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Human primary liver cancer organoids reveal intratumor and interpatient drug response heterogeneity

类有机物 癌症 肝癌 医学 药品 肿瘤异质性 癌细胞 癌症研究 药物反应 肿瘤科 内科学 病理 生物 药理学 遗传学
作者
Ling Li,Hildur Knútsdóttir,Ken Hui,Matthew J. Weiss,Jié He,Benjamin Philosophe,Andrew Cameron,Christopher L. Wolfgang,Timothy M. Pawlik,Gabriel Ghiaur,Andrew J. Ewald,Esteban Mezey,Joel S. Bader,Florin M. Selaru
出处
期刊:JCI insight [American Society for Clinical Investigation]
卷期号:4 (2) 被引量:139
标识
DOI:10.1172/jci.insight.121490
摘要

Liver cancer is the fourth leading cause of cancer-related mortality and is distinguished by a relative paucity of chemotherapy options. It has been hypothesized that intratumor genetic heterogeneity may contribute to the high failure rate of chemotherapy. Here, we evaluated functional heterogeneity in a cohort of primary human liver cancer organoid lines. Each primary human liver cancer surgical specimen was used to generate multiple cancer organoid lines, obtained from distinct regions of the tumor. A total of 27 liver cancer lines were established and tested with 129 cancer drugs, generating 3,483 cell survival data points. We found a rich intratumor, functional (drug response) heterogeneity in our liver cancer patients. Furthermore, we established that the majority of drugs were either ineffective, or effective only in select organoid lines. In contrast, we found that a subset of drugs appeared pan-effective, displaying at least moderate activity in the majority of these cancer organoid lines. These drugs, which are FDA approved for indications other than liver cancers, deserve further consideration as either systemic or local therapeutics. Of note, molecular profiles, obtained for a reduced sample set, did not correlate with the drug response heterogeneity of liver cancer organoid lines. Taken together, these findings lay the foundation for in-depth studies of pan-effective drugs, as well as for functional personalized oncology approaches. Lastly, these functional studies demonstrate the utility of cancer organoid drug testing as part of a drug discovery pipeline.

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