Comparing neoantigen cancer vaccines and immune checkpoint therapy unveils an effective vaccine and anti-TREM2 macrophage-targeting dual therapy

Sunita Keshari; Alexander S. Shavkunov; Qi Miao; Akata Saha; Tomoyuki Minowa; Martina Molgora; Charmelle D. Williams; Mehdi Chaib; Anna M. Highsmith; Josué E. Pineda; Sayan Alekseev; Elise Alspach; Kenneth H. Hu; Marco Colonna; Kristen E. Pauken; Ken Chen; Matthew M. Gubin

doi:10.1016/j.celrep.2024.114875

Comparing neoantigen cancer vaccines and immune checkpoint therapy unveils an effective vaccine and anti-TREM2 macrophage-targeting dual therapy

Sunita Keshari, Alexander S. Shavkunov, Qi Miao, Akata Saha, Tomoyuki Minowa, Martina Molgora, Charmelle D. Williams, Mehdi Chaib, Anna M. Highsmith, Josué E. Pineda, Sayan Alekseev, Elise Alspach, Kenneth H. Hu, Marco Colonna, Kristen E. Pauken, Ken Chen, Matthew M. Gubin

Research output: Contribution to journal › Article › peer-review

Abstract

The goal of therapeutic cancer vaccines and immune checkpoint therapy (ICT) is to promote T cells with anti-tumor capabilities. Here, we compared mutant neoantigen (neoAg) peptide-based vaccines with ICT in preclinical models. NeoAg vaccines induce the most robust expansion of proliferating and stem-like PD-1⁺TCF-1⁺ neoAg-specific CD8 T cells in tumors. Anti-CTLA-4 and/or anti-PD-1 ICT promotes intratumoral TCF-1⁻ neoAg-specific CD8 T cells, although their phenotype depends in part on the specific ICT used. Anti-CTLA-4 also prompts substantial changes to CD4 T cells, including induction of ICOS⁺Bhlhe40⁺ T helper 1 (Th1)-like cells. Although neoAg vaccines or ICTs expand iNOS⁺ macrophages, neoAg vaccines maintain CX3CR1⁺CD206⁺ macrophages expressing the TREM2 receptor, unlike ICT, which suppresses them. TREM2 blockade enhances neoAg vaccine efficacy and is associated with fewer CX3CR1⁺CD206⁺ macrophages and induction of neoAg-specific CD8 T cells. Our findings highlight different mechanisms underlying neoAg vaccines and different forms of ICT and identify combinatorial therapies to enhance neoAg vaccine efficacy.

Original language	English (US)
Article number	114875
Journal	Cell Reports
Volume	43
Issue number	11
DOIs	https://doi.org/10.1016/j.celrep.2024.114875
State	Published - Nov 26 2024

Keywords

CD4 T cells
CP: Cancer
CP: Immunology
TREM2
anti-CTLA-4/anti-PD-1
cancer immunotherapy
combination immunotherapy
immune checkpoint therapy
intratumoral macrophages
neoantigen cancer vaccines
neoantigen-specific CD8 T cells
tumor microenvironment

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1016/j.celrep.2024.114875

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Keshari, S., Shavkunov, A. S., Miao, Q., Saha, A., Minowa, T., Molgora, M., Williams, C. D., Chaib, M., Highsmith, A. M., Pineda, J. E., Alekseev, S., Alspach, E., Hu, K. H., Colonna, M., Pauken, K. E., Chen, K., & Gubin, M. M. (2024). Comparing neoantigen cancer vaccines and immune checkpoint therapy unveils an effective vaccine and anti-TREM2 macrophage-targeting dual therapy. Cell Reports, 43(11), Article 114875. https://doi.org/10.1016/j.celrep.2024.114875

Keshari, S, Shavkunov, AS, Miao, Q, Saha, A, Minowa, T, Molgora, M, Williams, CD, Chaib, M, Highsmith, AM, Pineda, JE, Alekseev, S, Alspach, E, Hu, KH, Colonna, M, Pauken, KE , Chen, K & Gubin, MM 2024, 'Comparing neoantigen cancer vaccines and immune checkpoint therapy unveils an effective vaccine and anti-TREM2 macrophage-targeting dual therapy', Cell Reports, vol. 43, no. 11, 114875. https://doi.org/10.1016/j.celrep.2024.114875

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title = "Comparing neoantigen cancer vaccines and immune checkpoint therapy unveils an effective vaccine and anti-TREM2 macrophage-targeting dual therapy",

abstract = "The goal of therapeutic cancer vaccines and immune checkpoint therapy (ICT) is to promote T cells with anti-tumor capabilities. Here, we compared mutant neoantigen (neoAg) peptide-based vaccines with ICT in preclinical models. NeoAg vaccines induce the most robust expansion of proliferating and stem-like PD-1+TCF-1+ neoAg-specific CD8 T cells in tumors. Anti-CTLA-4 and/or anti-PD-1 ICT promotes intratumoral TCF-1− neoAg-specific CD8 T cells, although their phenotype depends in part on the specific ICT used. Anti-CTLA-4 also prompts substantial changes to CD4 T cells, including induction of ICOS+Bhlhe40+ T helper 1 (Th1)-like cells. Although neoAg vaccines or ICTs expand iNOS+ macrophages, neoAg vaccines maintain CX3CR1+CD206+ macrophages expressing the TREM2 receptor, unlike ICT, which suppresses them. TREM2 blockade enhances neoAg vaccine efficacy and is associated with fewer CX3CR1+CD206+ macrophages and induction of neoAg-specific CD8 T cells. Our findings highlight different mechanisms underlying neoAg vaccines and different forms of ICT and identify combinatorial therapies to enhance neoAg vaccine efficacy.",

