Doxorubicin-induced cardiovascular toxicity: a longitudinal evaluation of functional and molecular markers

Matthias Bosman; Dustin Krüger; Charles Van Assche; Hanne Boen; Cédric Neutel; Kasper Favere; Constantijn Franssen; Wim Martinet; Lynn Roth; Guido R Y De Meyer; Berta Cillero-Pastor; Leen Delrue; Ward Heggermont; Emeline M Van Craenenbroeck; Pieter-Jan Guns

doi:10.1093/cvr/cvad136

Doxorubicin-induced cardiovascular toxicity: a longitudinal evaluation of functional and molecular markers

Cardiovasc Res. 2023 Nov 25;119(15):2579-2590. doi: 10.1093/cvr/cvad136.

Authors

Matthias Bosman¹, Dustin Krüger¹, Charles Van Assche², Hanne Boen^{3

4}, Cédric Neutel¹, Kasper Favere^{1

3

4}, Constantijn Franssen^{3

4}, Wim Martinet¹, Lynn Roth¹, Guido R Y De Meyer¹, Berta Cillero-Pastor^{2

5}, Leen Delrue⁶, Ward Heggermont^{6

7}, Emeline M Van Craenenbroeck^{3

4}, Pieter-Jan Guns¹

Affiliations

¹ Laboratory of Physiopharmacology, Faculty of Medicine and Health Sciences, Faculty of Pharmaceutical, Biomedical and Veterinary Sciences, Campus Drie Eiken, University of Antwerp, Universiteitsplein 1, Antwerp B-2610, Belgium.
² Research Group M4I-Imaging Mass Spectrometry (IMS); Faculty of Health, Medicine and Life Sciences, Maastricht MultiModal Molecular Imaging Institute, Maastricht University, Universiteitssingel 50, 6229 ER, Maastricht, The Netherlands.
³ Research Group Cardiovascular Diseases, GENCOR, University of Antwerp, Antwerp B-2610, Belgium.
⁴ Department of Cardiology, Antwerp University Hospital (UZA), Drie Eikenstraat 655, Edegem B-2650, Belgium.
⁵ Department of Cell Biology-Inspired Tissue Engineering, Institute for Technology-Inspired Regenerative Medicine, Universiteitssingel 40, 6229 ER Maastricht/Room C3.577, PO Box 616, Maastricht 6200 MD, The Netherlands.
⁶ Department of Cardiology, Cardiovascular Center OLV Hospital Aalst, Moorselbaan 164, Aalst B-9300, Belgium.
⁷ Department of Cardiology, Center for Molecular and Vascular Biology, KU Leuven, Herestraat 49, Leuven B-3000, Belgium.

Abstract

Aims: Apart from cardiotoxicity, the chemotherapeutic doxorubicin (DOX) induces vascular toxicity, represented by arterial stiffness and endothelial dysfunction. Both parameters are of interest for cardiovascular risk stratification as they are independent predictors of future cardiovascular events in the general population. However, the time course of DOX-induced cardiovascular toxicity remains unclear. Moreover, current biomarkers for cardiovascular toxicity prove insufficient. Here, we longitudinally evaluated functional and molecular markers of DOX-induced cardiovascular toxicity in a murine model. Molecular markers were further validated in patient plasma.

Methods and results: DOX (4 mg/kg) or saline (vehicle) was administered intra-peritoneally to young, male mice weekly for 6 weeks. In vivo cardiovascular function and ex vivo arterial stiffness and vascular reactivity were evaluated at baseline, during DOX therapy (Weeks 2 and 4) and after therapy cessation (Weeks 6, 9, and 15). Left ventricular ejection fraction (LVEF) declined from Week 4 in the DOX group. DOX increased arterial stiffness in vivo and ex vivo at Week 2, which reverted thereafter. Importantly, DOX-induced arterial stiffness preceded reduced LVEF. Further, DOX impaired endothelium-dependent vasodilation at Weeks 2 and 6, which recovered at Weeks 9 and 15. Conversely, contraction with phenylephrine was consistently higher in the DOX-treated group. Furthermore, proteomic analysis on aortic tissue identified increased thrombospondin-1 (THBS1) and alpha-1-antichymotrypsin (SERPINA3) at Weeks 2 and 6. Up-regulated THBS1 and SERPINA3 persisted during follow-up. Finally, THBS1 and SERPINA3 were quantified in plasma of patients. Cancer survivors with anthracycline-induced cardiotoxicity (AICT; LVEF < 50%) showed elevated THBS1 and SERPINA3 levels compared with age-matched control patients (LVEF ≥ 60%).

Conclusions: DOX increased arterial stiffness and impaired endothelial function, which both preceded reduced LVEF. Vascular dysfunction restored after DOX therapy cessation, whereas cardiac dysfunction persisted. Further, we identified SERPINA3 and THBS1 as promising biomarkers of DOX-induced cardiovascular toxicity, which were confirmed in AICT patients.

Keywords: Arterial stiffness; Cardiotoxicity; Doxorubicin; Endothelial dysfunction.

Publication types

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

MeSH terms

Animals
Biomarkers
Cardiotoxicity* / drug therapy
Doxorubicin / toxicity
Humans
Male
Mice
Proteomics*
Stroke Volume
Ventricular Function, Left

Substances

Doxorubicin
Biomarkers

Abstract

Publication types

MeSH terms

Substances

Grants and funding