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A robust deep learning workflow to predict CD8 + T-cell epitopes
A robust deep learning workflow to predict CD8 + T-cell epitopes
by Koohy, Hashem , Simmons, Alison , Pinho, Mariana Pereira , Fernandes, Ricardo A. , Lee, Chloe H. , Huh, Jaesung , Buckley, Paul R. , Jang, Myeongjun , Antanaviciute, Agne
in Algorithms / Amino acids / Antigen (tumor-associated) / Antigenic determinants / Antigens / Autoantigens / Autoimmunity / Bioinformatics / Biomedical and Life Sciences / Biomedicine / Cancer / Cancer Research / CD8 antigen / CD8-Positive T-Lymphocytes / CD8 + T-cell epitopes / Cell recognition / Computational immunology / Computer applications / COVID-19 / Datasets / Deep Learning / Drug development / Epitope prediction / Epitopes / Epitopes, T-Lymphocyte / Glioblastoma / Histocompatibility antigen HLA / Human Genetics / Humans / Immune response / Immune system / Immunogenicity / Immunological tolerance / Immunotherapy / Ligands / Lymphocytes T / Major histocompatibility complex / Medical research / Medicine, Experimental / Medicine/Public Health / Metabolomics / Natural language / Pathogens / Peptides / Predictions / Proteins / SARS-CoV-2 / Severe acute respiratory syndrome coronavirus 2 / Systems Biology / T cells / Thymus gland / Transfer learning / Workflow
2023
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A robust deep learning workflow to predict CD8 + T-cell epitopes
by Koohy, Hashem , Simmons, Alison , Pinho, Mariana Pereira , Fernandes, Ricardo A. , Lee, Chloe H. , Huh, Jaesung , Buckley, Paul R. , Jang, Myeongjun , Antanaviciute, Agne
in Algorithms / Amino acids / Antigen (tumor-associated) / Antigenic determinants / Antigens / Autoantigens / Autoimmunity / Bioinformatics / Biomedical and Life Sciences / Biomedicine / Cancer / Cancer Research / CD8 antigen / CD8-Positive T-Lymphocytes / CD8 + T-cell epitopes / Cell recognition / Computational immunology / Computer applications / COVID-19 / Datasets / Deep Learning / Drug development / Epitope prediction / Epitopes / Epitopes, T-Lymphocyte / Glioblastoma / Histocompatibility antigen HLA / Human Genetics / Humans / Immune response / Immune system / Immunogenicity / Immunological tolerance / Immunotherapy / Ligands / Lymphocytes T / Major histocompatibility complex / Medical research / Medicine, Experimental / Medicine/Public Health / Metabolomics / Natural language / Pathogens / Peptides / Predictions / Proteins / SARS-CoV-2 / Severe acute respiratory syndrome coronavirus 2 / Systems Biology / T cells / Thymus gland / Transfer learning / Workflow
2023
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A robust deep learning workflow to predict CD8 + T-cell epitopes
A robust deep learning workflow to predict CD8 + T-cell epitopes
by Koohy, Hashem , Simmons, Alison , Pinho, Mariana Pereira , Fernandes, Ricardo A. , Lee, Chloe H. , Huh, Jaesung , Buckley, Paul R. , Jang, Myeongjun , Antanaviciute, Agne
in Algorithms / Amino acids / Antigen (tumor-associated) / Antigenic determinants / Antigens / Autoantigens / Autoimmunity / Bioinformatics / Biomedical and Life Sciences / Biomedicine / Cancer / Cancer Research / CD8 antigen / CD8-Positive T-Lymphocytes / CD8 + T-cell epitopes / Cell recognition / Computational immunology / Computer applications / COVID-19 / Datasets / Deep Learning / Drug development / Epitope prediction / Epitopes / Epitopes, T-Lymphocyte / Glioblastoma / Histocompatibility antigen HLA / Human Genetics / Humans / Immune response / Immune system / Immunogenicity / Immunological tolerance / Immunotherapy / Ligands / Lymphocytes T / Major histocompatibility complex / Medical research / Medicine, Experimental / Medicine/Public Health / Metabolomics / Natural language / Pathogens / Peptides / Predictions / Proteins / SARS-CoV-2 / Severe acute respiratory syndrome coronavirus 2 / Systems Biology / T cells / Thymus gland / Transfer learning / Workflow
2023