keywords = "CD4 T cells, CP: Cancer, CP: Immunology, TREM2, anti-CTLA-4/anti-PD-1, cancer immunotherapy, combination immunotherapy, immune checkpoint therapy, intratumoral macrophages, neoantigen cancer vaccines, neoantigen-specific CD8 T cells, tumor microenvironment",

author = "Sunita Keshari and Shavkunov, {Alexander S.} and Qi Miao and Akata Saha and Tomoyuki Minowa and Martina Molgora and Williams, {Charmelle D.} and Mehdi Chaib and Highsmith, {Anna M.} and Pineda, {Josu{\'e} E.} and Sayan Alekseev and Elise Alspach and Hu, {Kenneth H.} and Marco Colonna and Pauken, {Kristen E.} and Ken Chen and Gubin, {Matthew M.}",

note = "Publisher Copyright: {\textcopyright} 2024 The Author(s)",

year = "2024",

month = nov,

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doi = "10.1016/j.celrep.2024.114875",

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AU - Keshari, Sunita

AU - Shavkunov, Alexander S.

AU - Miao, Qi

AU - Saha, Akata

AU - Minowa, Tomoyuki

AU - Molgora, Martina

AU - Williams, Charmelle D.

AU - Chaib, Mehdi

AU - Highsmith, Anna M.

AU - Pineda, Josué E.

AU - Alekseev, Sayan

AU - Alspach, Elise

AU - Hu, Kenneth H.

AU - Colonna, Marco

AU - Pauken, Kristen E.

AU - Chen, Ken

AU - Gubin, Matthew M.

PY - 2024/11/26

Y1 - 2024/11/26

N2 - The goal of therapeutic cancer vaccines and immune checkpoint therapy (ICT) is to promote T cells with anti-tumor capabilities. Here, we compared mutant neoantigen (neoAg) peptide-based vaccines with ICT in preclinical models. NeoAg vaccines induce the most robust expansion of proliferating and stem-like PD-1+TCF-1+ neoAg-specific CD8 T cells in tumors. Anti-CTLA-4 and/or anti-PD-1 ICT promotes intratumoral TCF-1− neoAg-specific CD8 T cells, although their phenotype depends in part on the specific ICT used. Anti-CTLA-4 also prompts substantial changes to CD4 T cells, including induction of ICOS+Bhlhe40+ T helper 1 (Th1)-like cells. Although neoAg vaccines or ICTs expand iNOS+ macrophages, neoAg vaccines maintain CX3CR1+CD206+ macrophages expressing the TREM2 receptor, unlike ICT, which suppresses them. TREM2 blockade enhances neoAg vaccine efficacy and is associated with fewer CX3CR1+CD206+ macrophages and induction of neoAg-specific CD8 T cells. Our findings highlight different mechanisms underlying neoAg vaccines and different forms of ICT and identify combinatorial therapies to enhance neoAg vaccine efficacy.

AB - The goal of therapeutic cancer vaccines and immune checkpoint therapy (ICT) is to promote T cells with anti-tumor capabilities. Here, we compared mutant neoantigen (neoAg) peptide-based vaccines with ICT in preclinical models. NeoAg vaccines induce the most robust expansion of proliferating and stem-like PD-1+TCF-1+ neoAg-specific CD8 T cells in tumors. Anti-CTLA-4 and/or anti-PD-1 ICT promotes intratumoral TCF-1− neoAg-specific CD8 T cells, although their phenotype depends in part on the specific ICT used. Anti-CTLA-4 also prompts substantial changes to CD4 T cells, including induction of ICOS+Bhlhe40+ T helper 1 (Th1)-like cells. Although neoAg vaccines or ICTs expand iNOS+ macrophages, neoAg vaccines maintain CX3CR1+CD206+ macrophages expressing the TREM2 receptor, unlike ICT, which suppresses them. TREM2 blockade enhances neoAg vaccine efficacy and is associated with fewer CX3CR1+CD206+ macrophages and induction of neoAg-specific CD8 T cells. Our findings highlight different mechanisms underlying neoAg vaccines and different forms of ICT and identify combinatorial therapies to enhance neoAg vaccine efficacy.

KW - CD4 T cells

KW - CP: Cancer

KW - CP: Immunology

KW - TREM2

KW - anti-CTLA-4/anti-PD-1

KW - cancer immunotherapy

KW - combination immunotherapy

KW - immune checkpoint therapy

KW - intratumoral macrophages

KW - neoantigen cancer vaccines

KW - neoantigen-specific CD8 T cells

KW - tumor microenvironment

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AN - SCOPUS:85207807992

SN - 2639-1856

VL - 43

JO - Cell Reports

JF - Cell Reports

IS - 11

M1 - 114875

ER -

Comparing neoantigen cancer vaccines and immune checkpoint therapy unveils an effective vaccine and anti-TREM2 macrophage-targeting dual therapy

Abstract

Keywords

ASJC Scopus subject areas

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