Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy

Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy

Background Immunotherapy of cancer is successful but tumor regression often is incomplete and followed by escape. Understanding the mechanisms underlying this acquired resistance will aid the development of more effective treatments.Methods We exploited a mouse model where tumor-specific therapeutic...

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Main Authors: Ziena Abdulrahman, Eva Rademaker, Tetje C van der Sluis, Amina F A.S Teunisse, Aart G Jochemsen, Jan Oosting
Format: Article
Language:English
Published: BMJ Publishing Group 2020-07-01
Series:Journal for ImmunoTherapy of Cancer
Online Access:https://jitc.bmj.com/content/8/2/e001326.full
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spelling doaj-520202f95b084831848aa302833ae70b2021-07-13T15:01:09ZengBMJ Publishing GroupJournal for ImmunoTherapy of Cancer2051-14262020-07-018210.1136/jitc-2020-001326Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapyZiena Abdulrahman0Eva Rademaker1Tetje C van der Sluis2Amina F A.S Teunisse3Aart G Jochemsen4Jan Oosting5Aff3 0000000089452978grid.10419.3dDepartment of Medical OncologyOncode Institute, Leiden University Medical Centre PO Box 9600 2300 RC Leiden The Netherlands Pathology, Leiden University Medical Center, Leiden, The NetherlandsImmunohematology and Bloodtransfusion, Leiden Universitair Medisch Centrum, Leiden, The NetherlandsCell and Chemical Biology, Leiden University Medical Center, Leiden, The NetherlandsCell and Chemical Biology, Leiden University Medical Center, Leiden, The NetherlandsPathology, Leiden University Medical Center, Leiden, The NetherlandsBackground Immunotherapy of cancer is successful but tumor regression often is incomplete and followed by escape. Understanding the mechanisms underlying this acquired resistance will aid the development of more effective treatments.Methods We exploited a mouse model where tumor-specific therapeutic vaccination results in tumor regression, followed by local recurrence and resistance. In depth studies on systemic, local and tumor intrinsic changes were performed with flow and mass cytometry, immunohistochemistry, transcriptomics and several perturbation studies with inhibitors or agonistic antibodies in mice. Main findings were recapitulated in vaccinated patients.Results Full tumor regression and cure of tumor-bearing mice is dependent on the magnitude of the vaccine-induced T-cell response. Recurrence of tumors did not involve classical immune escape mechanisms, such as antigen-presentation alterations, immune checkpoint expression, resistance to killing or local immune suppression. However, the recurrent tumors displayed a changed transcriptome with alterations in p53, tumor necrosis factor-α and transforming growth factor-β signaling pathways and they became immunologically cold. Remarkably, ex vivo cell-sorted recurrent tumors, directly reinjected in naïve hosts retained their resistance to vaccination despite a strong infiltration with tumor-specific CD8+ T cells, similar to that of vaccine-responsive tumors. The influx of inflammatory mature myeloid effector cells in the resistant tumors, however, was impaired and this turned out to be the underlying mechanisms as restoration of inflammatory myeloid cell infiltration reinstated the sensitivity of these refractory tumors to vaccination. Notably, impaired myeloid cell infiltration after vaccination was also associated with vaccine resistance in patients.Conclusion An immunotherapy-induced disability of tumor cells to attract innate myeloid effector cells formed a major mechanism underlying immune escape and acquired resistance. These data not only stresses the importance of myeloid effector cells during immunotherapy but also demands for new studies to harness their tumoricidal activities.https://jitc.bmj.com/content/8/2/e001326.full
collection DOAJ
language English
format Article
sources DOAJ
author Ziena Abdulrahman
Eva Rademaker
Tetje C van der Sluis
Amina F A.S Teunisse
Aart G Jochemsen
Jan Oosting
spellingShingle Ziena Abdulrahman
Eva Rademaker
Tetje C van der Sluis
Amina F A.S Teunisse
Aart G Jochemsen
Jan Oosting
Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy
Journal for ImmunoTherapy of Cancer
author_facet Ziena Abdulrahman
Eva Rademaker
Tetje C van der Sluis
Amina F A.S Teunisse
Aart G Jochemsen
Jan Oosting
author_sort Ziena Abdulrahman
title Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy
title_short Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy
title_full Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy
title_fullStr Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy
title_full_unstemmed Lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy
title_sort lack of myeloid cell infiltration as an acquired resistance strategy to immunotherapy
publisher BMJ Publishing Group
series Journal for ImmunoTherapy of Cancer
issn 2051-1426
publishDate 2020-07-01
description Background Immunotherapy of cancer is successful but tumor regression often is incomplete and followed by escape. Understanding the mechanisms underlying this acquired resistance will aid the development of more effective treatments.Methods We exploited a mouse model where tumor-specific therapeutic vaccination results in tumor regression, followed by local recurrence and resistance. In depth studies on systemic, local and tumor intrinsic changes were performed with flow and mass cytometry, immunohistochemistry, transcriptomics and several perturbation studies with inhibitors or agonistic antibodies in mice. Main findings were recapitulated in vaccinated patients.Results Full tumor regression and cure of tumor-bearing mice is dependent on the magnitude of the vaccine-induced T-cell response. Recurrence of tumors did not involve classical immune escape mechanisms, such as antigen-presentation alterations, immune checkpoint expression, resistance to killing or local immune suppression. However, the recurrent tumors displayed a changed transcriptome with alterations in p53, tumor necrosis factor-α and transforming growth factor-β signaling pathways and they became immunologically cold. Remarkably, ex vivo cell-sorted recurrent tumors, directly reinjected in naïve hosts retained their resistance to vaccination despite a strong infiltration with tumor-specific CD8+ T cells, similar to that of vaccine-responsive tumors. The influx of inflammatory mature myeloid effector cells in the resistant tumors, however, was impaired and this turned out to be the underlying mechanisms as restoration of inflammatory myeloid cell infiltration reinstated the sensitivity of these refractory tumors to vaccination. Notably, impaired myeloid cell infiltration after vaccination was also associated with vaccine resistance in patients.Conclusion An immunotherapy-induced disability of tumor cells to attract innate myeloid effector cells formed a major mechanism underlying immune escape and acquired resistance. These data not only stresses the importance of myeloid effector cells during immunotherapy but also demands for new studies to harness their tumoricidal activities.
url https://jitc.bmj.com/content/8/2/e001326.full
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