Programming a Ferroptosis‐to‐Apoptosis Transition Landscape Revealed Ferroptosis Biomarkers and Repressors for Cancer Therapy

Yaron Vinik; Avi Maimon; Vinay Dubey; Harsha Raj; Ifat Abramovitch; Sergey Malitsky; Maxim Itkin; Avi Ma'ayan; Frank Westermann; Eyal Gottlieb; Eytan Ruppin; Sima Lev

doi:10.1002/advs.202307263

Advanced Science (May 2024)

Programming a Ferroptosis‐to‐Apoptosis Transition Landscape Revealed Ferroptosis Biomarkers and Repressors for Cancer Therapy

Yaron Vinik,
Avi Maimon,
Vinay Dubey,
Harsha Raj,
Ifat Abramovitch,
Sergey Malitsky,
Maxim Itkin,
Avi Ma'ayan,
Frank Westermann,
Eyal Gottlieb,
Eytan Ruppin,
Sima Lev

Affiliations

Yaron Vinik: Molecular Cell Biology Department Weizmann Institute of Science Rehovot 76100 Israel
Avi Maimon: Molecular Cell Biology Department Weizmann Institute of Science Rehovot 76100 Israel
Vinay Dubey: Molecular Cell Biology Department Weizmann Institute of Science Rehovot 76100 Israel
Harsha Raj: Molecular Cell Biology Department Weizmann Institute of Science Rehovot 76100 Israel
Ifat Abramovitch: The Ruth and Bruce Rappaport Faculty of Medicine Technion–Israel Institute of Technology Haifa 3525433 Israel
Sergey Malitsky: Metabolic Profiling Unit Weizmann Institute of Science Rehovot 76100 Israel
Maxim Itkin: Metabolic Profiling Unit Weizmann Institute of Science Rehovot 76100 Israel
Avi Ma'ayan: Department of Pharmacological Sciences Mount Sinai Center for Bioinformatics Icahn School of Medicine at Mount Sinai New York NY 10029 USA
Frank Westermann: Neuroblastoma Genomics German Cancer Research Center (DKFZ) 69120 Heidelberg Germany
Eyal Gottlieb: The Ruth and Bruce Rappaport Faculty of Medicine Technion–Israel Institute of Technology Haifa 3525433 Israel
Eytan Ruppin: Cancer Data Science Laboratory National Cancer Institute National Institutes of Health Bethesda MD 20892 USA
Sima Lev: Molecular Cell Biology Department Weizmann Institute of Science Rehovot 76100 Israel

DOI: https://doi.org/10.1002/advs.202307263
Journal volume & issue: Vol. 11, no. 17
pp. n/a – n/a

Abstract

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Abstract Ferroptosis and apoptosis are key cell‐death pathways implicated in several human diseases including cancer. Ferroptosis is driven by iron‐dependent lipid peroxidation and currently has no characteristic biomarkers or gene signatures. Here a continuous phenotypic gradient between ferroptosis and apoptosis coupled to transcriptomic and metabolomic landscapes is established. The gradual ferroptosis‐to‐apoptosis transcriptomic landscape is used to generate a unique, unbiased transcriptomic predictor, the Gradient Gene Set (GGS), which classified ferroptosis and apoptosis with high accuracy. Further GGS optimization using multiple ferroptotic and apoptotic datasets revealed highly specific ferroptosis biomarkers, which are robustly validated in vitro and in vivo. A subset of the GGS is associated with poor prognosis in breast cancer patients and PDXs and contains different ferroptosis repressors. Depletion of one representative, PDGFA‐assaociated protein 1(PDAP1), is found to suppress basal‐like breast tumor growth in a mouse model. Omics and mechanistic studies revealed that ferroptosis is associated with enhanced lysosomal function, glutaminolysis, and the tricarboxylic acid (TCA) cycle, while its transition into apoptosis is attributed to enhanced endoplasmic reticulum(ER)‐stress and phosphatidylethanolamine (PE)‐to‐phosphatidylcholine (PC) metabolic shift. Collectively, this study highlights molecular mechanisms underlying ferroptosis execution, identified a highly predictive ferroptosis gene signature with prognostic value, ferroptosis versus apoptosis biomarkers, and ferroptosis repressors for breast cancer therapy.

Published in Advanced Science

ISSN: 2198-3844 (Online)
Publisher: Wiley
Country of publisher: Germany
LCC subjects: Science
Website: https://onlinelibrary.wiley.com/journal/21983844

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