology / methods
Machine Learning*
Neural Networks, Computer
RNA-Binding Proteins / metabolism*

Substances

RNA-Binding Proteins