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A therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified T cells

Therapeutic vaccines that augment T cell responses to tumor antigens have been limited by poor potency in clinical trials. In contrast, the transfer of T cells modified with foreign transgenes frequently induces potent endogenous T cell responses to epitopes in the transgene product, and these respo...

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Autores principales: Veatch, Joshua R., Singhi, Naina, Srivastava, Shivani, Szeto, Julia L., Jesernig, Brenda, Stull, Sylvia M., Fitzgibbon, Matthew, Sarvothama, Megha, Yechan-Gunja, Sushma, James, Scott E., Riddell, Stanley R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Clinical Investigation 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8363286/
https://www.ncbi.nlm.nih.gov/pubmed/34396986
http://dx.doi.org/10.1172/JCI144195
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author Veatch, Joshua R.
Singhi, Naina
Srivastava, Shivani
Szeto, Julia L.
Jesernig, Brenda
Stull, Sylvia M.
Fitzgibbon, Matthew
Sarvothama, Megha
Yechan-Gunja, Sushma
James, Scott E.
Riddell, Stanley R.
author_facet Veatch, Joshua R.
Singhi, Naina
Srivastava, Shivani
Szeto, Julia L.
Jesernig, Brenda
Stull, Sylvia M.
Fitzgibbon, Matthew
Sarvothama, Megha
Yechan-Gunja, Sushma
James, Scott E.
Riddell, Stanley R.
author_sort Veatch, Joshua R.
collection PubMed
description Therapeutic vaccines that augment T cell responses to tumor antigens have been limited by poor potency in clinical trials. In contrast, the transfer of T cells modified with foreign transgenes frequently induces potent endogenous T cell responses to epitopes in the transgene product, and these responses are undesirable, because they lead to rejection of the transferred T cells. We sought to harness gene-modified T cells as a vaccine platform and developed cancer vaccines composed of autologous T cells modified with tumor antigens and additional adjuvant signals (Tvax). T cells expressing model antigens and a broad range of tumor neoantigens induced robust and durable T cell responses through cross-presentation of antigens by host DCs. Providing Tvax with signals such as CD80, CD137L, IFN-β, IL-12, GM-CSF, and FLT3L enhanced T cell priming. Coexpression of IL-12 and GM-CSF induced the strongest CD4(+) and CD8(+) T cell responses through complimentary effects on the recruitment and activation of DCs, mediated by autocrine IL-12 receptor signaling in the Tvax. Therapeutic vaccination with Tvax and adjuvants showed antitumor activity in subcutaneous and metastatic preclinical mouse models. Human T cells modified with neoantigens readily activated specific T cells derived from patients, providing a path for clinical translation of this therapeutic platform in cancer.
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spelling pubmed-83632862021-08-19 A therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified T cells Veatch, Joshua R. Singhi, Naina Srivastava, Shivani Szeto, Julia L. Jesernig, Brenda Stull, Sylvia M. Fitzgibbon, Matthew Sarvothama, Megha Yechan-Gunja, Sushma James, Scott E. Riddell, Stanley R. J Clin Invest Research Article Therapeutic vaccines that augment T cell responses to tumor antigens have been limited by poor potency in clinical trials. In contrast, the transfer of T cells modified with foreign transgenes frequently induces potent endogenous T cell responses to epitopes in the transgene product, and these responses are undesirable, because they lead to rejection of the transferred T cells. We sought to harness gene-modified T cells as a vaccine platform and developed cancer vaccines composed of autologous T cells modified with tumor antigens and additional adjuvant signals (Tvax). T cells expressing model antigens and a broad range of tumor neoantigens induced robust and durable T cell responses through cross-presentation of antigens by host DCs. Providing Tvax with signals such as CD80, CD137L, IFN-β, IL-12, GM-CSF, and FLT3L enhanced T cell priming. Coexpression of IL-12 and GM-CSF induced the strongest CD4(+) and CD8(+) T cell responses through complimentary effects on the recruitment and activation of DCs, mediated by autocrine IL-12 receptor signaling in the Tvax. Therapeutic vaccination with Tvax and adjuvants showed antitumor activity in subcutaneous and metastatic preclinical mouse models. Human T cells modified with neoantigens readily activated specific T cells derived from patients, providing a path for clinical translation of this therapeutic platform in cancer. American Society for Clinical Investigation 2021-08-16 2021-08-16 /pmc/articles/PMC8363286/ /pubmed/34396986 http://dx.doi.org/10.1172/JCI144195 Text en © 2021 Veatch et al. https://creativecommons.org/licenses/by/4.0/This work is licensed under the Creative Commons Attribution 4.0 International License. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Veatch, Joshua R.
Singhi, Naina
Srivastava, Shivani
Szeto, Julia L.
Jesernig, Brenda
Stull, Sylvia M.
Fitzgibbon, Matthew
Sarvothama, Megha
Yechan-Gunja, Sushma
James, Scott E.
Riddell, Stanley R.
A therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified T cells
title A therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified T cells
title_full A therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified T cells
title_fullStr A therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified T cells
title_full_unstemmed A therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified T cells
title_short A therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified T cells
title_sort therapeutic cancer vaccine delivers antigens and adjuvants to lymphoid tissues using genetically modified t cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8363286/
https://www.ncbi.nlm.nih.gov/pubmed/34396986
http://dx.doi.org/10.1172/JCI144195
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