Identification of a CD8+ T-cell response to a predicted neoantigen in malignant mesothelioma

Neoantigens present unique and specific targets for personalized cancer immunotherapy strategies. Given the low mutational burden yet immunotherapy responsiveness of malignant mesothelioma (MM) when compared to other carcinogen-induced malignancies, identifying candidate neoantigens and T cells that...

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Veröffentlicht in:	Oncoimmunology 2020-01, Vol.9 (1), p.1684713
Hauptverfasser:	Sneddon, Sophie, Rive, Craig M., Ma, Shaokang, Dick, Ian M., Allcock, Richard J. N., Brown, Scott D., Holt, Robert A., Watson, Mark, Leary, Shay, Lee, Y. C. Gary, Robinson, Bruce W. S., Creaney, Jenette
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Sprache:	eng
Schlagworte:	Antigens, Neoplasm - genetics CD8-Positive T-Lymphocytes - immunology Humans Immunotherapy Malignant mesothelioma Mesothelioma, Malignant - immunology neoantigen Original Research pleural effusion Receptors, Cell Surface tumor-immune interface
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creator	Sneddon, Sophie Rive, Craig M. Ma, Shaokang Dick, Ian M. Allcock, Richard J. N. Brown, Scott D. Holt, Robert A. Watson, Mark Leary, Shay Lee, Y. C. Gary Robinson, Bruce W. S. Creaney, Jenette
description	Neoantigens present unique and specific targets for personalized cancer immunotherapy strategies. Given the low mutational burden yet immunotherapy responsiveness of malignant mesothelioma (MM) when compared to other carcinogen-induced malignancies, identifying candidate neoantigens and T cells that recognize them has been a challenge. We used pleural effusions to gain access to MM tumor cells as well as immune cells in order to characterize the tumor-immune interface in MM. We characterized the landscape of potential neoantigens from SNVs identified in 27 MM patients and performed whole transcriptome sequencing of cell populations from 18 patient-matched pleural effusions. IFNγ ELISpot was performed to detect a CD8+ T cell responses to predicted neoantigens in one patient. We detected a median of 68 (range 7-258) predicted neoantigens across the samples. Wild-type non-binding to mutant binding predicted neoantigens increased risk of death in a model adjusting for age, sex, smoking status, histology and treatment (HR: 33.22, CI: 2.55-433.02, p = .007). Gene expression analysis indicated a dynamic immune environment within the pleural effusions. TCR clonotypes increased with predicted neoantigen burden. A strong activated CD8+ T-cell response was identified for a predicted neoantigen produced by a spontaneous mutation in the ROBO3 gene. Despite the challenges associated with the identification of bonafide neoantigens, there is growing evidence that these molecular changes can provide an actionable target for personalized therapeutics in difficult to treat cancers. Our findings support the existence of candidate neoantigens in MM despite the low mutation burden of the tumor, and may present improved treatment opportunities for patients.
doi_str_mv	10.1080/2162402X.2019.1684713
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We characterized the landscape of potential neoantigens from SNVs identified in 27 MM patients and performed whole transcriptome sequencing of cell populations from 18 patient-matched pleural effusions. IFNγ ELISpot was performed to detect a CD8+ T cell responses to predicted neoantigens in one patient. We detected a median of 68 (range 7-258) predicted neoantigens across the samples. Wild-type non-binding to mutant binding predicted neoantigens increased risk of death in a model adjusting for age, sex, smoking status, histology and treatment (HR: 33.22, CI: 2.55-433.02, p = .007). Gene expression analysis indicated a dynamic immune environment within the pleural effusions. TCR clonotypes increased with predicted neoantigen burden. A strong activated CD8+ T-cell response was identified for a predicted neoantigen produced by a spontaneous mutation in the ROBO3 gene. 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Our findings support the existence of candidate neoantigens in MM despite the low mutation burden of the tumor, and may present improved treatment opportunities for patients.</description><subject>Antigens, Neoplasm - genetics</subject><subject>CD8-Positive T-Lymphocytes - immunology</subject><subject>Humans</subject><subject>Immunotherapy</subject><subject>Malignant mesothelioma</subject><subject>Mesothelioma, Malignant - immunology</subject><subject>neoantigen</subject><subject>Original Research</subject><subject>pleural effusion</subject><subject>Receptors, Cell Surface</subject><subject>tumor-immune interface</subject><issn>2162-4011</issn><issn>2162-402X</issn><issn>2162-402X</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2020</creationdate><recordtype>article</recordtype><sourceid>0YH</sourceid><sourceid>EIF</sourceid><sourceid>DOA</sourceid><recordid>eNp9kUtrGzEUhYfS0oQkPyFF-zKO3o9NaXHb1BDoxosuAkLWXDkKM5KRpg3595XjxDSbaiNxzz3fRfd03SXBC4I1vqJEUo7prwXFxCyI1FwR9qY73df7vfD2-CbkpLuo9R63I7GQzLzvThjFmFKjT7vb1QBpjiF6N8ecUA7IoeVX_RGtew_jiArUXU4V0JybsiswRD_DgBJk14xbSCgmNLkxblMroAlqnu9gjHly59274MYKF8_3Wbf-_m29_NHf_LxeLb_c9F5oOfcbplVQIpjBS4x5-07gChzj2g9CqBC4o96owMmGSiwNaGeUFwyoIVwIdtatDtghu3u7K3Fy5dFmF-1TIZetdWWOfgTrhGdSybYwaFTPNWWYcMOU4ZphkI316cDa_d5MMPi2nOLGV9DXSop3dpv_WGmE4Qw3gDgAfMm1FghHL8F2H559Cc_uw7PP4TXfh38HH10vUbWGz4eGmEIuk3vIZRzs7B7HXEJxycdq2f9n_AV7KaiX</recordid><startdate>20200101</startdate><enddate>20200101</enddate><creator>Sneddon, Sophie</creator><creator>Rive, Craig M.</creator><creator>Ma, Shaokang</creator><creator>Dick, Ian M.</creator><creator>Allcock, Richard J. 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S.</au><au>Creaney, Jenette</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Identification of a CD8+ T-cell response to a predicted neoantigen in malignant mesothelioma</atitle><jtitle>Oncoimmunology</jtitle><addtitle>Oncoimmunology</addtitle><date>2020-01-01</date><risdate>2020</risdate><volume>9</volume><issue>1</issue><spage>1684713</spage><pages>1684713-</pages><issn>2162-4011</issn><issn>2162-402X</issn><eissn>2162-402X</eissn><abstract>Neoantigens present unique and specific targets for personalized cancer immunotherapy strategies. Given the low mutational burden yet immunotherapy responsiveness of malignant mesothelioma (MM) when compared to other carcinogen-induced malignancies, identifying candidate neoantigens and T cells that recognize them has been a challenge. We used pleural effusions to gain access to MM tumor cells as well as immune cells in order to characterize the tumor-immune interface in MM. 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subjects	Antigens, Neoplasm - genetics CD8-Positive T-Lymphocytes - immunology Humans Immunotherapy Malignant mesothelioma Mesothelioma, Malignant - immunology neoantigen Original Research pleural effusion Receptors, Cell Surface tumor-immune interface
title	Identification of a CD8+ T-cell response to a predicted neoantigen in malignant mesothelioma
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