Exploiting a subtype-specific mitochondrial vulnerability for successful treatment of colorectal peritoneal metastases
Bootsma, Sanne; Dings, Mark P.G.; Kesselaar, Job; Helderman, Roxan F.C.P.A.; van Megesen, Kyah; Constantinides, Alexander; Moreno, Leandro Ferreira; Stelloo, Ellen; Scutigliani, Enzo M.; Bokan, Bella; Torang, Arezo; van Hooff, Sander R.; Zwijnenburg, Danny A.; Wouters, Valérie M.; van de Vlasakker, Vincent C.J.; Galanos, Laskarina J.K.; Nijman, Lisanne E.; Logiantara, Adrian; Veenstra, Veronique L.; Schlingemann, Sophie; van Piggelen, Sterre; van der Wel, Nicole; Krawczyk, Przemek M.; Platteeuw, Johannes J.; Tuynman, Jurriaan B.; de Hingh, Ignace H.; Klomp, Jan P.G.; Oubrie, Arthur; Snaebjornsson, Petur; Medema, Jan Paul; Oei, Arlene L.; Kranenburg, Onno; Elbers, Clara C.; Lenos, Kristiaan J.; Vermeulen, Louis; Bijlsma, Maarten F.
(2024) Cell Reports Medicine, volume 5, issue 5
(Article)
Abstract
Peritoneal metastases (PMs) from colorectal cancer (CRC) respond poorly to treatment and are associated with unfavorable prognosis. For example, the addition of hyperthermic intraperitoneal chemotherapy (HIPEC) to cytoreductive surgery in resectable patients shows limited benefit, and novel treatments are urgently needed. The majority of CRC-PMs represent the CMS4 molecular subtype
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of CRC, and here we queried the vulnerabilities of this subtype in pharmacogenomic databases to identify novel therapies. This reveals the copper ionophore elesclomol (ES) as highly effective against CRC-PMs. ES exhibits rapid cytotoxicity against CMS4 cells by targeting mitochondria. We find that a markedly reduced mitochondrial content in CMS4 cells explains their vulnerability to ES. ES demonstrates efficacy in preclinical models of PMs, including CRC-PMs and ovarian cancer organoids, mouse models, and a HIPEC rat model of PMs. The above proposes ES as a promising candidate for the local treatment of CRC-PMs, with broader implications for other PM-prone cancers.
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Keywords: copper, elesclomol, HIPEC, mesenchymal cancer cell, mitochondria, molecular subtype, oxidative phosphorylation, peritoneal metastases, General Biochemistry,Genetics and Molecular Biology
ISSN: 2666-3791
Publisher: Cell Press
Note: Publisher Copyright: © 2024 The Authors
(Peer reviewed)