A Mathematical Model of Electrotonic Interactions between Ventricular Myocytes and Fibroblasts

MacCannell, Keith A.; Bazzazi, Hojjat; Chilton, Lisa; Shibukawa, Yoshiyuki; Clark, Robert B.; Giles, Wayne R.

doi:10.1529/biophysj.106.101410

Cited by 193 publications

(381 citation statements)

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“…The elastic modulus rises from (18±2) kPa in the normal heart muscle of non-infarcted animals to (55±15) kPa in significant fibroblast proliferous muscle of infarcted animals, an almost three-fold increase (Berry et al, 2006). Therefore, the functional roles of the fibroblasts in cardiac electrical and mechanical activities have attracted increasing interest, and have been explored in experimental studies (Miragoli et al, 2007;Zlochiver et al, 2008) and computational models (MacCannell et al, 2007;Tanaka et al, 2007;Jacquemet and Henriquez, 2008;Zlochiver et al, 2008;Sachse et al, 2009). Both experimental and computational studies (Miragoli et al, 2006;Jacquemet and Henriquez, 2008;Zlochiver et al, 2008) have illustrated that non-monotonic changes in conduction velocity (CV) are caused by increasing the fibroblast population.…”

Section: Introductionmentioning

confidence: 99%

“…ten Tusscher and Panfilov (2007) showed that CV decreased from 0.7 to 0.3 m/s as the percentage of fibroblast proliferous cells rose from 0 to 40% in two-dimensional (2D) tissue. In simulation studies, it was reported that myocyte-fibroblast coupling modulated AP morphology (MacCannell et al, 2007;Jacquemet and Henriquez, 2008;Sachse et al, 2009). Coupling two or four fibroblasts to a ventricular myocyte resulted in a decrease in action potential duration (APD) from a control value of 263 ms to 195 or 155 ms, respectively (MacCannell et al, 2007).…”

Section: Introductionmentioning

confidence: 99%

“…In simulation studies, it was reported that myocyte-fibroblast coupling modulated AP morphology (MacCannell et al, 2007;Jacquemet and Henriquez, 2008;Sachse et al, 2009). Coupling two or four fibroblasts to a ventricular myocyte resulted in a decrease in action potential duration (APD) from a control value of 263 ms to 195 or 155 ms, respectively (MacCannell et al, 2007). These studies suggest that the effects of fibroblasts on cardiac electrophysiology and mechanics should not be ignored.…”

Section: Introductionmentioning

confidence: 99%

“…These studies suggest that the effects of fibroblasts on cardiac electrophysiology and mechanics should not be ignored. So far, two electrophysiological models of ventricular fibroblasts, a passive model (Xie et al, 2009b) and an active model (MacCannell et al, 2007), have been developed. However, to the best of our knowledge, there is no mechanical model for cardiac fibroblasts, although some experimental studies on the mechanics of the fibroblasts have been reported Eastwood et al, 1998).…”

Section: Introductionmentioning

confidence: 99%

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Fibroblast proliferation alters cardiac excitation conduction and contraction: a computational study

Zhan

Xia

Shou

et al. 2014

J. Zhejiang Univ. Sci. B

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Abstract:In this study, the effects of cardiac fibroblast proliferation on cardiac electric excitation conduction and mechanical contraction were investigated using a proposed integrated myocardial-fibroblastic electromechanical model. At the cellular level, models of the human ventricular myocyte and fibroblast were modified to incorporate a model of cardiac mechanical contraction and cooperativity mechanisms. Cellular electromechanical coupling was realized with a calcium buffer. At the tissue level, electrical excitation conduction was coupled to an elastic mechanics model in which the finite difference method (FDM) was used to solve electrical excitation equations, and the finite element method (FEM) was used to solve mechanics equations. The electromechanical properties of the proposed integrated model were investigated in one or two dimensions under normal and ischemic pathological conditions. Fibroblast proliferation slowed wave propagation, induced a conduction block, decreased strains in the fibroblast proliferous tissue, and increased dispersions in depolarization, repolarization, and action potential duration (APD). It also distorted the wave-front, leading to the initiation and maintenance of re-entry, and resulted in a sustained contraction in the proliferous areas. This study demonstrated the important role that fibroblast proliferation plays in modulating cardiac electromechanical behaviour and which should be considered in planning future heart-modeling studies.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Fibroblast proliferation alters cardiac excitation conduction and contraction: a computational study

Zhan

Xia

Shou

et al. 2014

J. Zhejiang Univ. Sci. B

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“…The fibroblasts are modelled as passive cells; for these fibroblasts, we use the model given by MacCannell, et al [10].…”

Section: Methodsmentioning

confidence: 99%

Spiral-wave Instability in a Medium with a Gradient in the Fibroblast Density: a Computational Study

