Personal neoantigen vaccines induce persistent memory T cell responses and epitope spreading in patients with melanoma
Author(s)
Holden, Rebecca Lynn; Pentelute, Bradley L.; Barouch, Dan H.
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© 2021, The Author(s), under exclusive licence to Springer Nature America, Inc. Personal neoantigen vaccines have been envisioned as an effective approach to induce, amplify and diversify antitumor T cell responses. To define the long-term effects of such a vaccine, we evaluated the clinical outcome and circulating immune responses of eight patients with surgically resected stage IIIB/C or IVM1a/b melanoma, at a median of almost 4 years after treatment with NeoVax, a long-peptide vaccine targeting up to 20 personal neoantigens per patient (NCT01970358). All patients were alive and six were without evidence of active disease. We observed long-term persistence of neoantigen-specific T cell responses following vaccination, with ex vivo detection of neoantigen-specific T cells exhibiting a memory phenotype. We also found diversification of neoantigen-specific T cell clones over time, with emergence of multiple T cell receptor clonotypes exhibiting distinct functional avidities. Furthermore, we detected evidence of tumor infiltration by neoantigen-specific T cell clones after vaccination and epitope spreading, suggesting on-target vaccine-induced tumor cell killing. Personal neoantigen peptide vaccines thus induce T cell responses that persist over years and broaden the spectrum of tumor-specific cytotoxicity in patients with melanoma.
Date issued
2021Department
Massachusetts Institute of Technology. Department of Chemistry; Koch Institute for Integrative Cancer Research at MIT; Ragon Institute of MGH, MIT and HarvardJournal
Nature Medicine
Publisher
Springer Science and Business Media LLC
Citation
2021. "Personal neoantigen vaccines induce persistent memory T cell responses and epitope spreading in patients with melanoma." Nature Medicine, 27 (3).
Version: Author's final manuscript