Meta learning for mutant HLA class I epitope immunogenicity prediction to accelerate cancer clinical immunotherapy

Long Xu; Qiang Yang; Weihe Dong; Xiaokun Li; Kuanquan Wang; Suyu Dong; Xianyu Zhang; Tiansong Yang; Gongning Luo; Xingyu Liao; Xin Gao; Guohua Wang

doi:10.1093/bib/bbae625

Meta learning for mutant HLA class I epitope immunogenicity prediction to accelerate cancer clinical immunotherapy

Long Xu
, Qiang Yang
, Weihe Dong
, Xiaokun Li^*
, Kuanquan Wang^*
, Suyu Dong
, Xianyu Zhang
, Tiansong Yang
, Gongning Luo^*
, Xingyu Liao
, Xin Gao
, Guohua Wang^*

^*Corresponding author for this work

School of Computer Science and Technology, Harbin Institute of Technology
School of Medicine and Health, Harbin Institute of Technology
Northeast Forestry University
Heilongjiang University
Ltd.
Shandong Hengxun Technology Co., Ltd.
Harbin Medical University
Heilongjiang University of Traditional Chinese Medicine
King Abdullah University of Science and Technology
Northwestern Polytechnical University Xian

Research output: Contribution to journal › Article › peer-review

8 Scopus citations

Abstract

Accurate prediction of binding between human leukocyte antigen (HLA) class I molecules and antigenic peptide segments is a challenging task and a key bottleneck in personalized immunotherapy for cancer. Although existing prediction tools have demonstrated significant results using established datasets, most can only predict the binding affinity of antigenic peptides to HLA and do not enable the immunogenic interpretation of new antigenic epitopes. This limitation results from the training data for the computational models relying heavily on a large amount of peptide-HLA (pHLA) eluting ligand data, in which most of the candidate epitopes lack immunogenicity. Here, we propose an adaptive immunogenicity prediction model, named MHLAPre, which is trained on the large-scale MS-derived HLA I eluted ligandome (mostly presented by epitopes) that are immunogenic. Allele-specific and pan-allelic prediction models are also provided for endogenous peptide presentation. Using a meta-learning strategy, MHLAPre rapidly assessed HLA class I peptide affinities across the whole pHLA pairs and accurately identified tumor-associated endogenous antigens. During the process of adaptive immune response of T-cells, pHLA-specific binding in the antigen presentation is only a pre-task for CD8+ T-cell recognition. The key factor in activating the immune response is the interaction between pHLA complexes and T-cell receptors (TCRs). Therefore, we performed transfer learning on the pHLA model using the pHLA-TCR dataset. In pHLA binding task, MHLAPre demonstrated significant improvement in identifying neoepitope immunogenicity compared with five state-of-the-art models, proving its effectiveness and robustness. After transfer learning of the pHLA-TCR data, MHLAPre also exhibited relatively superior performance in revealing the mechanism of immunotherapy. MHLAPre is a powerful tool to identify neoepitopes that can interact with TCR and induce immune responses. We believe that the proposed method will greatly contribute to clinical immunotherapy, such as anti-tumor immunity, tumor-specific T-cell engineering, and personalized tumor vaccine.

Original language	English
Article number	bbae625
Journal	Briefings in Bioinformatics
Volume	26
Issue number	1
DOIs	https://doi.org/10.1093/bib/bbae625
State	Published - 1 Jan 2025
Externally published	Yes

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This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

HLA genotyping
deep learning
epitope specificity
immunoinformatics
transfer learning

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10.1093/bib/bbae625

Cite this

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title = "Meta learning for mutant HLA class I epitope immunogenicity prediction to accelerate cancer clinical immunotherapy",

abstract = "Accurate prediction of binding between human leukocyte antigen (HLA) class I molecules and antigenic peptide segments is a challenging task and a key bottleneck in personalized immunotherapy for cancer. Although existing prediction tools have demonstrated significant results using established datasets, most can only predict the binding affinity of antigenic peptides to HLA and do not enable the immunogenic interpretation of new antigenic epitopes. This limitation results from the training data for the computational models relying heavily on a large amount of peptide-HLA (pHLA) eluting ligand data, in which most of the candidate epitopes lack immunogenicity. Here, we propose an adaptive immunogenicity prediction model, named MHLAPre, which is trained on the large-scale MS-derived HLA I eluted ligandome (mostly presented by epitopes) that are immunogenic. Allele-specific and pan-allelic prediction models are also provided for endogenous peptide presentation. Using a meta-learning strategy, MHLAPre rapidly assessed HLA class I peptide affinities across the whole pHLA pairs and accurately identified tumor-associated endogenous antigens. During the process of adaptive immune response of T-cells, pHLA-specific binding in the antigen presentation is only a pre-task for CD8+ T-cell recognition. The key factor in activating the immune response is the interaction between pHLA complexes and T-cell receptors (TCRs). Therefore, we performed transfer learning on the pHLA model using the pHLA-TCR dataset. In pHLA binding task, MHLAPre demonstrated significant improvement in identifying neoepitope immunogenicity compared with five state-of-the-art models, proving its effectiveness and robustness. After transfer learning of the pHLA-TCR data, MHLAPre also exhibited relatively superior performance in revealing the mechanism of immunotherapy. MHLAPre is a powerful tool to identify neoepitopes that can interact with TCR and induce immune responses. We believe that the proposed method will greatly contribute to clinical immunotherapy, such as anti-tumor immunity, tumor-specific T-cell engineering, and personalized tumor vaccine.",

keywords = "HLA genotyping, deep learning, epitope specificity, immunoinformatics, transfer learning",

author = "Long Xu and Qiang Yang and Weihe Dong and Xiaokun Li and Kuanquan Wang and Suyu Dong and Xianyu Zhang and Tiansong Yang and Gongning Luo and Xingyu Liao and Xin Gao and Guohua Wang",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024. Published by Oxford University Press.",

year = "2025",

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doi = "10.1093/bib/bbae625",

