Integrating artificial intelligence-driven digital pathology and genomics to establish patient-derived organoids as new approach methodologies for drug response in head and neck cancer
Rose Doerfler, Jie Chen, Carl Kim, Joshua D. Smith, Micah Harris, Krishna B. Singh, Brian R. Isett, Rebekah Dadey, Daniel D. Brown, Adrian V. Lee, Xuefeng Wang, Matthew E. Spector, Seungwon Kim, Shaum Sridharan, Kevin J. Contrera, Katelyn Smith, Carly Reeder, Maureen A. Lyons, Jianhua Luo, Silvia Liu, Dan P. Zandberg, Heath D. Skinner, Ioannis K. Zervantonakis, Lazar Vujanović, Robert L. Ferris, Raja R. Seethala, José P. Zevallos, Jason J. Luke, Riyue Bao
Abstract
• PDO system models HPV-negative HNSCC across clinical and demographic backgrounds. • TransferNet-PDO, a novel AI tool, accurately classifies tumor vs. normal PDOs. • PDOs preserve clonal architecture and low-prevalence subclones over time. • PDOs reveal patient-specific drug responses to standard treatment and targeted therapies. • An integrated platform enables scalable precision oncology in HNSCC. Patient-derived organoids (PDOs) emerge as advanced 3D ex vivo New Approach Methodologies (NAM) preclinical models, offering significant advantages over traditional cell lines and monolayer cultures for therapeutic development. In this study, we established PDOs from surgically resected fresh tissues of human papillomavirus (HPV)-negative head and neck squamous cell carcinoma (HNSCC) across anatomical sites, tumor T-categories, and sample types. These PDOs faithfully recapitulate the tumor’s pathology, mutational profile, and drug response. To enable rapid classification of PDO identity, we developed a new convolutional neural network (CNN) model, TransferNet-PDO, which accurately distinguished tumor versus normal PDOs in culture using digital histopathology images (AUC ≥ 0.88). PDOs maintained stable cultures and were cryopreserved between passages 5 and 12. Immunohistochemistry (IHC) staining (PanCK, p63, Cytokeratin 13, Ki67) confirmed squamous phenotype and histologic aggression of the original tumor. For tumors harboring TP53 mutations by whole-exome sequencing (WES), PDOs retained the corresponding p53 functional status as confirmed by IHC (enhanced or loss of protein expression). Somatic mutational landscape revealed that PDOs preserved driver somatic mutations, copy number variations (CNVs), and clonal architecture including low-prevalence subclones. Drug sensitivity assessment of PDOs showed that cisplatin reduced cell viability, whereas cetuximab and lenvatinib had minimal effects. Chemoradiation led to greater tumor organoid killing compared to radiation or chemotherapy alone. This study presents an integrated HNSCC PDO platform combining tissue biobanking, organoid establishment, multiomics characterization, functional drug screening, and AI-driven histopathologic classification, providing a comprehensive and scalable system for translational cancer research.