Proinflammatory cytokines driving cardiotoxicity in COVID-19

Maria Colzani; Johannes Bargehr; Federica Mescia; Eleanor C Williams; Vincent Knight-Schrijver; Jonathan Lee; Charlotte Summers; Irina Mohorianu; Kenneth G C Smith; Paul A Lyons; Sanjay Sinha

doi:10.1093/cvr/cvad174

Proinflammatory cytokines driving cardiotoxicity in COVID-19

Cardiovasc Res. 2024 Mar 13;120(2):174-187. doi: 10.1093/cvr/cvad174.

Authors

Maria Colzani^{1

2}, Johannes Bargehr^{1

2}, Federica Mescia^{2

3}, Eleanor C Williams¹, Vincent Knight-Schrijver^{1

2}, Jonathan Lee^{1

2}, Charlotte Summers^{2

4}, Irina Mohorianu¹, Kenneth G C Smith^{2

3}, Paul A Lyons^{2

3}, Sanjay Sinha^{1

2}

Affiliations

¹ Wellcome - MRC Cambridge Stem Cell Institute, Jeffrey Cheah Biomedical Centre, Cambridge Biomedical Campus, University of Cambridge, Puddicombe Way, CB2 0AW Cambridge, UK.
² Department of Medicine, School of Clinical Medicine, University of Cambridge, Cambridge Biomedical Campus, Addenbrooke's Hospital, Hills Rd, CB2 0SP Cambridge, UK.
³ Cambridge Institute of Therapeutic Immunology and Infectious Disease, Jeffrey Cheah Biomedical Centre, Cambridge Biomedical Campus, Puddicombe Way, CB2 0AW Cambridge, UK.
⁴ Wolfson Lung Injury Unit, Heart and Lung Research Institute, Cambridge Biomedical Campus, Papworth Road, CB2 0BB Cambridge, UK.

Abstract

Aims: Cardiac involvement is common in patients hospitalized with COVID-19 and correlates with an adverse disease trajectory. While cardiac injury has been attributed to direct viral cytotoxicity, serum-induced cardiotoxicity secondary to serological hyperinflammation constitutes a potentially amenable mechanism that remains largely unexplored.

Methods and results: To investigate serological drivers of cardiotoxicity in COVID-19 we have established a robust bioassay that assessed the effects of serum from COVID-19 confirmed patients on human embryonic stem cell (hESC)-derived cardiomyocytes. We demonstrate that serum from COVID-19 positive patients significantly reduced cardiomyocyte viability independent of viral transduction, an effect that was also seen in non-COVID-19 acute respiratory distress syndrome (ARDS). Serum from patients with greater disease severity led to worse cardiomyocyte viability and this significantly correlated with levels of key inflammatory cytokines, including IL-6, TNF-α, IL1-β, IL-10, CRP, and neutrophil to lymphocyte ratio with a specific reduction of CD4+ and CD8+ cells. Combinatorial blockade of IL-6 and TNF-α partly rescued the phenotype and preserved cardiomyocyte viability and function. Bulk RNA sequencing of serum-treated cardiomyocytes elucidated specific pathways involved in the COVID-19 response impacting cardiomyocyte viability, structure, and function. The observed effects of serum-induced cytotoxicity were cell-type selective as serum exposure did not adversely affect microvascular endothelial cell viability but resulted in endothelial activation and a procoagulant state.

Conclusion: These results provide direct evidence that inflammatory cytokines are at least in part responsible for the cardiovascular damage seen in COVID-19 and characterise the downstream activated pathways in human cardiomyocytes. The serum signature of patients with severe disease indicates possible targets for therapeutic intervention.

Keywords: COVID-19; Cardiotoxicity; Inflammation; Stem cell derived cardiomyocytes.

Publication types

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

MeSH terms

COVID-19*
Cardiotoxicity
Cytokines
Humans
Interleukin-6
Tumor Necrosis Factor-alpha

Substances

Cytokines
Interleukin-6
Tumor Necrosis Factor-alpha

Abstract

Publication types

MeSH terms

Substances

Grants and funding