A Novel AMPK Inhibitor Sensitizes Pancreatic Cancer Cells to Ferroptosis Induction

Author:

Schneider Carolin1,Hilbert Jorina1,Genevaux Franziska2,Höfer Stefanie3,Krauß Lukas1,Schicktanz Felix4,Contreras Constanza Tapia1,Jansari Shaishavi5,Papargyriou Aristeidis2678,Richter Thorsten1,Alfayomy Abdallah M.910,Falcomatà Chiara1112,Schneeweis Christian11,Orben Felix2,Öllinger Ruppert13,Wegwitz Florian5,Boshnakovska Angela14,Rehling Peter1415,Müller Denise16,Ströbel Philipp161718,Ellenrieder Volker171819,Conradi Lena11718,Hessmann Elisabeth171819,Ghadimi Michael118,Grade Marian118,Wirth Matthias120,Steiger Katja421,Rad Roland1321,Kuster Bernhard321,Sippl Wolfgang9,Reichert Maximilian2782122,Saur Dieter1121,Schneider Günter1111718ORCID

Affiliation:

1. Department of General, Visceral and Pediatric Surgery University Medical Center Göttingen 37075 Göttingen Germany

2. Medical Clinic and Polyclinic II Klinikum rechts der Isar Technical University of Munich 81675 Munich Germany

3. Proteomics and Bioanalytics Department of Molecular Life Sciences School of Life Sciences Technical University of Munich 85354 Freising Germany

4. Institute of Pathology Technical University of Munich 81675 Munich Germany

5. Department of Gynecology and Obstetrics University Medical Center Göttingen Göttingen Germany

6. Institute of Stem Cell Research Helmholtz Zentrum Muenchen D‐85764 Neuherberg Germany

7. Translational Pancreatic Research Cancer Center Medical Clinic and Polyclinic II Klinikum rechts der Isar Technical University of Munich 81675 Munich Germany

8. Center for Organoid Systems (COS) Technical University of Munich 85747 Garching Germany

9. Department of Medicinal Chemistry Institute of Pharmacy Martin‐Luther University Halle‐Wittenberg 06120 Halle (Saale) Germany

10. Department of Pharmaceutical Chemistry Al‐Azhar University Assiut 71524 Egypt

11. Institute for Translational Cancer Research and Experimental Cancer Therapy Technical University Munich 81675 Munich Germany

12. Precision Immunology Institute Icahn School of Medicine at Mount Sinai New York NY USA

13. Institute of Molecular Oncology and Functional Genomics TUM School of Medicine Technical University of Munich 81675 Munich Germany

14. Department of Cellular Biochemistry University Medical Center 37073 Göttingen Germany

15. Max Planck Institute for Biophysical Chemistry 37077 Göttingen Germany

16. Institute of Pathology University Medical Center 37075 Göttingen Germany

17. Clinical Research Unit 5002 KFO5002 University Medical Center Göttingen 37075 Göttingen Germany

18. CCC‐N (Comprehensive Cancer Center Lower Saxony) 37075 Göttingen Germany

19. Department of Gastroenterology Gastrointestinal Oncology and Endocrinology University Medical Center Göttingen 37075 Göttingen Germany

20. Department of Hematology Oncology and Cancer Immunology Campus Benjamin Franklin Charité – Universitätsmedizin Berlin Corporate Member of Freie Universität Berlin and Humboldt‐Universität zu Berlin 12203 Berlin Germany

21. German Cancer Consortium (DKTK) partner site Munich a partnership between DKFZ and University Hospital Klinikum rechts der Isar 81675 München Germany

22. Center for Protein Assemblies (CPA) Technical University of Munich 85747 Garching Germany

Abstract

AbstractCancer cells must develop strategies to adapt to the dynamically changing stresses caused by intrinsic or extrinsic processes, or therapeutic agents. Metabolic adaptability is crucial to mitigate such challenges. Considering metabolism as a central node of adaptability, it is focused on an energy sensor, the AMP‐activated protein kinase (AMPK). In a subtype of pancreatic ductal adenocarcinoma (PDAC) elevated AMPK expression and phosphorylation is identified. Using drug repurposing that combined screening experiments and chemoproteomic affinity profiling, it is identified and characterized PF‐3758309, initially developed as an inhibitor of PAK4, as an AMPK inhibitor. PF‐3758309 shows activity in pre‐clinical PDAC models, including primary patient‐derived organoids. Genetic loss‐of‐function experiments showed that AMPK limits the induction of ferroptosis, and consequently, PF‐3758309 treatment restores the sensitivity toward ferroptosis inducers. The work established a chemical scaffold for the development of specific AMPK‐targeting compounds and deciphered the framework for the development of AMPK inhibitor‐based combination therapies tailored for PDAC.

Funder

Deutsche Krebshilfe

Deutsche Forschungsgemeinschaft

Publisher

Wiley

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