APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy

Christopher B. Driscoll; Matthew R. Schuelke; Timothy Kottke; Jill M. Thompson; Phonphimon Wongthida; Jason M. Tonne; Amanda L. Huff; Amber Miller; Kevin G. Shim; Amy Molan; Cynthia Wetmore; Peter Selby; Adel Samson; Kevin Harrington; Hardev Pandha; Alan Melcher; Jose S. Pulido; Reuben Harris; Laura Evgin; Richard G. Vile

doi:10.1038/s41467-020-14568-7

APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy

Christopher B. Driscoll
, Matthew R. Schuelke
, Timothy Kottke
, Jill M. Thompson
, Phonphimon Wongthida
, Jason M. Tonne
, Amanda L. Huff
, Amber Miller
, Kevin G. Shim
, Amy Molan
, Cynthia Wetmore
, Peter Selby
, Adel Samson
, Kevin Harrington
, Hardev Pandha
, Alan Melcher
, Jose S. Pulido
, Reuben Harris
, Laura Evgin
, Richard G. Vile

Producción científica: Article › revisión exhaustiva

53 Citas (Scopus)

Resumen

APOBEC3B, an anti-viral cytidine deaminase which induces DNA mutations, has been implicated as a mediator of cancer evolution and therapeutic resistance. Mutational plasticity also drives generation of neoepitopes, which prime anti-tumor T cells. Here, we show that overexpression of APOBEC3B in tumors increases resistance to chemotherapy, but simultaneously heightens sensitivity to immune checkpoint blockade in a murine model of melanoma. However, in the vaccine setting, APOBEC3B-mediated mutations reproducibly generate heteroclitic neoepitopes in vaccine cells which activate de novo T cell responses. These cross react against parental, unmodified tumors and lead to a high rate of cures in both subcutaneous and intra-cranial tumor models. Heteroclitic Epitope Activated Therapy (HEAT) dispenses with the need to identify patient specific neoepitopes and tumor reactive T cells ex vivo. Thus, actively driving a high mutational load in tumor cell vaccines increases their immunogenicity to drive anti-tumor therapy in combination with immune checkpoint blockade.

Idioma original	English (US)
Número de artículo	790
Publicación	Nature communications
Volumen	11
N.º	1
DOI	https://doi.org/10.1038/s41467-020-14568-7
Estado	Published - dic 1 2020
Publicado de forma externa	Sí

ASJC Scopus subject areas

General Chemistry
General Biochemistry, Genetics and Molecular Biology
General Physics and Astronomy

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10.1038/s41467-020-14568-7

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Driscoll, C. B., Schuelke, M. R., Kottke, T., Thompson, J. M., Wongthida, P., Tonne, J. M., Huff, A. L., Miller, A., Shim, K. G., Molan, A., Wetmore, C., Selby, P., Samson, A., Harrington, K., Pandha, H., Melcher, A., Pulido, J. S., Harris, R., Evgin, L., & Vile, R. G. (2020). APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy. Nature communications, 11(1), Artículo 790. https://doi.org/10.1038/s41467-020-14568-7

Driscoll, CB, Schuelke, MR, Kottke, T, Thompson, JM, Wongthida, P, Tonne, JM, Huff, AL, Miller, A, Shim, KG, Molan, A, Wetmore, C, Selby, P, Samson, A, Harrington, K, Pandha, H, Melcher, A, Pulido, JS, Harris, R, Evgin, L & Vile, RG 2020, 'APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy', Nature communications, vol. 11, n.º 1, 790. https://doi.org/10.1038/s41467-020-14568-7

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title = "APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy",

abstract = "APOBEC3B, an anti-viral cytidine deaminase which induces DNA mutations, has been implicated as a mediator of cancer evolution and therapeutic resistance. Mutational plasticity also drives generation of neoepitopes, which prime anti-tumor T cells. Here, we show that overexpression of APOBEC3B in tumors increases resistance to chemotherapy, but simultaneously heightens sensitivity to immune checkpoint blockade in a murine model of melanoma. However, in the vaccine setting, APOBEC3B-mediated mutations reproducibly generate heteroclitic neoepitopes in vaccine cells which activate de novo T cell responses. These cross react against parental, unmodified tumors and lead to a high rate of cures in both subcutaneous and intra-cranial tumor models. Heteroclitic Epitope Activated Therapy (HEAT) dispenses with the need to identify patient specific neoepitopes and tumor reactive T cells ex vivo. Thus, actively driving a high mutational load in tumor cell vaccines increases their immunogenicity to drive anti-tumor therapy in combination with immune checkpoint blockade.",

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AU - Huff, Amanda L.

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AU - Shim, Kevin G.

AU - Molan, Amy

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AU - Samson, Adel

AU - Harrington, Kevin

AU - Pandha, Hardev

AU - Melcher, Alan

AU - Pulido, Jose S.

AU - Harris, Reuben

AU - Evgin, Laura

AU - Vile, Richard G.

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APOBEC3B-mediated corruption of the tumor cell immunopeptidome induces heteroclitic neoepitopes for cancer immunotherapy

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