Pancreatic cancer–restricted cryptic antigens are targets for T cell recognition

Ely, Zackery A.; Kulstad, Zachary; Günaydın, Gürcan; Addepalli, Sudarsana; Verzani, Eva K.; Casarrubios, Marta; Clauser, Karl R.; Wang, Xilin; Lippincott, Isabelle E; Louvet, Cédric; Schmitt, Thomas M.; Kapner, Kevin S.; Agus, Miles; Hennessey, Connor J.; Cleary, James M.; Hadrup, Sine Reker; Klaeger, Susan; Su, Jennifer; Jaeger, Alex M.; Wolpin, Brian M.; Raghavan, Srivatsan; Smith, Eric L.; Greenberg, Philip D.; Aguirre, Andrew J.; Abelin, Jennifer G.; Carr, Steven A.; Jacks, Tyler; Freed-Pastor, William A.

doi:10.1126/science.adk3487

articleScienceMay 8, 2025Closed access

Pancreatic cancer–restricted cryptic antigens are targets for T cell recognition

ZAZackery A. Ely ZKZachary Kulstad GGGürcan Günaydın SASudarsana Addepalli EKEva K. Verzani

Massachusetts Institute of Technology · Broad Institute · +7 more institutions

PubMed

Indexed incrossrefpubmed

Abstract

Translation of the noncoding genome in cancer can generate cryptic (noncanonical) peptides capable of presentation by human leukocyte antigen class I (HLA-I); however, the cancer specificity and immunogenicity of noncanonical HLA-I-bound peptides (ncHLAp) are incompletely understood. Using high-resolution immunopeptidomics, we discovered that cryptic peptides are abundant in the pancreatic cancer immunopeptidome. Approximately 30% of ncHLAp exhibited cancer-restricted translation, and a substantial subset were shared among patients. Cancer-restricted ncHLAp displayed robust immunogenic potential in a sensitive ex vivo T cell priming platform. ncHLAp-reactive, T cell receptor-redirected T cells exhibited…

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Topics & keywords

Topics

Keywords

Pancreatic cancer
Cytotoxic T cell
Biology
Immunogenicity
Cancer cell
Cancer
Cancer research
Human leukocyte antigen

UN Sustainable Development Goals

Good health and well-being

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