AI Article Synopsis

  • Predicting how peptides bind to major histocompatibility complex (MHC) is crucial for developing cancer immunotherapies, prompting the creation of the MHCRoBERTa method to improve these predictions using natural language processing (NLP) techniques.
  • The MHCRoBERTa model outperforms existing methods, achieving notable increases in the Spearman rank correlation coefficient (SRCC) and the area under the curve (AUC) values, indicating better prediction accuracy.
  • Furthermore, the model's ability to visualize token representations showcases its understanding of relevant syntax and semantics, making it a valuable tool for identifying potential neoantigens in cancer treatment, and it is available for public use on GitHub.

Article Abstract

Predicting the binding of peptide and major histocompatibility complex (MHC) plays a vital role in immunotherapy for cancer. The success of Alphafold of applying natural language processing (NLP) algorithms in protein secondary struction prediction has inspired us to explore the possibility of NLP methods in predicting peptide-MHC class I binding. Based on the above motivations, we propose the MHCRoBERTa method, RoBERTa pre-training approach, for predicting the binding affinity between type I MHC and peptides. Analysis of the results on benchmark dataset demonstrates that MHCRoBERTa can outperform other state-of-art prediction methods with an increase of the Spearman rank correlation coefficient (SRCC) value. Notably, our model gave a significant improvement on IC50 value. Our method has achieved SRCC value and AUC value as 0.785 and 0.817, respectively. Our SRCC value is 14.3% higher than NetMHCpan3.0 (the second highest SRCC value on pan-specific) and is 3% higher than MHCflurry (the second highest SRCC value on all methods). The AUC value is also better than any other pan-specific methods. Moreover, we visualize the multi-head self-attention for the token representation across the layers and heads by this method. Through the analysis of the representation of each layer and head, we can show whether the model has learned the syntax and semantics necessary to perform the prediction task well. All these results demonstrate that our model can accurately predict the peptide-MHC class I binding affinity and that MHCRoBERTa is a powerful tool for screening potential neoantigens for cancer immunotherapy. MHCRoBERTa is available as an open source software at github (https://github.com/FuxuWang/MHCRoBERTa).

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Source
http://dx.doi.org/10.1093/bib/bbab595DOI Listing

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