4.6 Article

Explant Modeling of the Immune Environment of Head and Neck Cancer

Journal

FRONTIERS IN ONCOLOGY
Volume 11, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fonc.2021.611365

Keywords

tumor; head and neck cancer; immunotherapy; explant; cytokine; PD1; OX40; CTLA4

Categories

Funding

  1. NCI [R01CA182311, R01CA244142, R01CA208644]
  2. Israel Cancer Association
  3. Israel Science Foundation

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Patients exhibit distinct responses to immunotherapies, even when matched for baseline tumor environments, indicating that the biological response to treatment cannot currently be predicted accurately through snapshot analysis of tumor infiltrates. Further research is needed to better understand the relationship between the immune environment of tumors and responses to therapy.
Patients exhibit distinct responses to immunotherapies that are thought to be linked to their tumor immune environment. However, wide variations in outcomes are also observed in patients with matched baseline tumor environments, indicating that the biological response to treatment is not currently predictable using a snapshot analysis. To investigate the relationship between the immune environment of tumors and the biological response to immunotherapies, we characterized four murine head and neck squamous cell carcinoma (HNSCC) models on two genetic backgrounds. Using tumor explants from those models, we identified correlations between the composition of infiltrating immune cells and baseline cytokine profiles prior to treatment. Following treatment with PD-1 blockade, CTLA-4 blockade, or OX40 stimulation, we observed inter-individual variability in the response to therapy between genetically identical animals bearing the same tumor. These distinct biological responses to treatment were not linked to the initial tumor immune environment, meaning that outcome would not be predictable from a baseline analysis of the tumor infiltrates. We similarly performed the explant assay on patient HNSCC tumors and found significant variability between the baseline environment of the tumors and their response to therapy. We propose that tumor explants provide a rapid biological assay to assess response to candidate immunotherapies that may allow matching therapies to individual patient tumors. Further development of explant approaches may allow screening and monitoring of treatment responses in HNSCC.

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