Ex vivo modelling of cardiac injury identifies ferroptosis-related pathways as a potential therapeutic avenue for translational medicine

Naisam Abbas; Marco Bentele; Florian J G Waleczek; Maximilian Fuchs; Annette Just; Angelika Pfanne; Andreas Pich; Sophie Linke; Susanne Neumüller; Angelika Stucki-Koch; Maria Jordan; Filippo Perbellini; Christopher Werlein; Wilhelm Korte; Fabio Ius; Arjang Ruhparwar; Natalie Weber; Jan Fiedler; Thomas Thum

doi:10.1016/j.yjmcc.2024.09.012

Ex vivo modelling of cardiac injury identifies ferroptosis-related pathways as a potential therapeutic avenue for translational medicine

J Mol Cell Cardiol. 2024 Sep 26:196:125-140. doi: 10.1016/j.yjmcc.2024.09.012. Online ahead of print.

Authors

Naisam Abbas¹, Marco Bentele², Florian J G Waleczek¹, Maximilian Fuchs³, Annette Just⁴, Angelika Pfanne⁴, Andreas Pich⁵, Sophie Linke⁴, Susanne Neumüller⁴, Angelika Stucki-Koch³, Maria Jordan³, Filippo Perbellini⁴, Christopher Werlein⁶, Wilhelm Korte⁷, Fabio Ius⁷, Arjang Ruhparwar⁷, Natalie Weber⁴, Jan Fiedler³, Thomas Thum⁸

Affiliations

¹ Institute of Molecular and Translational Therapeutic Strategies (IMTTS), Hannover Medical School, Hannover, Germany; Fraunhofer Institute of Toxicology and Experimental Medicine (ITEM), Hannover, Germany; Fraunhofer Cluster of Excellence Immune-Mediated Diseases (CIMD), Hannover, Germany.
² Institute of Molecular and Translational Therapeutic Strategies (IMTTS), Hannover Medical School, Hannover, Germany; Fraunhofer Cluster of Excellence Immune-Mediated Diseases (CIMD), Hannover, Germany.
³ Fraunhofer Institute of Toxicology and Experimental Medicine (ITEM), Hannover, Germany; Fraunhofer Cluster of Excellence Immune-Mediated Diseases (CIMD), Hannover, Germany.
⁴ Institute of Molecular and Translational Therapeutic Strategies (IMTTS), Hannover Medical School, Hannover, Germany.
⁵ Institute of Toxicology and Core Unit Proteomics, Hannover Medical School, Hannover, Germany.
⁶ Institute of Pathology, Hannover Medical School, Hannover, Germany.
⁷ Department of Cardiothoracic, Transplantation and Vascular Surgery, Hannover Medical School, Hannover, Germany.
⁸ Institute of Molecular and Translational Therapeutic Strategies (IMTTS), Hannover Medical School, Hannover, Germany; Center for Translational Regenerative Medicine, Hannover Medical School, Hannover, Germany. Electronic address: Thum.Thomas@mh-hannover.de.

PMID: 39341589
DOI: 10.1016/j.yjmcc.2024.09.012

Abstract

Background: Heart failure (HF) is a burgeoning health problem worldwide. Often arising as a result of cardiac injury, HF has become a major cause of mortality with limited availability of effective treatments. Ferroptotic pathways, triggering an iron-dependent form of cell death, are known to be potential key players in heart disease. This form of cell death does not exhibit typical characteristics of programmed cell death, and is mediated by impaired iron metabolism and lipid peroxidation signalling.

Objectives: The aim of this study is to establish an ex-vivo model of myocardial injury in living myocardial slices (LMS) and to identify novel underlying mechanisms and potential therapeutic druggable target(s).

Methods and results: In this study, we employed LMS as an ex vivo model of cardiac injury to investigate underlying mechanisms and potential therapeutic targets. Cryoinjury was induced in adult rat LMS, resulting in 30 % tissue damage. Cryoinjured LMS demonstrated impaired contractile function, cardiomyocyte hypertrophy, inflammation, and cardiac fibrosis, closely resembling in vivo cardiac injury characteristics. Proteomic analysis revealed an enrichment of factors associated with ferroptosis in the injured LMS, suggesting a potential causative role. To test this hypothesis, we pharmacologically inhibited ferroptotic pathways using ferrostatin (Fer-1) in the cryoinjured rat LMS, resulting in attenuation of structural changes and repression of pro-fibrotic processes. Furthermore, LMS generated from failing human hearts were used as a model of chronic heart failure. In this model, Fer-1 treatment was observed to reduce the expression of ferroptotic genes, enhances contractile function and improves tissue viability. Blocking ferroptosis-associated pathways in human cardiac fibroblasts (HCFs) resulted in a downregulation of fibroblast activation genes, a decrease in fibroblast migration capacity, and a reduction in reactive oxygen species production. RNA sequencing analysis of Fer-1-treated human LMS implicated metallothioneins as a potential underlying mechanism for the inhibition of these pathways. This effect is possibly mediated through the replenishment of glutathione reserves.

Conclusions: Our findings highlight the potential of targeting ferroptosis-related pathways and metallothioneins as a promising strategy for the treatment of heart disease.

Keywords: Cardiac fibroblast; Cardiac injury; Ferrostatin; Living myocardial slice; Metallothionein.