Literature DB >> 32142462

DeepAVP: A Dual-Channel Deep Neural Network for Identifying Variable-Length Antiviral Peptides.

Jiawei Li, Yuqian Pu, Jijun Tang, Quan Zou, Fei Guo.   

Abstract

Antiviral peptides (AVPs) have been experimentally verified to block virus into host cells, which have antiviral activity with decapeptide amide. Therefore, utilization of experimentally validated antiviral peptides is a potential alternative strategy for targeting medically important viruses. In this article, we propose a dual-channel deep neural network ensemble method for analyzing variable-length antiviral peptides. The LSTM channel can capture long-term dependencies for effectively studying original variable-length sequence data. The CONV channel can build dynamic neural network for analyzing the local evolution information. Also, our model can fine-tune the substitution matrix for specifically functional peptides. Applying it to a novel experimentally verified dataset, our AVPs predictor, DeepAVP, demonstrates state-of-the-art performance of [Formula: see text] accuracy and 0.85 MCC, which is far better than existing prediction methods for identifying antiviral peptides. Therefore, DeepAVP, web server for predicting the effective AVPs, would make significantly contributions to peptide-based antiviral research.

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Year:  2020        PMID: 32142462     DOI: 10.1109/JBHI.2020.2977091

Source DB:  PubMed          Journal:  IEEE J Biomed Health Inform        ISSN: 2168-2194            Impact factor:   5.772


  22 in total

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4.  Identification of Methicillin-Resistant Staphylococcus Aureus From Methicillin-Sensitive Staphylococcus Aureus and Molecular Characterization in Quanzhou, China.

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5.  6mA-Pred: identifying DNA N6-methyladenine sites based on deep learning.

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Review 7.  Application of Multilayer Network Models in Bioinformatics.

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9.  Discrimination of Thermophilic Proteins and Non-thermophilic Proteins Using Feature Dimension Reduction.

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Review 10.  Recent Advances in Predicting Protein S-Nitrosylation Sites.

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