Author
Listed:
- Dylan Calhoon
(University of Texas Southwestern Medical Center)
- Lingjie Sang
(University of Texas Southwestern Medical Center)
- Fubo Ji
(University of Texas Southwestern Medical Center)
- Divya Bezwada
(University of Texas Southwestern Medical Center)
- Sheng-Chieh Hsu
(University of Texas Southwestern Medical Center)
- Feng Cai
(University of Texas Southwestern Medical Center)
- Nathaniel Kim
(University of Texas Southwestern Medical Center)
- Amrita Basu
(University of Georgia)
- Renfei Wu
(University of Texas Southwestern Medical Center)
- Anastasia Pimentel
(University of Texas Southwestern Medical Center)
- Bailey Brooks
(University of Texas Southwestern Medical Center)
- Konnor La
(The Rockefeller University)
- Ana Paulina Serrano
(University of Texas Southwestern Medical Center)
- Daniel L. Cassidy
(University of Texas Southwestern Medical Center)
- Ling Cai
(University of Texas Southwestern Medical Center
University of Texas Southwestern)
- Vanina Toffessi-Tcheuyap
(University of Texas Southwestern Medical Center
University of Texas Southwestern Medical Center)
- Maryam E. Moussa
(University of Ottawa)
- Winnie Uritboonthai
(The Scripps Research Institute)
- Linh Truc Hoang
(The Scripps Research Institute)
- Meghana Kolli
(University of Texas Southwestern Medical Center)
- Brooklyn Jackson
(University of Texas Southwestern Medical Center
University of Texas Southwestern Medical Center)
- Vitaly Margulis
(University of Texas Southwestern Medical Center)
- Gary Siuzdak
(The Scripps Research Institute)
- James Brugarolas
(University of Texas Southwestern Medical Center
University of Texas Southwestern Medical Center)
- Ian Corbin
(University of Texas Southwestern Medical Center)
- Derek A. Pratt
(University of Ottawa)
- Ryan J. Weiss
(University of Georgia
University of Georgia)
- Ralph J. DeBerardinis
(University of Texas Southwestern Medical Center
University of Texas Southwestern Medical Center)
- Kıvanç Birsoy
(The Rockefeller University)
- Javier Garcia-Bermudez
(University of Texas Southwestern Medical Center)
Abstract
Lipids are essential components of cancer cells due to their structural and signalling roles1. To meet metabolic demands, many cancers take up extracellular lipids2–5; however, how these lipids contribute to cancer growth and progression remains poorly understood. Here, using functional genetic screens, we identify uptake of lipoproteins—the primary mechanism for lipid transport in circulation—as a key determinant of ferroptosis sensitivity in cancer. Lipoprotein supplementation robustly inhibits ferroptosis across diverse cancer types, primarily through the delivery of α-tocopherol (α-toc), the most abundant form of vitamin E in human lipoproteins. Mechanistically, cancer cells take up lipoproteins through a pathway dependent on sulfated glycosaminoglycans (GAGs) linked to cell-surface proteoglycans. Disrupting GAG biosynthesis or acutely degrading surface GAGs reduces lipoprotein uptake, sensitizes cancer cells to ferroptosis and impairs tumour growth in mice. Notably, human clear cell renal cell carcinomas—a lipid-rich malignancy—exhibit elevated levels of chondroitin sulfate and increased lipoprotein-derived α-toc compared with normal kidney tissue. Together, our study establishes lipoprotein uptake as a critical anti-ferroptotic mechanism in cancer and implicates GAG biosynthesis as a therapeutic target.
Suggested Citation
Dylan Calhoon & Lingjie Sang & Fubo Ji & Divya Bezwada & Sheng-Chieh Hsu & Feng Cai & Nathaniel Kim & Amrita Basu & Renfei Wu & Anastasia Pimentel & Bailey Brooks & Konnor La & Ana Paulina Serrano & D, 2025.
"Glycosaminoglycan-driven lipoprotein uptake protects tumours from ferroptosis,"
Nature, Nature, vol. 644(8077), pages 799-808, August.
Handle:
RePEc:nat:nature:v:644:y:2025:i:8077:d:10.1038_s41586-025-09162-0
DOI: 10.1038/s41586-025-09162-0
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