IGPRED-Multitask: A Deep Learning Model to Predict Protein Secondary Structure, Torsion Angles and Solvent Accessibility
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Date
2023
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Publisher
IEEE Computer Soc
Open Access Color
Green Open Access
No
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No
Abstract
Protein secondary structure, solvent accessibility and torsion angle predictions are preliminary steps to predict 3D structure of a protein. Deep learning approaches have achieved significant improvements in predicting various features of protein structure. In this study, IGPRED-Multitask, a deep learning model with multi task learning architecture based on deep inception network, graph convolutional network and a bidirectional long short-term memory is proposed. Moreover, hyper-parameters of the model are fine-tuned using Bayesian optimization, which is faster and more effective than grid search. The same benchmark test data sets as in the OPUS-TASS paper including TEST2016, TEST2018, CASP12, CASP13, CASPFM, HARD68, CAMEO93, CAMEO93_HARD, as well as the train and validation sets, are used for fair comparison with the literature. Statistically significant improvements are observed in secondary structure prediction on 4 datasets, in phi angle prediction on 2 datasets and in psi angel prediction on 3 datasets compared to the state-of-the-art methods. For solvent accessibility prediction, TEST2016 and TEST2018 datasets are used only to assess the performance of the proposed model.
Description
Gormez, Yasin/0000-0001-8276-2030
ORCID
Keywords
Proteins, Predictive Models, Deep Learning, Solvents, Amino Acids, Recurrent Neural Networks, Feature Extraction, Feature Extraction Or Construction, Machine Learning, Protein Structure Predicition, Bioinformatics, Deep Learning, Deep Learning, Solvents, Proteins, Bayes Theorem, Neural Networks, Computer
Turkish CoHE Thesis Center URL
Fields of Science
0301 basic medicine, 03 medical and health sciences, 0206 medical engineering, 02 engineering and technology
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OpenCitations Citation Count
6
Source
IEEE-Acm Transactions on Computational Biology and Bioinformatics
Volume
20
Issue
2
Start Page
1104
End Page
1113
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CrossRef : 1
Scopus : 5
PubMed : 5
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5
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3
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1
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