journal contribution
posted on 2025-01-10, 05:27 authored by David Kar Wah LauDavid Kar Wah Lau, D Mouradov, W Wasenang, Ian LukIan Luk, Cameron Scott, David WilliamsDavid Williams, YH Yeung, T Limpaiboon, Georgios Iatropoulos, Laura JenkinsLaura Jenkins, Camilla Marstrander ReehorstCamilla Marstrander Reehorst, Fiona ChionhFiona Chionh, M Nikfarjam, D Croagh, Amardeep Dhillon, Andrew WeickhardtAndrew Weickhardt, T Muramatsu, Y Saito, Niall TebbuttNiall Tebbutt, OM Sieber, John MariadasonJohn Mariadason Biliary tract cancers (BTCs) currently have no approved targeted therapies. Although genomic profiling of primary BTCs has identified multiple potential drug targets, accurate models are needed for their evaluation. Genomic profiling of 22 BTC cell lines revealed they harbor similar mutational signatures, recurrently mutated genes, and genomic alterations to primary tumors. Transcriptomic profiling identified two major subtypes, enriched for epithelial and mesenchymal genes, which were also evident in patient-derived organoids and primary tumors. Interrogating these models revealed multiple mechanisms of MAPK signaling activation in BTC, including co-occurrence of low-activity BRAF and MEK mutations with receptor tyrosine kinase overexpression. Finally, BTC cell lines with altered ERBB2 or FGFRs were exquisitely sensitive to specific targeted agents, whereas surprisingly, IDH1-mutant lines did not respond to IDH1 inhibitors in vitro. These findings establish BTC cell lines as robust models of primary disease, reveal specific molecular disease subsets, and highlight specific molecular vulnerabilities in these cancers.
Funding
This project was supported by the Victorian Cancer Agency (TRP13083), NHMRC Senior Research Fellowships to JMM (1046092) and OMS (1126119), and the Operational Infrastructure Support Program, Victorian Government, Australia. DL, LJ, and GI were supported by La Trobe University Australian Postgraduate Awards, and DL a scholarship from the Pancare Foundation, and GI a scholarship from the Hellenic Society of Medical Oncology. FC was supported by NHMRC Medical Postgraduate Scholarship (1017737), and YHY supported by a Fellowship from the ANZ Trustees Foundation (Brian Smith Endowment).
History
Publication Date
2019-11-22Journal
iScienceVolume
21Pagination
14p. (p. 624-637)Publisher
ElsevierISSN
2589-0042Rights Statement
© 2019 The Author(s).
This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).