Association of Homologous Recombination–DNA Damage Response Gene Mutations with Immune Biomarkers in Gastroesophageal Cancers

Michael Cerniglia; Joanne Xiu; Axel Grothey; Michael J. Pishvaian; Yasmine Baca; Jimmy J. Hwang; John L. Marshall; Ari M. VanderWalde; Anthony F. Shields; Heinz Josef Lenz; W. Michael Korn; Mohamed Salem; Philip A. Philip; Richard M. Goldberg; Jia Zeng; Sunnie S. Kim

doi:10.1158/1535-7163.MCT-20-0879

Association of Homologous Recombination–DNA Damage Response Gene Mutations with Immune Biomarkers in Gastroesophageal Cancers

Michael Cerniglia, Joanne Xiu, Axel Grothey, Michael J. Pishvaian, Yasmine Baca, Jimmy J. Hwang, John L. Marshall, Ari M. VanderWalde, Anthony F. Shields, Heinz Josef Lenz, W. Michael Korn, Mohamed Salem, Philip A. Philip, Richard M. Goldberg, Jia Zeng, Sunnie S. Kim

School of Medicine

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

Abstract

The prevalence of homologous recombination–DNA damage response (HR-DDR) genetic alterations is of therapeutic interest in gastroesophageal cancers. This study is a comprehensive assessment of HR-DDR mutation prevalence across gastroesophageal adenocarcinomas and squamous cell carcinomas. Here we investigate the association of HR-DDR mutations with known predictors for immune-checkpoint inhibition [deficiency in mismatch-repair (dMMRP), tumor mutational burden (TMB), and programmed death ligand 1 (PD-L1)]. We confirmed HR-DDR mutations are present in a subset of gastroesophageal adenocarcinomas (23%) and gastroesophageal squamous cell carcinomas (20%). Biomarker expression of dMMRP (18% vs. 1%) and TMB-high with a cutoff of ≥10 mt/MB (27% vs. 9%) was significantly more prevalent in the DDR-mutated cohort compared with the non-DDR-mutated cohort. Mean combined positive score for PD-L1 in the total adenocarcinoma cohort was significantly higher in the DDR-mutated cohort compared with the non–DDR-mutated cohort (10.1 vs. 5.8). We demonstrated that alterations in ARID1A, BRCA2, PTEN, and ATM are correlated with dMMRP, TMB-high, and increased PD-L1 expression in gastroesophageal adenocarcinomas. Our findings show that a subset of gastroesophageal tumors harbor HR-DDR mutations correlated with established immune biomarkers. By better understanding the relationship between HR-DDR mutations and immune biomarkers, we may be able to develop better immunotherapy combination strategies to target these tumors.

Original language	English (US)
Pages (from-to)	227-236
Number of pages	10
Journal	Molecular cancer therapeutics
Volume	21
Issue number	1
DOIs	https://doi.org/10.1158/1535-7163.MCT-20-0879
State	Published - Jan 2022

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/1535-7163.MCT-20-0879

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Cerniglia, M., Xiu, J., Grothey, A., Pishvaian, M. J., Baca, Y., Hwang, J. J., Marshall, J. L., VanderWalde, A. M., Shields, A. F., Lenz, H. J., Michael Korn, W., Salem, M., Philip, P. A., Goldberg, R. M., Zeng, J., & Kim, S. S. (2022). Association of Homologous Recombination–DNA Damage Response Gene Mutations with Immune Biomarkers in Gastroesophageal Cancers. Molecular cancer therapeutics, 21(1), 227-236. https://doi.org/10.1158/1535-7163.MCT-20-0879

