The AP-1 transcription factor Fosl-2 drives cardiac fibrosis and arrhythmias under immunofibrotic conditions.
Mara StellatoMatthias DewenterMichal RudnikAmela HukaraÇağla ÖzsoyFlorian RenouxElena PacheraFelix GantenbeinPetra SeebeckSiim UhtjaervElena OstoDaniel RazanskyKarin KlingelJoerg HenesOliver DistlerPrzemysław BłyszczukGabriela KaniaPublished in: Communications biology (2023)
Fibrotic changes in the myocardium and cardiac arrhythmias represent fatal complications in systemic sclerosis (SSc), however the underlying mechanisms remain elusive. Mice overexpressing transcription factor Fosl-2 (Fosl-2 tg ) represent animal model of SSc. Fosl-2 tg mice showed interstitial cardiac fibrosis, disorganized connexin-43/40 in intercalated discs and deregulated expression of genes controlling conduction system, and developed higher heart rate (HR), prolonged QT intervals, arrhythmias with prevalence of premature ventricular contractions, ventricular tachycardias, II-degree atrio-ventricular blocks and reduced HR variability. Following stimulation with isoproterenol Fosl-2 tg mice showed impaired HR response. In contrast to Fosl-2 tg , immunodeficient Rag2 -/- Fosl-2 tg mice were protected from enhanced myocardial fibrosis and ECG abnormalities. Transcriptomics analysis demonstrated that Fosl-2-overexpression was responsible for profibrotic signature of cardiac fibroblasts, whereas inflammatory component in Fosl-2 tg mice activated their fibrotic and arrhythmogenic phenotype. In human cardiac fibroblasts FOSL-2-overexpression enhanced myofibroblast signature under proinflammatory or profibrotic stimuli. These results demonstrate that under immunofibrotic conditions transcription factor Fosl-2 exaggerates myocardial fibrosis, arrhythmias and aberrant response to stress.
Keyphrases
- left ventricular
- transcription factor
- systemic sclerosis
- heart rate
- high fat diet induced
- heart failure
- heart rate variability
- insulin resistance
- interstitial lung disease
- dna binding
- cell proliferation
- endothelial cells
- type diabetes
- risk factors
- poor prognosis
- metabolic syndrome
- single cell
- adipose tissue
- skeletal muscle
- blood pressure
- genome wide
- genome wide identification
- wild type
- catheter ablation
- epithelial mesenchymal transition