Zimik

Pandit

2017

Computing in Cardiology Conference (CinC)

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Fibrosis, a process of fibroblast proliferation in cardiac tissue, is a major concern for patients with diseases like ischemia, heart failure, and cardiomyopathy, because of its arrhythmogenic effects. Fibroblasts, in appreciable densities, are IntroductionThe occurrence of abnormal spatiotemporal patterns of electrical waves in cardiac tissue, in the form of spiral waves, has been associated with cardiac arrhythmias [1]. The existence of a single spiral wave is associated with tachycardia [2], and a multiple-spiral-wave state is associated with a life-threatening arrhythmia known as fibrillation [3]. A single-spiral-wave state can transition into a multiple-spiral-wave state if the spiral becomes unstable and breaks up, giving rise to many daughter spirals [1]. Given that fibrillation is a more lethal condition than tachycardia, it is important to understand the mechanisms of the transition process from a single-to a multiple-spiral-wave state. Here, we present a mechanism of spiral-wave instability in a medium with a gradient in fibroblast density (GFD).Fibroblasts are passive cells that are needed for the proper functioning of a heart, because they, along with other cells, form the extracellular matrix and ensure the structural integrity of the heart. However, the abnormal proliferation of fibroblasts because of diseases like ischemia, heart failure, and cardiomyopathy is considered to be arrhythmogenic [4]. Fibroblasts, if they form gapjunctional coupling, can change the electrophysiology of myocytes in cardiac tissue [5]. This, in turn, can affect the dynamics of electrical waves in cardiac tissue. Many studies have been performed to investigate the effects of fibroblasts on wave dynamics in cardiac tissue [6,7]; however, most of the studies, which consider fibroblast-myocyte (FM) coupling, deal with a homogeneous distribution of fibroblasts in the domain. But, the density of fibroblasts in a diseased cardiac tissue may not necessarily be homogeneous [8]. Therefore, it is important to study the effects of FM coupling on wave dynamics in a domain with heterogeneous distributions of fibroblast density.We investigate the effects of GFD on spiral-wave dynamics in a mathematical model for human-ventricular tissue. We find that GFD induces a spatial variation of the local spiral-wave frequency ω in the domain. This variation of ω in the domain leads to spiral-wave instability, and the degree of instability depends on the magnitude of the variation of ω. We also investigate the factors that modulate the variation of ω in the domain. We find that, for a given GFD, the resting membrane potential E f of the fibroblasts, and the number of fibroblasts N f that are coupled to a myocyte can change the spatial variation of ω in the domain. Finally, we also show that GFD can spontaneously initiate spiral waves via high-frequency pacing.

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Bio‐Conductive Polymers for Treating Myocardial Conductive Defects: Long‐Term Efficacy Study

Yang

et al. 2021

Adv Healthcare Materials

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Following myocardial infarction (MI), the resulting fibrotic scar is nonconductive and leads to ventricular dysfunction via electrical uncoupling of the remaining viable cardiomyocytes. The uneven conductive properties between normal myocardium and scar tissue result in arrhythmia, yielding sudden cardiac death/heart failure. A conductive biopolymer, poly-3-amino-4-methoxybenzoic acid-gelatin (PAMB-G), is able to resynchronize myocardial contractions in vivo. Intravenous PAMB-G injections into mice show that it does not cause any acute toxicity, up to the maximum tolerated dose (1.6 mL kg −1 ), which includes the determined therapeutic dose (0.4 mL kg −1 ). There is also no short-or long-term toxicity when PAMB-G is injected into the myocardium of MI rats, with no significant changes in body weight, organ-brain ratio, hematologic, and histological parameters for up to 12 months post-injection. At the therapeutic dose, PAMB-G restores electrical conduction in infarcted rat hearts, resulting in lowered arrhythmia susceptibility and improved cardiac function. PAMB-G is also durable, as mass spectrometry detected the biopolymer for up to 12 months post-injection. PAMB-G did not impact reproductive organ function or offspring characteristics when given intravenously into healthy adult rats. Thus, PAMB-G is a nontoxic, durable, and conductive biomaterial that is able to improve cardiac function for up to 1 year post-implantation.

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A Mathematical Model of Electrotonic Interactions between Ventricular Myocytes and Fibroblasts

Cited by 193 publications

References 43 publications

Fibroblast proliferation alters cardiac excitation conduction and contraction: a computational study

Fibroblast proliferation alters cardiac excitation conduction and contraction: a computational study

Spiral-wave Instability in a Medium with a Gradient in the Fibroblast Density: a Computational Study

Bio‐Conductive Polymers for Treating Myocardial Conductive Defects: Long‐Term Efficacy Study

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