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Mohammed Bin Rashid Library /
Catalogue /
A robust deep learning workflow to predict CD8 + T-cell epitopes
A robust deep learning workflow to predict CD8 + T-cell epitopes
Journal Article

A robust deep learning workflow to predict CD8 + T-cell epitopes

Koohy, Hashem,
Simmons, Alison,
Pinho, Mariana Pereira,
Fernandes, Ricardo A.,
Lee, Chloe H.,
Huh, Jaesung,
Buckley, Paul R.,
Jang, Myeongjun,
Antanaviciute, Agne
2023
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Overview
Background T-cells play a crucial role in the adaptive immune system by triggering responses against cancer cells and pathogens, while maintaining tolerance against self-antigens, which has sparked interest in the development of various T-cell-focused immunotherapies. However, the identification of antigens recognised by T-cells is low-throughput and laborious. To overcome some of these limitations, computational methods for predicting CD8 + T-cell epitopes have emerged. Despite recent developments, most immunogenicity algorithms struggle to learn features of peptide immunogenicity from small datasets, suffer from HLA bias and are unable to reliably predict pathology-specific CD8 + T-cell epitopes. Methods We developed TRAP (T-cell recognition potential of HLA-I presented peptides), a robust deep learning workflow for predicting CD8 + T-cell epitopes from MHC-I presented pathogenic and self-peptides. TRAP uses transfer learning, deep learning architecture and MHC binding information to make context-specific predictions of CD8 + T-cell epitopes. TRAP also detects low-confidence predictions for peptides that differ significantly from those in the training datasets to abstain from making incorrect predictions. To estimate the immunogenicity of pathogenic peptides with low-confidence predictions, we further developed a novel metric, RSAT (relative similarity to autoantigens and tumour-associated antigens), as a complementary to ‘dissimilarity to self’ from cancer studies. Results TRAP was used to identify epitopes from glioblastoma patients as well as SARS-CoV-2 peptides, and it outperformed other algorithms in both cancer and pathogenic settings. TRAP was especially effective at extracting immunogenicity-associated properties from restricted data of emerging pathogens and translating them onto related species, as well as minimising the loss of likely epitopes in imbalanced datasets. We also demonstrated that the novel metric termed RSAT was able to estimate immunogenic of pathogenic peptides of various lengths and species. TRAP implementation is available at: https://github.com/ChloeHJ/TRAP . Conclusions This study presents a novel computational workflow for accurately predicting CD8 + T-cell epitopes to foster a better understanding of antigen-specific T-cell response and the development of effective clinical therapeutics.
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Publisher
BioMed Central,BioMed Central Ltd,Springer Nature B.V,BMC
Subject

Algorithms

/ Amino acids

/ Antigen (tumor-associated)

/ Antigenic determinants

/ Antigens

/ Autoantigens

/ Autoimmunity

/ Bioinformatics

/ Biomedical and Life Sciences

/ Biomedicine

/ Cancer

/ Cancer Research

/ CD8 antigen

/ CD8-Positive T-Lymphocytes

/ CD8 + T-cell epitopes

/ Cell recognition

/ Computational immunology

/ Computer applications

/ COVID-19

/ Datasets

/ Deep Learning

/ Drug development

/ Epitope prediction

/ Epitopes

/ Epitopes, T-Lymphocyte

/ Glioblastoma

/ Histocompatibility antigen HLA

/ Human Genetics

/ Humans

/ Immune response

/ Immune system

/ Immunogenicity

/ Immunological tolerance

/ Immunotherapy

/ Ligands

/ Lymphocytes T

/ Major histocompatibility complex

/ Medical research

/ Medicine, Experimental

/ Medicine/Public Health

/ Metabolomics

/ Natural language

/ Pathogens

/ Peptides

/ Predictions

/ Proteins

/ SARS-CoV-2

/ Severe acute respiratory syndrome coronavirus 2

/ Systems Biology

/ T cells

/ Thymus gland

/ Transfer learning

/ Workflow

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