Cerniglia, M, Xiu, J, Grothey, A, Pishvaian, MJ, Baca, Y, Hwang, JJ, Marshall, JL, VanderWalde, AM, Shields, AF, Lenz, HJ, Michael Korn, W, Salem, M, Philip, PA, Goldberg, RM, Zeng, J & Kim, SS 2022, 'Association of Homologous Recombination–DNA Damage Response Gene Mutations with Immune Biomarkers in Gastroesophageal Cancers', Molecular cancer therapeutics, vol. 21, no. 1, pp. 227-236. https://doi.org/10.1158/1535-7163.MCT-20-0879

@article{0ace556e04624890b3330d04d861845b,

title = "Association of Homologous Recombination–DNA Damage Response Gene Mutations with Immune Biomarkers in Gastroesophageal Cancers",

abstract = "The prevalence of homologous recombination–DNA damage response (HR-DDR) genetic alterations is of therapeutic interest in gastroesophageal cancers. This study is a comprehensive assessment of HR-DDR mutation prevalence across gastroesophageal adenocarcinomas and squamous cell carcinomas. Here we investigate the association of HR-DDR mutations with known predictors for immune-checkpoint inhibition [deficiency in mismatch-repair (dMMRP), tumor mutational burden (TMB), and programmed death ligand 1 (PD-L1)]. We confirmed HR-DDR mutations are present in a subset of gastroesophageal adenocarcinomas (23%) and gastroesophageal squamous cell carcinomas (20%). Biomarker expression of dMMRP (18% vs. 1%) and TMB-high with a cutoff of ≥10 mt/MB (27% vs. 9%) was significantly more prevalent in the DDR-mutated cohort compared with the non-DDR-mutated cohort. Mean combined positive score for PD-L1 in the total adenocarcinoma cohort was significantly higher in the DDR-mutated cohort compared with the non–DDR-mutated cohort (10.1 vs. 5.8). We demonstrated that alterations in ARID1A, BRCA2, PTEN, and ATM are correlated with dMMRP, TMB-high, and increased PD-L1 expression in gastroesophageal adenocarcinomas. Our findings show that a subset of gastroesophageal tumors harbor HR-DDR mutations correlated with established immune biomarkers. By better understanding the relationship between HR-DDR mutations and immune biomarkers, we may be able to develop better immunotherapy combination strategies to target these tumors.",

author = "Michael Cerniglia and Joanne Xiu and Axel Grothey and Pishvaian, {Michael J.} and Yasmine Baca and Hwang, {Jimmy J.} and Marshall, {John L.} and VanderWalde, {Ari M.} and Shields, {Anthony F.} and Lenz, {Heinz Josef} and {Michael Korn}, W. and Mohamed Salem and Philip, {Philip A.} and Goldberg, {Richard M.} and Jia Zeng and Kim, {Sunnie S.}",

note = "Funding Information: J. Xiu reports other support from Caris Life Sciences during the conduct of the study. A. Grothey reports grants, personal fees, and nonfinancial support from Bayer and Roche/Genentech, grants and personal fees from Merck, grants from OBI Pharmaceuticals, Boston Biomedicals, Natera, Amgen, and BMS outside the submitted work. M.J. Pishvaian reports personal fees from Merck, Astra Zeneca, Perthera, and Foundation Medicine, other support from Seattle Genetics, Pfizer, Genentech, AbbVie, Tesaro, Novartis, Celldex, Curegenix, BMS, Regeneron, Fibrogen, ARMO, GSK, RenovoRx, Bayer, and Calithera and personal fees and other support from Halozyme outside the submitted work; in addition, M.J. Pishvaian has a patent for Perthera issued to Myself and a patent for AbbVie pending to Myself. J.J. Hwang reports personal fees from Bristol Myers Squibb, Boehringer Ingelheim, Pfizer, Incyte, QED, Eisai, Deciphera, Genentech/Roche, Funding Information: Amgen, and Ipsen outside the submitted work. J.L. Marshall reports personal fees from Caris Life Science outside the submitted work; and Indivumed-Oncology CMO. A.M. VanderWalde reports nonfinancial support from Caris Life Sciences during the conduct of the study; grants from Amgen, personal fees and nonfinancial support from AstraZeneca, personal fees from Bristol Myers Squibb, Roche/Genentech, Caris Life Sciences, Elsevier, Mirati, ConcertAI, and Bayer outside the submitted work. A.F. Shields reports personal fees and other support from Caris Life Sciences outside the submitted work. W. Korn reports personal fees from Merck outside the submitted work; and Caris Life Sciences, employment, stock options, stock ownership. M. Salem reports other support from Taiho, BMS, Merck, AZ/Daiichi Sankyo, and Exelixis during the conduct of the study. R.M. Goldberg reports personal fees from Amgen, Bayer, Astra Zeneca, Merck, Novartis, Genentech, adaptimmune, GlaxoSmithKline, Compass Therapeutics, and GI Therapeutics outside the submitted work. J. Zeng reports personal fees from Caris Life Sciences during the conduct of the study. S.S. Kim reports Astellas, Merck, and Daiichi outside the submitted work. No disclosures were reported by the other authors. Publisher Copyright: 2021 American Association for Cancer Research",

