Pancreatic cancer-restricted cryptic antigens are targets for T cell recognition.

抗原 癌症 胰腺癌 生物 计算生物学 癌症研究 免疫学 遗传学
作者
Zackery A. Ely,Zachary Kulstad,Gürcan Günaydın,Sudarsana Addepalli,Eva K Verzani,Marta Casarrubios,Karl R. Clauser,X Wang,Isabelle E Lippincott,Cédric Louvet,Thomas M. Schmitt,Kevin S. Kapner,Miles Agus,Connor J. Hennessey,James M. Cleary,Sine Reker Hadrup,Susan Klaeger,Jennifer Su,Alex M. Jaeger,Brian M. Wolpin
出处
期刊:PubMed 卷期号:388 (6747): eadk3487-eadk3487
标识
DOI:10.1126/science.adk3487
摘要

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 tumoricidal activity against patient-derived pancreatic cancer organoids. These findings demonstrate that pancreatic cancer harbors cancer-restricted ncHLAp that can be recognized by cytotoxic T cells. Future therapeutic strategies for pancreatic cancer, and potentially other solid tumors, may include targeting cryptic antigens.
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