Multiple oestradiol functions inhibit ferroptosis and acute kidney injury

Wulf Tonnus; Francesca Maremonti; Shubhangi Gavali; Marlena Nastassja Schlecht; Florian Gembardt; Alexia Belavgeni; Nadja Leinung; Karolin Flade; Natalie Bethe; Sofia Traikov; Anne Haag; Danny Schilling; Sider Penkov; Melodie Mallais; Christine Gaillet; Claudia Meyer; Melika Katebi; Anushka Ray; Louisa M S Gerhardt; Anne Brucker; Jorunn Naila Becker; Mirela Tmava; Lisa Schlicker; Almut Schulze; Nina Himmerkus; Andrej Shevchenko; Mirko Peitzsch; Uladzimir Barayeu; Sonia Nasi; Juliane Putz; Kenneth S Korach; Joel Neugarten; Ladan Golestaneh; Christian Hugo; Jan Ulrich Becker; Joel M Weinberg; Svenja Lorenz; Bettina Proneth; Marcus Conrad; Eckhard Wolf; Bernd Plietker; Raphaël Rodriguez; Derek A Pratt; Tobias P Dick; Maria Fedorova; Stefan R Bornstein; Andreas Linkermann

doi:10.1038/s41586-025-09389-x

Multiple oestradiol functions inhibit ferroptosis and acute kidney injury

Nature. 2025 Sep;645(8082):1011-1019. doi: 10.1038/s41586-025-09389-x. Epub 2025 Aug 13.

Authors

Wulf Tonnus^#¹, Francesca Maremonti^#², Shubhangi Gavali^#², Marlena Nastassja Schlecht¹, Florian Gembardt², Alexia Belavgeni³, Nadja Leinung², Karolin Flade¹, Natalie Bethe¹, Sofia Traikov^{3

4}, Anne Haag⁵, Danny Schilling^{6

7}, Sider Penkov⁸, Melodie Mallais⁹, Christine Gaillet¹⁰, Claudia Meyer², Melika Katebi², Anushka Ray², Louisa M S Gerhardt², Anne Brucker¹, Jorunn Naila Becker¹, Mirela Tmava¹, Lisa Schlicker¹¹, Almut Schulze¹¹, Nina Himmerkus¹², Andrej Shevchenko⁴, Mirko Peitzsch³, Uladzimir Barayeu¹³, Sonia Nasi¹⁴, Juliane Putz¹⁵, Kenneth S Korach¹⁶, Joel Neugarten¹⁷, Ladan Golestaneh¹⁷, Christian Hugo¹, Jan Ulrich Becker¹⁸, Joel M Weinberg¹⁹, Svenja Lorenz²⁰, Bettina Proneth²⁰, Marcus Conrad²⁰, Eckhard Wolf^{21

