Author
Listed:
- Saymon Tejay
(Department of Medicine, University of Alberta
Cardiovascular Research Institute, University of Alberta
Cancer Research Institute of Northern Alberta, University of Alberta)
- Maria Areli Lorenzana-Carrillo
(Department of Medicine, University of Alberta
Cardiovascular Research Institute, University of Alberta
Cancer Research Institute of Northern Alberta, University of Alberta)
- Guocheng Huang
(Cancer Research Institute of Northern Alberta, University of Alberta
Division of Urology, Department of Surgery, University of Alberta)
- Seyed Amirhossein Tabatabaei Dakhili
(Cardiovascular Research Institute, University of Alberta
Faculty of Pharmacy and Pharmaceutical Sciences, University of Alberta)
- Yuan -Yuan Zhao
(Department of Medicine, University of Alberta
Cardiovascular Research Institute, University of Alberta
Cancer Research Institute of Northern Alberta, University of Alberta)
- Farah Eaton
(Cardiovascular Research Institute, University of Alberta
Faculty of Pharmacy and Pharmaceutical Sciences, University of Alberta)
- Michelle Mendiola Pla
(Department of Surgery, Duke University)
- Dawn E. Bowles
(Department of Surgery, Duke University)
- Adam Kinnaird
(Cancer Research Institute of Northern Alberta, University of Alberta
Division of Urology, Department of Surgery, University of Alberta
University of Alberta)
- D. Ian Paterson
(University of Ottawa Heart Institute, University of Ottawa)
- Edith Pituskin
(Cancer Research Institute of Northern Alberta, University of Alberta
Faculty of Nursing, University of Alberta)
- John R. Ussher
(Cardiovascular Research Institute, University of Alberta
Faculty of Pharmacy and Pharmaceutical Sciences, University of Alberta)
- Evangelos D. Michelakis
(Department of Medicine, University of Alberta
Cardiovascular Research Institute, University of Alberta)
- Gopinath Sutendra
(Department of Medicine, University of Alberta
Cardiovascular Research Institute, University of Alberta
Cancer Research Institute of Northern Alberta, University of Alberta)
Abstract
It is well established tumour cells secrete signalling factors affecting distant normal tissues. What remains unresolved is whether these factors initiate a signalling cascade rendering terminally differentiated cardiomyocytes susceptible to apoptosis, a feature of chemotherapy-induced cardiotoxicity (CIC). Here we show in MANTICORE trial cancer patients, cumulative baseline plasma levels of the nucleoside inosine and its derivative hypoxanthine predict cardiotoxicity. We found the Zn2+ finger transcription factor ZNF281 increases synthesis and release of inosine and hypoxanthine, which bind the A2A receptor on cardiomyocytes, activating CAMKIIδ which phosphorylates the postnatal mRNA splicing factor RBFOX1, resulting in its caspase-dependent degradation. RBFOX1 loss reverts cardiomyocytes to a less mature state with open chromatin and susceptibility to DNA damage, apoptosis or CIC, when treated with DNA intercalating or alkylating anticancer agents. These findings suggest cumulative inosine and hypoxanthine levels may be a biomarker predicting patient susceptibility to DNA damaging anti-cancer agents.
Suggested Citation
Saymon Tejay & Maria Areli Lorenzana-Carrillo & Guocheng Huang & Seyed Amirhossein Tabatabaei Dakhili & Yuan -Yuan Zhao & Farah Eaton & Michelle Mendiola Pla & Dawn E. Bowles & Adam Kinnaird & D. Ian , 2025.
"Tumour initiated purinergic signalling promotes cardiomyocyte RBFOX1 degradation and cardiotoxicity from DNA damaging anticancer agents,"
Nature Communications, Nature, vol. 16(1), pages 1-16, December.
Handle:
RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-62172-4
DOI: 10.1038/s41467-025-62172-4
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