Membrane-localized neoantigens predict the efficacy of cancer immunotherapy

Zoe Goldberger; Sylvie Hauert; Kevin Chang; Trevin Kurtanich; Aaron T. Alpar; Grégoire Repond; Yue Wang; Suzana Gomes; Raga Krishnakumar; Prabha Siddarth; Melody A. Swartz; Jeffrey A. Hubbell; Priscilla S. Briquez

doi:10.1016/j.xcrm.2023.101145

Membrane-localized neoantigens predict the efficacy of cancer immunotherapy

Zoe Goldberger, Sylvie Hauert, Kevin Chang, Trevin Kurtanich, Aaron T. Alpar, Grégoire Repond, Yue Wang, Suzana Gomes, Raga Krishnakumar, Prabha Siddarth, Melody A. Swartz, Jeffrey A. Hubbell, Priscilla S. Briquez

Chemical and Biomolecular Engineering

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

Abstract

Immune checkpoint immunotherapy (ICI) can re-activate immune reactions against neoantigens, leading to remarkable remission in cancer patients. Nevertheless, only a minority of patients are responsive to ICI, and approaches for prediction of responsiveness are needed to improve the success of cancer treatments. While the tumor mutational burden (TMB) correlates positively with responsiveness and survival of patients undergoing ICI, the influence of the subcellular localizations of the neoantigens remains unclear. Here, we demonstrate in both a mouse melanoma model and human clinical datasets of 1,722 ICI-treated patients that a high proportion of membrane-localized neoantigens, particularly at the plasma membrane, correlate with responsiveness to ICI therapy and improved overall survival across multiple cancer types. We further show that combining membrane localization and TMB analyses can enhance the predictability of cancer patient response to ICI. Our results may have important implications for establishing future clinical guidelines to direct the choice of treatment toward ICI.

Original language	English (US)
Article number	101145
Journal	Cell Reports Medicine
Volume	4
Issue number	8
DOIs	https://doi.org/10.1016/j.xcrm.2023.101145
State	Published - Aug 15 2023

Keywords

biomarkers
cancer
cell membrane
immunotherapy
neoantigens
tumor mutational burden

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1016/j.xcrm.2023.101145

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title = "Membrane-localized neoantigens predict the efficacy of cancer immunotherapy",

abstract = "Immune checkpoint immunotherapy (ICI) can re-activate immune reactions against neoantigens, leading to remarkable remission in cancer patients. Nevertheless, only a minority of patients are responsive to ICI, and approaches for prediction of responsiveness are needed to improve the success of cancer treatments. While the tumor mutational burden (TMB) correlates positively with responsiveness and survival of patients undergoing ICI, the influence of the subcellular localizations of the neoantigens remains unclear. Here, we demonstrate in both a mouse melanoma model and human clinical datasets of 1,722 ICI-treated patients that a high proportion of membrane-localized neoantigens, particularly at the plasma membrane, correlate with responsiveness to ICI therapy and improved overall survival across multiple cancer types. We further show that combining membrane localization and TMB analyses can enhance the predictability of cancer patient response to ICI. Our results may have important implications for establishing future clinical guidelines to direct the choice of treatment toward ICI.",

keywords = "biomarkers, cancer, cell membrane, immunotherapy, neoantigens, tumor mutational burden",

author = "Zoe Goldberger and Sylvie Hauert and Kevin Chang and Trevin Kurtanich and Alpar, {Aaron T.} and Gr{\'e}goire Repond and Yue Wang and Suzana Gomes and Raga Krishnakumar and Prabha Siddarth and Swartz, {Melody A.} and Hubbell, {Jeffrey A.} and Briquez, {Priscilla S.}",

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year = "2023",

month = aug,

day = "15",

doi = "10.1016/j.xcrm.2023.101145",

language = "English (US)",

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AU - Goldberger, Zoe

AU - Hauert, Sylvie

AU - Chang, Kevin

AU - Kurtanich, Trevin

AU - Alpar, Aaron T.

AU - Repond, Grégoire

AU - Wang, Yue

AU - Gomes, Suzana

AU - Krishnakumar, Raga

AU - Siddarth, Prabha

AU - Swartz, Melody A.

AU - Hubbell, Jeffrey A.

AU - Briquez, Priscilla S.

PY - 2023/8/15

Y1 - 2023/8/15

N2 - Immune checkpoint immunotherapy (ICI) can re-activate immune reactions against neoantigens, leading to remarkable remission in cancer patients. Nevertheless, only a minority of patients are responsive to ICI, and approaches for prediction of responsiveness are needed to improve the success of cancer treatments. While the tumor mutational burden (TMB) correlates positively with responsiveness and survival of patients undergoing ICI, the influence of the subcellular localizations of the neoantigens remains unclear. Here, we demonstrate in both a mouse melanoma model and human clinical datasets of 1,722 ICI-treated patients that a high proportion of membrane-localized neoantigens, particularly at the plasma membrane, correlate with responsiveness to ICI therapy and improved overall survival across multiple cancer types. We further show that combining membrane localization and TMB analyses can enhance the predictability of cancer patient response to ICI. Our results may have important implications for establishing future clinical guidelines to direct the choice of treatment toward ICI.

AB - Immune checkpoint immunotherapy (ICI) can re-activate immune reactions against neoantigens, leading to remarkable remission in cancer patients. Nevertheless, only a minority of patients are responsive to ICI, and approaches for prediction of responsiveness are needed to improve the success of cancer treatments. While the tumor mutational burden (TMB) correlates positively with responsiveness and survival of patients undergoing ICI, the influence of the subcellular localizations of the neoantigens remains unclear. Here, we demonstrate in both a mouse melanoma model and human clinical datasets of 1,722 ICI-treated patients that a high proportion of membrane-localized neoantigens, particularly at the plasma membrane, correlate with responsiveness to ICI therapy and improved overall survival across multiple cancer types. We further show that combining membrane localization and TMB analyses can enhance the predictability of cancer patient response to ICI. Our results may have important implications for establishing future clinical guidelines to direct the choice of treatment toward ICI.

KW - biomarkers

KW - cancer

KW - cell membrane

KW - immunotherapy

KW - neoantigens

KW - tumor mutational burden

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Membrane-localized neoantigens predict the efficacy of cancer immunotherapy

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Keywords

ASJC Scopus subject areas

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