Abstract
Desmosomes are critical adhesion structures in cardiomyocytes, with mutation/loss linked to the heritable cardiac disease, arrhythmogenic right ventricular cardiomyopathy (ARVC). Early studies revealed the ability of desmosomal protein loss to trigger ARVC disease features including structural remodeling, arrhythmias, and inflammation; however, the precise mechanisms contributing to diverse disease presentations are not fully understood. Recent mechanistic studies demonstrated the protein degradation component CSN6 is a resident cardiac desmosomal protein which selectively restricts cardiomyocyte desmosomal degradation and disease. This suggests defects in protein degradation can trigger the structural remodeling underlying ARVC. Additionally, a subset of ARVC-related mutations show enhanced vulnerability to calpain-mediated degradation, further supporting the relevance of these mechanisms in disease. Desmosomal gene mutations/loss has been shown to impact arrhythmogenic pathways in the absence of structural disease within ARVC patients and model systems. Studies have shown the involvement of connexins, calcium handling machinery, and sodium channels as early drivers of arrhythmias, suggesting these may be distinct pathways regulating electrical function from the desmosome. Emerging evidence has suggested inflammation may be an early mechanism in disease pathogenesis, as clinical reports have shown an overlap between myocarditis and ARVC. Recent studies focus on the association between desmosomal mutations/loss and inflammatory processes including autoantibodies and signaling pathways as a way to understand the involvement of inflammation in ARVC pathogenesis. A specific focus will be to dissect ongoing fields of investigation to highlight diverse pathogenic pathways associated with desmosomal mutations/loss.
Highlights
The desmosome is integral for maintaining structural integrity in tissues undergoing constant mechanical stress such as the heart (Najor 2018)
The cardiac desmosome is thought to have canonical functions as a structural element in the cardiomyocyte, recent studies have highlighted new resident regulatory functions that relate to its protein turnover as well as cross talk with electrical channels as well as inflammatory cell types and pathways
At least two pathways have been linked to cardiac desmosomal protein homeostasis, one which is resident (CSN6) to the desmosome and one found in the cytosol; future studies should focus on how these pathways work cooperatively to degrade desmosomal proteins in the context of human arrhythmogenic right ventricular cardiomyopathy (ARVC)-associated desmosomal mutations
Summary
The desmosome is integral for maintaining structural integrity in tissues undergoing constant mechanical stress such as the heart (Najor 2018). Crosstalk between desmosomes and neighboring gap junction protein, connexins, membrane-associated voltage-gated Na+ channels, and most recently calcium handling machinery has been postulated in driving cardiac arrhythmias independent of the structural remodeling response associated with desmosomal mutations/protein loss (Cerrone et al 2012; Lyon et al 2014; Mezzano et al 2016; Cerrone et al 2017; Kim et al 2019).
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