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Mutation position is an important determinant for predicting cancer neoantigens

J Exp Med. 2020-04; 
Capietto AH, Jhunjhunwala S, Pollock SB, Lupardus P, Wong J, Hänsch L, Cevallos J, Chestnut Y, Fernandez A, Lounsbury N, Nozawa T, Singh M, Fan Z, de la Cruz CC, Phung QT, Taraborrelli L, Haley B, Lill JR, Mellman I, Bourgon R, Delamarre L.
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Peptide Synthesis All samples were tested in technical duplicate and/or 3–5 biological replicates in each individual experiment, and 3–11 experiments were performed depending on the mutation. One screening study was outsourced to WuXi (China). Peptide synthesis was performed by New England Peptide, Anaspec, or Genscript (75% purity). Get A Quote

摘要

Tumor-specific mutations can generate neoantigens that drive CD8 T cell responses against cancer. Next-generation sequencing and computational methods have been successfully applied to identify mutations and predict neoantigens. However, only a small fraction of predicted neoantigens are immunogenic. Currently, predicted peptide binding affinity for MHC-I is often the major criterion for prioritizing neoantigens, although little progress has been made toward understanding the precise functional relationship between affinity and immunogenicity. We therefore systematically assessed the immunogenicity of peptides containing single amino acid mutations in mouse tumor models and divided them into two classes of immu... More

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