22

23}, Bernd Plietker⁵, Raphaël Rodriguez¹⁰, Derek A Pratt⁹, Tobias P Dick^{6

7}, Maria Fedorova⁸, Stefan R Bornstein^{24

25

26

27}, Andreas Linkermann^{28

29

30}

Affiliations

¹ Division of Nephrology, Department of Internal Medicine 3, University Hospital Carl Gustav Carus at the Technische Universität Dresden, Dresden, Germany.
² Department of Medicine V, University Medical Centre Mannheim, University of Heidelberg, Mannheim, Germany.
³ Institute of Clinical Chemistry and Laboratory Medicine, University Hospital Carl Gustav Carus at the Technische Universität Dresden, Dresden, Germany.
⁴ Max Planck Institute of Molecular Cell Biology and Genetics, Dresden, Germany.
⁵ Chair of Organic Chemistry, Technische Universität Dresden, Dresden, Germany.
⁶ Division of Redox Regulation, German Cancer Research Center (DKFZ), DKFZ-ZMBH Alliance, Heidelberg, Germany.
⁷ Faculty of Biosciences, Heidelberg University, Heidelberg, Germany.
⁸ Center of Membrane Biochemistry and Lipid Research, University Hospital and Faculty of Medicine Carl Gustav Carus, Technische Universität Dresden, Dresden, Germany.
⁹ Department of Chemistry and Biomolecular Sciences, University of Ottawa, Ottawa, Ontario, Canada.
¹⁰ Equipe Labellisée Ligue Contre le Cancer, Institut Curie, CNRS, INSERM, PSL Research University, Paris, France.
¹¹ Division of Tumor Metabolism and Microenvironment, German Cancer Research Center (DKFZ), Heidelberg, Germany.
¹² Institute of Physiology, Christian-Albrecht-University Kiel, Kiel, Germany.
¹³ Max Planck Institute for Polymer Research, Mainz, Germany.
¹⁴ Service of Rheumatology, Department of Musculoskeletal Medicine, Centre Hospitalier Universitaire Vaudois, University of Lausanne, Lausanne, Switzerland.
¹⁵ Clinic for Urology, University Hospital Carl Gustav Carus at the Technische Universität Dresden, Dresden, Germany.
¹⁶ Laboratories of Reproductive and Developmental Toxicology, NIEHS, National Institutes of Health, Research Triangle Park, NC, USA.
¹⁷ Renal Division, Montefiore Medical Center, Albert Einstein College of Medicine, New York, NY, USA.
¹⁸ Institute of Pathology, University Hospital of Cologne, Cologne, Germany.
¹⁹ Division for Nephrology, University of Michigan Medical Center, Ann Arbor, MI, USA.
²⁰ Institute of Metabolism and Cell Death, Helmholtz Zentrum München, Neuherberg, Germany.
²¹ Chair for Molecular Animal Breeding and Biotechnology, Gene Center and Department of Veterinary Sciences, LMU Munich, Munich, Germany.
²² Center for Innovative Medical Models (CiMM), LMU Munich, Oberschleißheim, Germany.
²³ German Center for Diabetes Research (DZD), Neuherberg, Germany.
²⁴ Department of Internal Medicine 3, University Hospital Carl Gustav Carus at the Technische Universität Dresden, Dresden, Germany.
²⁵ Diabetes and Nutritional Sciences, King's College London, London, UK.
²⁶ Center for Regenerative Therapies, Technische Universität Dresden, Dresden, Germany.
²⁷ Paul Langerhans Institute Dresden of Helmholtz Centre Munich at University Clinic Carl Gustav Carus of TU Dresden Faculty of Medicine, Dresden, Germany.
²⁸ Department of Medicine V, University Medical Centre Mannheim, University of Heidelberg, Mannheim, Germany. andreas.linkermann@medma.uni-heidelberg.de.
²⁹ Department of Internal Medicine 3, University Hospital Carl Gustav Carus at the Technische Universität Dresden, Dresden, Germany. andreas.linkermann@medma.uni-heidelberg.de.
³⁰ Division of Nephrology, Department of Medicine, Albert Einstein College of Medicine, New York, NY, USA. andreas.linkermann@medma.uni-heidelberg.de.

^# Contributed equally.

Abstract

Acute tubular necrosis mediates acute kidney injury (AKI) and nephron loss¹, the hallmark of end-stage renal disease^2-4. For decades, it has been known that female kidneys are less sensitive to AKI^5,6. Acute tubular necrosis involves dynamic cell death propagation by ferroptosis along the tubular compartment^7,8. Here we demonstrate abrogated ferroptotic cell death propagation in female kidney tubules. 17β-oestradiol establishes an anti-ferroptotic state through non-genomic and genomic mechanisms. These include the potent direct inhibition of ferroptosis by hydroxyoestradiol derivatives, which function as radical trapping antioxidants, are present at high concentrations in kidney tubules and, when exogenously applied, protect male mice from AKI. In cells, the oxidized hydroxyoestradiols are recycled by FSP1^9,10, but FSP1-deficient female mice were not sensitive to AKI. At the genomic level, female ESR1-deficient kidney tubules partially lose their anti-ferroptotic capacity, similar to ovariectomized mice. While ESR1 promotes the anti-ferroptotic hydropersulfide system, male tubules express pro-ferroptotic proteins of the ether lipid pathway which are suppressed by ESR1 in female tissues until menopause. In summary, we identified non-genomic and genomic mechanisms that collectively explain ferroptosis resistance in female tubules and may function as therapeutic targets for male and postmenopausal female individuals.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Acute Kidney Injury* / drug therapy
Acute Kidney Injury* / metabolism
Acute Kidney Injury* / pathology
Acute Kidney Injury* / prevention & control
Animals
Estradiol* / metabolism
Estradiol* / pharmacology
Estrogen Receptor alpha / deficiency
Estrogen Receptor alpha / genetics
Estrogen Receptor alpha / metabolism
Female
Ferroptosis* / drug effects
Humans
Kidney Tubules / cytology
Kidney Tubules / drug effects
Kidney Tubules / metabolism
Kidney Tubules / pathology
Male
Mice
Mice, Inbred C57BL
Ovariectomy

Substances

Estradiol
Estrogen Receptor alpha
Esr1 protein, mouse