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T1 - Meta learning for mutant HLA class I epitope immunogenicity prediction to accelerate cancer clinical immunotherapy

AU - Xu, Long

AU - Yang, Qiang

AU - Dong, Weihe

AU - Li, Xiaokun

AU - Wang, Kuanquan

AU - Dong, Suyu

AU - Zhang, Xianyu

AU - Yang, Tiansong

AU - Luo, Gongning

AU - Liao, Xingyu

AU - Gao, Xin

AU - Wang, Guohua

PY - 2025/1/1

Y1 - 2025/1/1

N2 - Accurate prediction of binding between human leukocyte antigen (HLA) class I molecules and antigenic peptide segments is a challenging task and a key bottleneck in personalized immunotherapy for cancer. Although existing prediction tools have demonstrated significant results using established datasets, most can only predict the binding affinity of antigenic peptides to HLA and do not enable the immunogenic interpretation of new antigenic epitopes. This limitation results from the training data for the computational models relying heavily on a large amount of peptide-HLA (pHLA) eluting ligand data, in which most of the candidate epitopes lack immunogenicity. Here, we propose an adaptive immunogenicity prediction model, named MHLAPre, which is trained on the large-scale MS-derived HLA I eluted ligandome (mostly presented by epitopes) that are immunogenic. Allele-specific and pan-allelic prediction models are also provided for endogenous peptide presentation. Using a meta-learning strategy, MHLAPre rapidly assessed HLA class I peptide affinities across the whole pHLA pairs and accurately identified tumor-associated endogenous antigens. During the process of adaptive immune response of T-cells, pHLA-specific binding in the antigen presentation is only a pre-task for CD8+ T-cell recognition. The key factor in activating the immune response is the interaction between pHLA complexes and T-cell receptors (TCRs). Therefore, we performed transfer learning on the pHLA model using the pHLA-TCR dataset. In pHLA binding task, MHLAPre demonstrated significant improvement in identifying neoepitope immunogenicity compared with five state-of-the-art models, proving its effectiveness and robustness. After transfer learning of the pHLA-TCR data, MHLAPre also exhibited relatively superior performance in revealing the mechanism of immunotherapy. MHLAPre is a powerful tool to identify neoepitopes that can interact with TCR and induce immune responses. We believe that the proposed method will greatly contribute to clinical immunotherapy, such as anti-tumor immunity, tumor-specific T-cell engineering, and personalized tumor vaccine.

AB - Accurate prediction of binding between human leukocyte antigen (HLA) class I molecules and antigenic peptide segments is a challenging task and a key bottleneck in personalized immunotherapy for cancer. Although existing prediction tools have demonstrated significant results using established datasets, most can only predict the binding affinity of antigenic peptides to HLA and do not enable the immunogenic interpretation of new antigenic epitopes. This limitation results from the training data for the computational models relying heavily on a large amount of peptide-HLA (pHLA) eluting ligand data, in which most of the candidate epitopes lack immunogenicity. Here, we propose an adaptive immunogenicity prediction model, named MHLAPre, which is trained on the large-scale MS-derived HLA I eluted ligandome (mostly presented by epitopes) that are immunogenic. Allele-specific and pan-allelic prediction models are also provided for endogenous peptide presentation. Using a meta-learning strategy, MHLAPre rapidly assessed HLA class I peptide affinities across the whole pHLA pairs and accurately identified tumor-associated endogenous antigens. During the process of adaptive immune response of T-cells, pHLA-specific binding in the antigen presentation is only a pre-task for CD8+ T-cell recognition. The key factor in activating the immune response is the interaction between pHLA complexes and T-cell receptors (TCRs). Therefore, we performed transfer learning on the pHLA model using the pHLA-TCR dataset. In pHLA binding task, MHLAPre demonstrated significant improvement in identifying neoepitope immunogenicity compared with five state-of-the-art models, proving its effectiveness and robustness. After transfer learning of the pHLA-TCR data, MHLAPre also exhibited relatively superior performance in revealing the mechanism of immunotherapy. MHLAPre is a powerful tool to identify neoepitopes that can interact with TCR and induce immune responses. We believe that the proposed method will greatly contribute to clinical immunotherapy, such as anti-tumor immunity, tumor-specific T-cell engineering, and personalized tumor vaccine.

KW - HLA genotyping

KW - deep learning

KW - epitope specificity

KW - immunoinformatics

KW - transfer learning

UR - https://www.scopus.com/pages/publications/85212891823

U2 - 10.1093/bib/bbae625

DO - 10.1093/bib/bbae625

M3 - 文章

C2 - 39656887

AN - SCOPUS:85212891823

SN - 1467-5463

VL - 26

JO - Briefings in Bioinformatics

JF - Briefings in Bioinformatics

IS - 1

M1 - bbae625

ER -

Meta learning for mutant HLA class I epitope immunogenicity prediction to accelerate cancer clinical immunotherapy

Abstract

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Keywords

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