Recharacterization of RSL3 reveals that the selenoproteome is a druggable target in colorectal cancer

DeAngelo, Stephen L.; Dziechciarz, Sofia; Solanki, Sumeet; Shin, Myungsun; Zhao, Liang; Balia, Andrii; El-Derany, Marwa O; Das, Nupur K; Castillo, Cristina; Bell, Hannah N; Paulo, Joao A.; Zhang, Yuezhong; Rossiter, Nicholas J; McCulla, Elizabeth C.; He, Jianping; Talukder, Indrani; Schafer, Zachary T.; Neamati, Nouri; Mancias, Joseph D.; Koutmos, Markos; Shah, Yatrik M.

doi:10.1101/2024.03.29.587381

Cited by 2 publications

References 66 publications

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Glutamine-addiction in cisplatin resistant cancer cells is mediated by SLC7A11 and can be targeted with asparaginase therapy

Wang,

Strauss,

Bartek

et al. 2024

Preprint

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Linking disease phenotypes with molecular targets is key to the rational design of treatment interventions. Resistance to the chemotherapeutic cisplatin is one of the major factors limiting the clinical utility of this therapy, which is central to the treatment of a variety of solid malignancies. In this study, we couple the upregulation of a chemoresistant factor, the glutamate-cystine antiporter SLC7A11, with the addiction of cisplatin-resistant cancer cells to extracellular glutamine. In doing so, we thus provide a putative biomarker for this acquired metabolic dependency of chemoresistance. Subsequently, we evaluate various therapeutic strategies to selectively kill SLC7A11highcisplatin-resistant cancer cells, identifying cross-resistance to ferroptosis-inducing compounds and hypersensitivity to glutaminase inhibitor CB-839. We identify enzymatic depletion of extracellular glutamine using the long-standing anti-leukemic therapy asparaginase (ASNase), which possesses glutaminase activity, as a potential approach, and show this can be successfully combined with cisplatin in cell models. In summary, this study mechanistically links an acquired metabolic dependency of chemoresistant cancer cells with a putative biomarker and provides a potentially actionable strategy to target these drug resistant cells warranting further investigation.

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Glutamine-addiction in cisplatin resistant cancer cells is mediated by SLC7A11 and can be targeted with asparaginase therapy

Wang,

Strauss,

Bartek

et al. 2024

Preprint

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Immunometabolism of ferroptosis in the tumor microenvironment

Lupica-Tondo,

Arner,

Mogilenko

et al. 2024

Front. Oncol.

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Ferroptosis is an iron-dependent form of cell death that results from excess lipid peroxidation in cellular membranes. Within the last decade, physiological and pathological roles for ferroptosis have been uncovered in autoimmune diseases, inflammatory conditions, infection, and cancer biology. Excitingly, cancer cell metabolism may be targeted to induce death by ferroptosis in cancers that are resistant to other forms of cell death. Ferroptosis sensitivity is regulated by oxidative stress, lipid metabolism, and iron metabolism, which are all influenced by the tumor microenvironment (TME). Whereas some cancer cell types have been shown to adapt to these stressors, it is not clear how immune cells regulate their sensitivities to ferroptosis. In this review, we discuss the mechanisms of ferroptosis sensitivity in different immune cell subsets, how ferroptosis influences which immune cells infiltrate the TME, and how these interactions can determine epithelial-to-mesenchymal transition (EMT) and metastasis. While much focus has been placed on inducing ferroptosis in cancer cells, these are important considerations for how ferroptosis-modulating strategies impact anti-tumor immunity. From this perspective, we also discuss some promising immunotherapies in the field of ferroptosis and the challenges associated with targeting ferroptosis in specific immune cell populations.

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Recharacterization of RSL3 reveals that the selenoproteome is a druggable target in colorectal cancer

Cited by 2 publications

References 66 publications

Glutamine-addiction in cisplatin resistant cancer cells is mediated by SLC7A11 and can be targeted with asparaginase therapy

Glutamine-addiction in cisplatin resistant cancer cells is mediated by SLC7A11 and can be targeted with asparaginase therapy

Immunometabolism of ferroptosis in the tumor microenvironment

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