Atrial remodeling in atrial fibrillation shares structural, metabolic, and electrophysiologic traits with hibernating myocardium, representing a conserved adaptive response to chronic stress.
Understanding the shared pathophysiologic traits between AF and hibernating myocardium may facilitate the discovery of novel therapeutic targets for AF.
Atrial fibrillation (AF) is the most common arrhythmia and is associated with a high risk of morbidity and mortality. However, there are limited treatment strategies for prevention of disease onset and progression. Development of novel therapies for primary and secondary prevention of AF is critical and requires improved understanding of the cellular and molecular mechanisms underlying the AF disease process. Translational and clinical studies conducted over the past twenty years have revealed that atrial remodeling in AF shares several important pathophysiologic traits with the remodeling processes exhibited by hibernating myocardium that develop in response to chronic ischemia. These shared features, which include an array of structural, metabolic, and electrophysiologic changes, appear to represent a conserved adaptive myocyte response to chronic stress that involves dedifferentiation towards a fetal phenotype to promote survival. In this review, we discuss the pathophysiology of AF, summarize studies supporting a common remodeling program in AF and hibernating myocardium, and propose future therapeutic implications of this emerging paradigm. Ultimately, better understanding of the molecular mechanisms of atrial myocyte remodeling during the onset of AF and the transition from paroxysmal to persistent stages of the disease may facilitate discovery of new therapeutic targets.
Weil et al. (Thu,) conducted a review in Atrial fibrillation. Atrial remodeling in atrial fibrillation shares structural, metabolic, and electrophysiologic traits with hibernating myocardium, representing a conserved adaptive response to chronic stress.
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