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A conjoined universal helper epitope can unveil antitumor effects of a neoantigen vaccine targeting an MHC class I-restricted neoepitope

npj Vaccines. 2021-01; 
Adam M Swartz, Kendra L Congdon, Smita K Nair, Qi-Jing Li, James E Herndon, Carter M Suryadevara, Katherine A Riccione, Gary E Archer, Pamela K Norberg, Luis A Sanchez-Perez, John H Sampson
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Catalog Peptides … All peptides were synthesized by Genscript. The sequences of all tested SMA560 29mer SLPs, with the mutation at residue 15, are listed in Supplementary Table 1. The peptide sequences used for Lama4 and Alg8 vaccines were QKISFFDGFEVGFNFRTLQPNGLLFYYT and … Get A Quote

摘要

Personalized cancer vaccines targeting neoantigens arising from somatic missense mutations are currently being evaluated for the treatment of various cancers due to their potential to elicit a multivalent, tumor-specific immune response. Several cancers express a low number of neoantigens; in these cases, ensuring the immunotherapeutic potential of each neoantigen-derived epitope (neoepitope) is crucial. In this study, we discovered that therapeutic vaccines targeting immunodominant major histocompatibility complex (MHC) I-restricted neoepitopes require a conjoined helper epitope in order to induce a cytotoxic, neoepitope-specific CD8+ T-cell response. Furthermore, we show that the universally immunogenic helpe... More

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