AI Article Synopsis

  • Many methods for identifying neoantigens rely on tumor sequencing paired with bioinformatics, but there's a lack of reference data and clarity on what makes tumor epitopes immunogenic.
  • A global consortium was formed to predict immunogenic epitopes from shared tumor sequencing, leading to the assessment of 608 epitopes for T cell binding in patient samples.
  • A new model for tumor epitope immunogenicity was created, which was able to accurately filter out non-immunogenic peptides and improve prediction performance, providing valuable data for understanding anti-tumor immunity.

Article Abstract

Many approaches to identify therapeutically relevant neoantigens couple tumor sequencing with bioinformatic algorithms and inferred rules of tumor epitope immunogenicity. However, there are no reference data to compare these approaches, and the parameters governing tumor epitope immunogenicity remain unclear. Here, we assembled a global consortium wherein each participant predicted immunogenic epitopes from shared tumor sequencing data. 608 epitopes were subsequently assessed for T cell binding in patient-matched samples. By integrating peptide features associated with presentation and recognition, we developed a model of tumor epitope immunogenicity that filtered out 98% of non-immunogenic peptides with a precision above 0.70. Pipelines prioritizing model features had superior performance, and pipeline alterations leveraging them improved prediction performance. These findings were validated in an independent cohort of 310 epitopes prioritized from tumor sequencing data and assessed for T cell binding. This data resource enables identification of parameters underlying effective anti-tumor immunity and is available to the research community.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7652061PMC
http://dx.doi.org/10.1016/j.cell.2020.09.015DOI Listing

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