What question did this study set out to answer?

The study aims to develop patient-derived organoid models of PDAC to evaluate drug response and understand tumor complexity.

May 29, 2026

Next-generation cancer organoids 2.0 in precision cancer medicine: Patient-derived pancreatic ductal adenocarcinoma organoids model to describe drug sensitivity and complexity of tumor biology.

Key Points

The study aims to develop patient-derived organoid models of PDAC to evaluate drug response and understand tumor complexity.
Prospective enrollment of 735 PDAC patients for EUS-guided fine needle biopsy and surgical resection.
Establishment of patient-derived organoid models analyzed through histology, NGS, and HTS drug sensitivity tests.
Assessment of genetic alterations and drug responses through whole exome, genome, and transcriptome sequencing.
PDAC PDOs successfully established from various specimens with high success rates (e.g., 100% from ascites).
HTS drug sensitivity tests showed a clinical correlation with patient chemotherapeutic responses (84.0% to 91.2%).
Transcriptome analysis identified key genes related to drug resistance and early recurrence, providing insights into tumor biology.

Abstract

4221 Background: Organotypic models of patient-specific tumors are revolutionizing our understanding of cancer heterogeneity and its implications for personalized medicine. The study's aims were as follows: 1) to establish a PDAC patient-derived organoid (PDO) model obtained from various PDAC specimens. 2) to find out clinicogenomic factors affecting patients’ outcomes. Methods: The SMC PDAC Cohort Patients were prospectively enrolled and underwent EUS-guided FNB, metastatic sites (such as liver, ascites, lung, and bone), and surgical resection. PDAC PDOs were comprehensively analyzed for histology, next generation sequencing (NGS), and high-throughput screening (HTS) drug sensitivity tests. Results: The 735 PDAC patients were prospectively enrolled in this study. PDAC PDO platform has been trying to establish from the following cancer specimens: ascites, biopsies from bone, liver, lung, and pancreas, or surgical resection. The success rate was as follows according to the source of obtaining site; ascites due to peritoneal seeding (3/3: 100%), bone mets (1/1: 100%), EUS-FNB (195/183: 87.8%), liver mets (7/8: 87.5%), lung mets (1/1: 100%), surgical specimens (394/500: 78.8%) and PDO was successfully established within 8.2±2.6 days. It took approximately 3 weeks to acquire each specimen and generate sufficient PDAC PDOs for the simultaneous HTS drug sensitivity test and NGS. Whole exome or genome sequencing (WES/WGS, n = 357) showed an almost identical concordance between original PDAC tissues and matched PDOs and the increased frequency of genetic alterations in PDOs. The HTS drug sensitivity test (n = 151) revealed the clinical correlation between the PDO response and the actual chemotherapeutic response of the study patients in both palliative and adjuvant in real-world settings (ranging from 84.0~ to 91.2%). In addition, whole transcriptome sequencing (n = 373) identified nab-paclitaxel resistance-associated genes such as ITGB7, ANPEP, and ST3GAL1, and also found early recurrence-related genes including COL2A1, CALB1, and CYP24A1 in the extracellular matrix, calcium signaling, and vitamin D metabolism. Conclusions: The PDAC PDO platform may become a valuable tool for personalized medicine and may give us insights into tumor biology.

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Cite This Study

Park et al. (Wed,) studied this question.

synapsesocial.com/papers/6a192d2dfab5b468c4415fe3 https://doi.org/https://doi.org/10.1200/jco.2026.44.16_suppl.4221

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