Preclinical evidence for anaplastic lymphoma kinase inhibitors as novel therapeutic treatments for cholangiocarcinoma

Kyaw Zwar Myint; Mireia Sueca-Comes; Pamela Collier; Brinda Balasubramanian; Simran Venkatraman; John Gordan; Abed M Zaitoun; Abhik Mukherjee; Arvind Arora; Noppadol Larbcharoensub; Chinnawut Suriyonplengsaeng; Kanokpan Wongprasert; Tavan Janvilisri; Dhanny Gomez; Anna M Grabowska; Rutaiwan Tohtong; David O Bates; Kiren Yacqub-Usman

doi:10.3389/fonc.2023.1184900

Preclinical evidence for anaplastic lymphoma kinase inhibitors as novel therapeutic treatments for cholangiocarcinoma

Front Oncol. 2023 Dec 7:13:1184900. doi: 10.3389/fonc.2023.1184900. eCollection 2023.

Authors

Kyaw Zwar Myint¹, Mireia Sueca-Comes², Pamela Collier², Brinda Balasubramanian¹, Simran Venkatraman¹, John Gordan³, Abed M Zaitoun⁴, Abhik Mukherjee^{2

4}, Arvind Arora^{2

5}, Noppadol Larbcharoensub⁶, Chinnawut Suriyonplengsaeng⁷, Kanokpan Wongprasert⁷, Tavan Janvilisri^{1

8}, Dhanny Gomez⁹, Anna M Grabowska², Rutaiwan Tohtong⁸, David O Bates², Kiren Yacqub-Usman²

Affiliations

¹ Graduate Program in Molecular Medicine, Faculty of Science, Mahidol University, Bangkok, Thailand.
² Division of Cancer and Stem Cells, Biodiscovery Institute, School of Medicine, Biodiscovery Institute, University of Nottingham, Nottingham, United Kingdom.
³ Department of Medicine, University of California, San Francisco, San Francisco, CA, United States.
⁴ Department of Pathology, Nottingham Universities National Health Service (NHS) Hospital Trust, Queens Medical Centre, Nottingham, United Kingdom.
⁵ Department of Medical Oncology, Nottingham Universities National Health Service (NHS) Hospital Trust, Queens Medical Centre, Nottingham, United Kingdom.
⁶ Department of Pathology, Faculty of Medicine Ramathibodi Hospital, Mahidol University, Bangkok, Thailand.
⁷ Department of Anatomy, Faculty of Science, Mahidol University, Bangkok, Thailand.
⁸ Department of Biochemistry, Faculty of Science, Mahidol University, Bangkok, Thailand.
⁹ Department of Hepatobiliary and Pancreatic Surgery, and National Institute of Health Care Research (NIHR) Nottingham Digestive Disease Biomedical Research Unit, University of Nottingham, Nottingham, United Kingdom.

Abstract

Introduction: Bile duct cancer (cholangiocarcinoma, CCA) has a poor prognosis for patients, and despite recent advances in targeted therapies for other cancer types, it is still treated with standard chemotherapy. Anaplastic lymphoma kinase (ALK) has been shown to be a primary driver of disease progression in lung cancer, and ALK inhibitors are effective therapeutics in aberrant ALK-expressing tumors. Aberrant ALK expression has been documented in CCA, but the use of ALK inhibitors has not been investigated. Using CCA cell lines and close-to-patient primary cholangiocarcinoma cells, we investigated the potential for ALK inhibitors in CCA.

Methods: ALK, cMET, and ROS1 expression was determined in CCA patient tissue by immunohistochemistry and digital droplet polymerase chain reaction, and that in cell lines was determined by immunoblot and immunofluorescence. The effect on cell viability and mechanism of action of ALK, cMet, and ROS1 inhibitors was determined in CCA cell lines. To determine whether ceritinib could affect primary CCA cells, tissue was taken from four patients with biliary tract cancer, without ALK rearrangement, mutation, or overexpression, and grown in three-dimensional tumor growth assays in the presence or absence of humanized mesenchymal cells.

Results: ALK and cMet but not ROS were both upregulated in CCA tissues and cell lines. Cell survival was inhibited by crizotinib, a c-met/ALK/ROS inhibitor. To determine the mechanism of this effect, we tested c-Met-specific and ALK/ROS-specific inhibitors, capmatinib and ceritinib, respectively. Whereas capmatinib did not affect cell survival, ceritinib dose-dependently inhibited survival in all cell lines, with IC₅₀ ranging from 1 to 9 µM and co-treatments with gemcitabine and cisplatin further sensitized cells, with IC₅₀ ranging from IC₅₀ 0.60 to 2.32 µM. Ceritinib did not inhibit cMet phosphorylation but did inhibit ALK phosphorylation. ALK was not mutated in any of these cell lines. Only ceritinib inhibited 3D growth of all four patient samples below mean peak serum concentration, in the presence and absence of mesenchymal cells, whereas crizotinib and capmatinib failed to do this. Ceritinib appeared to exert its effect more through autophagy than apoptosis.

Discussion: These results indicate that ceritinib or other ALK/ROS inhibitors could be therapeutically useful in cholangiocarcinoma even in the absence of aberrant ALK/ROS1 expression.

Keywords: Opisthorchis viverrini; anaplastic lymphoma kinase 1; cholangiocarcinoma; cytotoxicity and autophagy; novel therapeutics.

Copyright © 2023 Myint, Sueca-Comes, Collier, Balasubramanian, Venkatraman, Gordan, Zaitoun, Mukherjee, Arora, Larbcharoensub, Suriyonplengsaeng, Wongprasert, Janvilisri, Gomez, Grabowska, Tohtong, Bates and Yacqub-Usman.

Grants and funding

The author(s) declare financial support was received for the research, authorship, and/or publication of this article. This work is supported by the Thailand Research Funds project No. DBG 5980006, the Medical Research Council UK, Newton Fund MR/N01247X/1, Rajavithi Hospital Research Fund, “Young Research development program 2018” from the National Research Council of Thailand (NRCT), and Research Assistantship, Faculty of Graduate Studies, Mahidol University, and Nottingham University NHS trust.