year = "2022",

month = jan,

doi = "10.1158/1535-7163.MCT-20-0879",

language = "English (US)",

volume = "21",

pages = "227--236",

journal = "Molecular Cancer Therapeutics",

issn = "1535-7163",

publisher = "American Association for Cancer Research Inc.",

number = "1",

}

TY - JOUR

T1 - Association of Homologous Recombination–DNA Damage Response Gene Mutations with Immune Biomarkers in Gastroesophageal Cancers

AU - Cerniglia, Michael

AU - Xiu, Joanne

AU - Grothey, Axel

AU - Pishvaian, Michael J.

AU - Baca, Yasmine

AU - Hwang, Jimmy J.

AU - Marshall, John L.

AU - VanderWalde, Ari M.

AU - Shields, Anthony F.

AU - Lenz, Heinz Josef

AU - Michael Korn, W.

AU - Salem, Mohamed

AU - Philip, Philip A.

AU - Goldberg, Richard M.

AU - Zeng, Jia

AU - Kim, Sunnie S.

N1 - Funding Information: J. Xiu reports other support from Caris Life Sciences during the conduct of the study. A. Grothey reports grants, personal fees, and nonfinancial support from Bayer and Roche/Genentech, grants and personal fees from Merck, grants from OBI Pharmaceuticals, Boston Biomedicals, Natera, Amgen, and BMS outside the submitted work. M.J. Pishvaian reports personal fees from Merck, Astra Zeneca, Perthera, and Foundation Medicine, other support from Seattle Genetics, Pfizer, Genentech, AbbVie, Tesaro, Novartis, Celldex, Curegenix, BMS, Regeneron, Fibrogen, ARMO, GSK, RenovoRx, Bayer, and Calithera and personal fees and other support from Halozyme outside the submitted work; in addition, M.J. Pishvaian has a patent for Perthera issued to Myself and a patent for AbbVie pending to Myself. J.J. Hwang reports personal fees from Bristol Myers Squibb, Boehringer Ingelheim, Pfizer, Incyte, QED, Eisai, Deciphera, Genentech/Roche, Funding Information: Amgen, and Ipsen outside the submitted work. J.L. Marshall reports personal fees from Caris Life Science outside the submitted work; and Indivumed-Oncology CMO. A.M. VanderWalde reports nonfinancial support from Caris Life Sciences during the conduct of the study; grants from Amgen, personal fees and nonfinancial support from AstraZeneca, personal fees from Bristol Myers Squibb, Roche/Genentech, Caris Life Sciences, Elsevier, Mirati, ConcertAI, and Bayer outside the submitted work. A.F. Shields reports personal fees and other support from Caris Life Sciences outside the submitted work. W. Korn reports personal fees from Merck outside the submitted work; and Caris Life Sciences, employment, stock options, stock ownership. M. Salem reports other support from Taiho, BMS, Merck, AZ/Daiichi Sankyo, and Exelixis during the conduct of the study. R.M. Goldberg reports personal fees from Amgen, Bayer, Astra Zeneca, Merck, Novartis, Genentech, adaptimmune, GlaxoSmithKline, Compass Therapeutics, and GI Therapeutics outside the submitted work. J. Zeng reports personal fees from Caris Life Sciences during the conduct of the study. S.S. Kim reports Astellas, Merck, and Daiichi outside the submitted work. No disclosures were reported by the other authors. Publisher Copyright: 2021 American Association for Cancer Research

