Improving protein domain classification for third-generation sequencing reads using deep learning

With the development of third-generation sequencing (TGS) technologies, people are able to obtain DNA sequences with lengths from 10s to 100s of kb. These long reads allow protein domain annotation without assembly, thus can produce important insights into the biological functions of the underlying...

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Bibliographic Details
Published inBMC genomics Vol. 22; no. 1; p. 251
Main Authors Du, Nan, Shang, Jiayu, Sun, Yanni
Format Journal Article
LanguageEnglish
Published England BioMed Central Ltd 09.04.2021
BioMed Central
BMC
Subjects
Accuracy
Algorithms
Annotations
Artificial neural networks
Classification
Computer applications
Deep Learning
Deoxyribonucleic acid
DNA
DNA sequencing
Error correction
Error correction & detection
Experiments
Genes
Genomes
Genomics
High-Throughput Nucleotide Sequencing
Humans
Identification and classification
Innovations
Machine learning
Methods
Model testing
Neural networks
Nucleotide sequence
Nucleotide sequencing
Protein Domains
Proteins
Reading
Sequence Analysis, DNA
Software
Translations
United States
China
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Summary:With the development of third-generation sequencing (TGS) technologies, people are able to obtain DNA sequences with lengths from 10s to 100s of kb. These long reads allow protein domain annotation without assembly, thus can produce important insights into the biological functions of the underlying data. However, the high error rate in TGS data raises a new challenge to established domain analysis pipelines. The state-of-the-art methods are not optimized for noisy reads and have shown unsatisfactory accuracy of domain classification in TGS data. New computational methods are still needed to improve the performance of domain prediction in long noisy reads. In this work, we introduce ProDOMA, a deep learning model that conducts domain classification for TGS reads. It uses deep neural networks with 3-frame translation encoding to learn conserved features from partially correct translations. In addition, we formulate our problem as an open-set problem and thus our model can reject reads not containing the targeted domains. In the experiments on simulated long reads of protein coding sequences and real TGS reads from the human genome, our model outperforms HMMER and DeepFam on protein domain classification. In summary, ProDOMA is a useful end-to-end protein domain analysis tool for long noisy reads without relying on error correction.
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ISSN:1471-2164
1471-2164
DOI:10.1186/s12864-021-07468-7