Patient-derived head and neck cancer organoids allow treatment stratification and serve as a tool for biomarker validation and identification
Millen, Rosemary; De Kort, Willem W B; Koomen, Mandy; van Son, Gijs J F; Gobits, Roán; Penning de Vries, Bas; Begthel, Harry; Zandvliet, Maurice; Doornaert, Patricia; Raaijmakers, Cornelis P J; Geurts, Maarten H; Elias, Sjoerd G; van Es, Robert J J; de Bree, Remco; Devriese, Lot A; Willems, Stefan M; Kranenburg, Onno; Driehuis, Else; Clevers, Hans
(2023) Med (New York, N.Y.), volume 4, issue 5, pp. 290 - 310.e12
(Article)
Abstract
Background: Organoids are in vitro three-dimensional structures that can be grown from patient tissue. Head and neck cancer (HNC) is a collective term used for multiple tumor types including squamous cell carcinomas and salivary gland adenocarcinomas. Methods: Organoids were established from HNC patient tumor tissue and characterized using immunohistochemistry and
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DNA sequencing. Organoids were exposed to chemo- and radiotherapy and a panel of targeted agents. Organoid response was correlated with patient clinical response. CRISPR-Cas9-based gene editing of organoids was applied for biomarker validation. Findings: A HNC biobank consisting of 110 models, including 65 tumor models, was generated. Organoids retained DNA alterations found in HNC. Comparison of organoid and patient response to radiotherapy (primary [n = 6] and adjuvant [n = 15]) indicated potential for guiding treatment options in the adjuvant setting. In organoids, the radio-sensitizing potential of cisplatin and carboplatin could be validated. However, cetuximab conveyed radioprotection in most models. HNC-targeted treatments were tested on 31 models, indicating possible novel treatment options with the potential for treatment stratification in the future. Activating PIK3CA mutations did not predict alpelisib response in organoids. Protein arginine methyltransferase 5 (PRMT5) inhibitors were identified as a potential treatment option for cyclin-dependent kinase inhibitor 2A (CDKN2A) null HNC. Conclusions: Organoids hold potential as a diagnostic tool in personalized medicine for HNC. In vitro organoid response to radiotherapy (RT) showed a trend that mimics clinical response, indicating the predictive potential of patient-derived organoids. Moreover, organoids could be used for biomarker discovery and validation.
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Keywords: 3D models, CRISPR, Foundational research, cancer, head and neck cancer, organoids, patient-derived models, personalised medicine, radiotherapy, targeted therapy, General Medicine
ISSN: 2666-6340
Publisher: Cell Press
Note: Funding Information: We thank Wendy de Leng, Karen Scheidel-Jacobse, Domenico Castigliego, and Gerben Breimer of the Department of Pathology at the University Medical Center Utrecht for their help with immunohistochemistry and HPV testing of samples. We would like to thank UPORT for their support with patient inclusion. We would like to thank Marjolijn Gross, Ingrid Boots, and Masha de Koning-Hoogeboom for their help with organoid irradiation. We thank all patients who participated in this study. We thank Frans Schutgens for his review of the manuscript. This work was supported by an Oncode Institute fund ( Poc 2018-P0003 ), by an award from the Cancer Research UK Grand Challenge ( C6307/A29058 ), and by the Mark Foundation For Cancer Research to the SPECIFICANCER team (H.C. and M.H.G.). Publisher Copyright: © 2023 The Author(s)
(Peer reviewed)