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A New Supervised Over-Sampling Algorithm with Application to Protein-Nucleotide Binding Residue Prediction

Author

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  • Jun Hu
  • Xue He
  • Dong-Jun Yu
  • Xi-Bei Yang
  • Jing-Yu Yang
  • Hong-Bin Shen

Abstract

Protein-nucleotide interactions are ubiquitous in a wide variety of biological processes. Accurately identifying interaction residues solely from protein sequences is useful for both protein function annotation and drug design, especially in the post-genomic era, as large volumes of protein data have not been functionally annotated. Protein-nucleotide binding residue prediction is a typical imbalanced learning problem, where binding residues are extremely fewer in number than non-binding residues. Alleviating the severity of class imbalance has been demonstrated to be a promising means of improving the prediction performance of a machine-learning-based predictor for class imbalance problems. However, little attention has been paid to the negative impact of class imbalance on protein-nucleotide binding residue prediction. In this study, we propose a new supervised over-sampling algorithm that synthesizes additional minority class samples to address class imbalance. The experimental results from protein-nucleotide interaction datasets demonstrate that the proposed supervised over-sampling algorithm can relieve the severity of class imbalance and help to improve prediction performance. Based on the proposed over-sampling algorithm, a predictor, called TargetSOS, is implemented for protein-nucleotide binding residue prediction. Cross-validation tests and independent validation tests demonstrate the effectiveness of TargetSOS. The web-server and datasets used in this study are freely available at http://www.csbio.sjtu.edu.cn/bioinf/TargetSOS/.

Suggested Citation

  • Jun Hu & Xue He & Dong-Jun Yu & Xi-Bei Yang & Jing-Yu Yang & Hong-Bin Shen, 2014. "A New Supervised Over-Sampling Algorithm with Application to Protein-Nucleotide Binding Residue Prediction," PLOS ONE, Public Library of Science, vol. 9(9), pages 1-10, September.
  • Handle: RePEc:plo:pone00:0107676
    DOI: 10.1371/journal.pone.0107676
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