PY - 2022/1

Y1 - 2022/1

N2 - The prevalence of homologous recombination–DNA damage response (HR-DDR) genetic alterations is of therapeutic interest in gastroesophageal cancers. This study is a comprehensive assessment of HR-DDR mutation prevalence across gastroesophageal adenocarcinomas and squamous cell carcinomas. Here we investigate the association of HR-DDR mutations with known predictors for immune-checkpoint inhibition [deficiency in mismatch-repair (dMMRP), tumor mutational burden (TMB), and programmed death ligand 1 (PD-L1)]. We confirmed HR-DDR mutations are present in a subset of gastroesophageal adenocarcinomas (23%) and gastroesophageal squamous cell carcinomas (20%). Biomarker expression of dMMRP (18% vs. 1%) and TMB-high with a cutoff of ≥10 mt/MB (27% vs. 9%) was significantly more prevalent in the DDR-mutated cohort compared with the non-DDR-mutated cohort. Mean combined positive score for PD-L1 in the total adenocarcinoma cohort was significantly higher in the DDR-mutated cohort compared with the non–DDR-mutated cohort (10.1 vs. 5.8). We demonstrated that alterations in ARID1A, BRCA2, PTEN, and ATM are correlated with dMMRP, TMB-high, and increased PD-L1 expression in gastroesophageal adenocarcinomas. Our findings show that a subset of gastroesophageal tumors harbor HR-DDR mutations correlated with established immune biomarkers. By better understanding the relationship between HR-DDR mutations and immune biomarkers, we may be able to develop better immunotherapy combination strategies to target these tumors.

AB - The prevalence of homologous recombination–DNA damage response (HR-DDR) genetic alterations is of therapeutic interest in gastroesophageal cancers. This study is a comprehensive assessment of HR-DDR mutation prevalence across gastroesophageal adenocarcinomas and squamous cell carcinomas. Here we investigate the association of HR-DDR mutations with known predictors for immune-checkpoint inhibition [deficiency in mismatch-repair (dMMRP), tumor mutational burden (TMB), and programmed death ligand 1 (PD-L1)]. We confirmed HR-DDR mutations are present in a subset of gastroesophageal adenocarcinomas (23%) and gastroesophageal squamous cell carcinomas (20%). Biomarker expression of dMMRP (18% vs. 1%) and TMB-high with a cutoff of ≥10 mt/MB (27% vs. 9%) was significantly more prevalent in the DDR-mutated cohort compared with the non-DDR-mutated cohort. Mean combined positive score for PD-L1 in the total adenocarcinoma cohort was significantly higher in the DDR-mutated cohort compared with the non–DDR-mutated cohort (10.1 vs. 5.8). We demonstrated that alterations in ARID1A, BRCA2, PTEN, and ATM are correlated with dMMRP, TMB-high, and increased PD-L1 expression in gastroesophageal adenocarcinomas. Our findings show that a subset of gastroesophageal tumors harbor HR-DDR mutations correlated with established immune biomarkers. By better understanding the relationship between HR-DDR mutations and immune biomarkers, we may be able to develop better immunotherapy combination strategies to target these tumors.

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Association of Homologous Recombination–DNA Damage Response Gene Mutations with Immune Biomarkers in Gastroesophageal Cancers

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