Doxorubicin induces cardiotoxicity in a pluripotent stem cell model of aggressive B cell lymphoma cancer patients

Luis Peter Haupt; Sabine Rebs; Wiebke Maurer; Daniela Hübscher; Malte Tiburcy; Steffen Pabel; Andreas Maus; Steffen Köhne; Rewati Tappu; Jan Haas; Yun Li; Andre Sasse; Celio C X Santos; Ralf Dressel; Leszek Wojnowski; Gertrude Bunt; Wiebke Möbius; Ajay M Shah; Benjamin Meder; Bernd Wollnik; Samuel Sossalla; Gerd Hasenfuss; Katrin Streckfuss-Bömeke

doi:10.1007/s00395-022-00918-7

Doxorubicin induces cardiotoxicity in a pluripotent stem cell model of aggressive B cell lymphoma cancer patients

Basic Res Cardiol. 2022 Mar 8;117(1):13. doi: 10.1007/s00395-022-00918-7.

Authors

Luis Peter Haupt^#^{1

2}, Sabine Rebs^#^{1

2

3}, Wiebke Maurer^{1

2}, Daniela Hübscher^{1

2}, Malte Tiburcy^{2

4}, Steffen Pabel⁵, Andreas Maus^{1

2

6}, Steffen Köhne^{1

2}, Rewati Tappu^{7

8}, Jan Haas^{7

8}, Yun Li⁹, Andre Sasse¹⁰, Celio C X Santos⁶, Ralf Dressel^{1

2

10}, Leszek Wojnowski¹¹, Gertrude Bunt¹², Wiebke Möbius^{13

14}, Ajay M Shah⁶, Benjamin Meder^{7

8}, Bernd Wollnik^{2

9}, Samuel Sossalla^{1

2

5}, Gerd Hasenfuss^{1

2}, Katrin Streckfuss-Bömeke^{15

16

17}

Affiliations

¹ Clinic for Cardiology and Pneumology, University Medical Centre Göttingen, Göttingen, Germany.
² DZHK (German Centre for Cardiovascular Research), partner site Göttingen, Göttingen, Germany.
³ Institute of Pharmacology and Toxicology, Würzburg University, Würzburg, Germany.
⁴ Institute of Pharmacology and Toxicology, University Medical Centre Göttingen, Göttingen, Germany.
⁵ Department of Internal Medicine 2, Cardiology, University Medical Centre Regensburg, Regensburg, Germany.
⁶ King's College London, British Heart Foundation Centre of Excellence, London, UK.
⁷ Department of Cardiology, University of Heidelberg, Heidelberg, Germany.
⁸ DZHK (German Centrefor Cardiovascular Research), partner site Heidelberg, Heidelberg, Germany.
⁹ Institute of Human Genetics, University Hospital Centre Göttingen, Göttingen, Germany.
¹⁰ Institute of Cellular and Molecular Immunology, University Medical Centre Göttingen, Göttingen, Germany.
¹¹ Department of Pharmacology, University Medical Centre Mainz, Mainz, Germany.
¹² Clinical Optical Microscopy, University Medical Centre Göttingen, Göttingen, Germany.
¹³ Department of Neurogenetics, Electron Microscopy Core Unit, Max Planck Institute for Multidisciplinary Sciences, Göttingen, Germany.
¹⁴ Cluster of Excellence "Multiscale Bioimaging: From Molecular Machines to Networks of Excitable Cells" (MBExC), University of Göttingen, Göttingen, Germany.
¹⁵ Clinic for Cardiology and Pneumology, University Medical Centre Göttingen, Göttingen, Germany. katrin.streckfuss@med.uni-goettingen.de.
¹⁶ DZHK (German Centre for Cardiovascular Research), partner site Göttingen, Göttingen, Germany. katrin.streckfuss@med.uni-goettingen.de.
¹⁷ Institute of Pharmacology and Toxicology, Würzburg University, Würzburg, Germany. katrin.streckfuss@med.uni-goettingen.de.

^# Contributed equally.

Abstract

Cancer therapies with anthracyclines have been shown to induce cardiovascular complications. The aims of this study were to establish an in vitro induced pluripotent stem cell model (iPSC) of anthracycline-induced cardiotoxicity (ACT) from patients with an aggressive form of B-cell lymphoma and to examine whether doxorubicin (DOX)-treated ACT-iPSC cardiomyocytes (CM) can recapitulate the clinical features exhibited by patients, and thus help uncover a DOX-dependent pathomechanism. ACT-iPSC CM generated from individuals with CD20⁺ B-cell lymphoma who had received high doses of DOX and suffered cardiac dysfunction were studied and compared to control-iPSC CM from cancer survivors without cardiac symptoms. In cellular studies, ACT-iPSC CM were persistently more susceptible to DOX toxicity including augmented disorganized myofilament structure, changed mitochondrial shape, and increased apoptotic events. Consistently, ACT-iPSC CM and cardiac fibroblasts isolated from fibrotic human ACT myocardium exhibited higher DOX-dependent reactive oxygen species. In functional studies, Ca²⁺ transient amplitude of ACT-iPSC CM was reduced compared to control cells, and diastolic sarcoplasmic reticulum Ca²⁺ leak was DOX-dependently increased. This could be explained by overactive CaMKIIδ in ACT CM. Together with DOX-dependent augmented proarrhythmic cellular triggers and prolonged action potentials in ACT CM, this suggests a cellular link to arrhythmogenic events and contractile dysfunction especially found in ACT engineered human myocardium. CamKIIδ inhibition prevented proarrhythmic triggers in ACT. In contrast, control CM upregulated SERCA2a expression in a DOX-dependent manner, possibly to avoid heart failure conditions. In conclusion, we developed the first human patient-specific stem cell model of DOX-induced cardiac dysfunction from patients with B-cell lymphoma. Our results suggest that DOX-induced stress resulted in arrhythmogenic events associated with contractile dysfunction and finally in heart failure after persistent stress activation in ACT patients.

Keywords: Anthracyclin-induced cardiotoxicity (ACT); Cardiac fibroblasts; Cardiomyocytes; Doxorubicin; Heart failure; Induced pluripotent stem cells (iPSC).

Publication types

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

MeSH terms

Cardiotoxicity / metabolism
Cardiotoxicity / pathology
Doxorubicin / metabolism
Doxorubicin / toxicity
Heart Diseases* / metabolism
Heart Failure* / metabolism
Humans
Induced Pluripotent Stem Cells* / metabolism
Lymphoma, B-Cell* / metabolism
Lymphoma, B-Cell* / pathology
Myocytes, Cardiac / metabolism
Neoplasms* / metabolism

Substances

Doxorubicin

Grants and funding

RG/20/3/34823/BHF_/British Heart Foundation/United Kingdom