Abstract
During cardiac diseases many types of anatomical and functional remodeling of cardiac tissue can occur. In this work, we focus on two conditions: hypoxia and fibrosis, which are part of complex pathological modifications that take place in many cardiac diseases (hypertrophic cardiomyopathy, hypertensive heart disease, and recurrent myocardial infarction) and respiratory diseases (obstructive pulmonary disease, obstructive sleep apnea, and cystic fibrosis). Using computational models of cardiac electrophysiology, we evaluate if the interplay between hypoxia and fibrosis is sufficient to trigger cardiac arrhythmia. We study the mechanisms behind the generation of ectopic beats, an arrhythmic trigger also known as premature ventricular contractions (PVCs), in regions with high hypoxia and fibrosis. First, we modify an electrophysiological model of myocytes of the human left ventricle to include the effects of hypoxia. Second, diffuse fibrosis is modeled by randomly replacing cardiac myocytes by non-excitable and non-conducting cells. The Monte Carlo method is used to evaluate the probability of a region to generate ectopic beats with respect to different levels of hypoxia and fibrosis. In addition, we evaluate the minimum size of three-dimensional slabs needed to sustain reentries for different stimulation protocols. The observed mechanism behind the initiation of ectopic beats is unidirectional block, giving rise to sustained micro-reentries inside the region with diffuse fibrosis and hypoxia. In summary, our results suggest that hypoxia and fibrosis are sufficient for the creation of a focal region in the heart that generates PVCs.
Highlights
If the fraction φ of fibrosis is close to the percolation limit of the grid (Alonso and Bär, 2013; Alonso et al, 2016) the waves propagate slower inside the injured region in comparison with the speed on the healthy tissue, see Figures 2C,D
The computer simulations presented in this work suggest that the combination of fibrosis and hypoxia in a localized region of the myocardium can provide a sufficient condition for the genesis of ectopic beats
Specific regions have been correlated with the generation of ectopic beats, such as the pulmonary veins (Haïssaguerre et al, 1998) during atrial fibrillation or border zone of infarct regions after coronary occlusion (Boineau and Cox, 1973), the mechanism behind this remains unclear
Summary
Studies suggest the existence of anatomical triggers for dangerous arrhythmias (de Bakker et al, 1988; Haïssaguerre et al, 1998; Ng, 2006; Jalife, 2011). These pathological regions would repeatedly re-excite the neighboring cardiac tissue, acting as sources, drivers, or foci of ectopic beats. When the region is in the left ventricle, it is the source of premature ventricular contractions (PVCs) (Boineau and Cox, 1973; Ruberman et al, 1977).
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