A human organoid model of aggressive hepatoblastoma for disease modeling and drug testing
Saltsman, James A.; Hammond, William J.; Narayan, Nicole J.C.; Requena, David; Gehart, Helmuth; Lalazar, Gadi; Laquaglia, Michael P.; Clevers, Hans; Simon, Sanford
(2020) Cancers, volume 12, issue 9
(Article)
Abstract
Hepatoblastoma is the most common childhood liver cancer. Although survival has improved significantly over the past few decades, there remains a group of children with aggressive disease who do not respond to current treatment regimens. There is a critical need for novel models to study aggressive hepatoblastoma as research to
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find new treatments is hampered by the small number of laboratory models of the disease. Organoids have emerged as robust models for many diseases, including cancer. We have generated and characterized a novel organoid model of aggressive hepatoblastoma directly from freshly resected patient tumors as a proof of concept for this approach. Hepatoblastoma tumor organoids recapitulate the key elements of patient tumors, including tumor architecture, mutational profile, gene expression patterns, and features of Wnt/β-catenin signaling that are hallmarks of hepatoblastoma pathophysiology. Tumor organoids were successfully used alongside non-tumor liver organoids from the same patient to perform a drug screen using twelve candidate compounds. One drug, JQ1, demonstrated increased destruction of liver organoids from hepatoblastoma tumor tissue relative to organoids from the adjacent non-tumor liver. Our findings suggest that hepatoblastoma organoids could be used for a variety of applications and have the potential to improve treatment options for the subset of hepatoblastoma patients who do not respond to existing treatments.
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Keywords: 3-D culture, Hepatoblastoma, Liver cancer, Oncology, Organoids, Pediatric oncology, Pediatric solid tumor, Pediatrics, Sequencing, Oncology, Cancer Research
ISSN: 2072-6694
Publisher: Multidisciplinary Digital Publishing Institute (MDPI)
Note: Funding Information: Funding: We are grateful for the support of Bear Necessities Pediatric Cancer Foundation (JAS, MSM), The Rally Foundation for Childhood Cancer Research grants 519023 and 401943 (WJH) and the Truth 365 (JAS, SMS), the support of the NIH/NCI grant P50CA210964 (SMS) and NIH/NCI U54CA243126 (SMS), NIH/NCI P30CA008748 (NJC, MPL), NIH/NCATS grants Clinical and Translation Science Awards UL1TR001866 (GL, SMS) and UL1TR000043 (WJH and SMS). We acknowledge the use of the Integrated Genomics Operation Core, funded by the NCI Cancer Center Support Grant (CCSG, P30 CA08748), Cycle for Survival, and the Marie-Josée and Henry R. Kravis Center for Molecular Oncology. We are also grateful for the support and contributions of the patients and caregivers. Funding Information: We are grateful for the support of Bear Necessities Pediatric Cancer Foundation (JAS, MSM), The Rally Foundation for Childhood Cancer Research grants 519023 and 401943 (WJH) and the Truth 365 (JAS, SMS), the support of the NIH/NCI grant P50CA210964 (SMS) and NIH/NCI U54CA243126 (SMS), NIH/NCI P30CA008748 (NJC, MPL), NIH/NCATS grants Clinical and Translation Science Awards UL1TR001866 (GL, SMS) and UL1TR000043 (WJH and SMS). We acknowledge the use of the Integrated Genomics Operation Core, funded by the NCI Cancer Center Support Grant (CCSG, P30 CA08748), Cycle for Survival, and the Marie-Jos?e and Henry R. Kravis Center for Molecular Oncology. We are also grateful for the support and contributions of the patients and caregivers. Publisher Copyright: © 2020 by the authors. Licensee MDPI, Basel, Switzerland.
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