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Heterogeneous cardiac sympathetic innervation gradients promote arrhythmogenesis in murine dilated cardiomyopathy
Al-Hassan J. Dajani, Michael B. Liu, Michael A. Olaopa, Lucian Cao, Carla Valenzuela-Ripoll, Timothy J. Davis, Megan D. Poston, Elizabeth H. Smith, Jaime Contreras, Marissa Pennino, Christopher M. Waldmann, Donald B. Hoover, Jason T. Lee, Patrick Y. Jay, Ali Javaheri, Roger Slavik, Zhilin Qu, Olujimi A. Ajijola
Al-Hassan J. Dajani, Michael B. Liu, Michael A. Olaopa, Lucian Cao, Carla Valenzuela-Ripoll, Timothy J. Davis, Megan D. Poston, Elizabeth H. Smith, Jaime Contreras, Marissa Pennino, Christopher M. Waldmann, Donald B. Hoover, Jason T. Lee, Patrick Y. Jay, Ali Javaheri, Roger Slavik, Zhilin Qu, Olujimi A. Ajijola
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Research Article Cardiology

Heterogeneous cardiac sympathetic innervation gradients promote arrhythmogenesis in murine dilated cardiomyopathy

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Abstract

Ventricular arrhythmias (VAs) in heart failure are enhanced by sympathoexcitation. However, radiotracer studies of catecholamine uptake in failing human hearts demonstrate a proclivity for VAs in patients with reduced cardiac sympathetic innervation. We hypothesized that this counterintuitive finding is explained by heterogeneous loss of sympathetic nerves in the failing heart. In a murine model of dilated cardiomyopathy (DCM), delayed PET imaging of sympathetic nerve density using the catecholamine analog [11C]meta-Hydroxyephedrine demonstrated global hypoinnervation in ventricular myocardium. Although reduced, sympathetic innervation in 2 distinct DCM models invariably exhibited transmural (epicardial to endocardial) gradients, with the endocardium being devoid of sympathetic nerve fibers versus controls. Further, the severity of transmural innervation gradients was correlated with VAs. Transmural innervation gradients were also identified in human left ventricular free wall samples from DCM versus controls. We investigated mechanisms underlying this relationship by in silico studies in 1D, 2D, and 3D models of failing and normal human hearts, finding that arrhythmogenesis increased as heterogeneity in sympathetic innervation worsened. Specifically, both DCM-induced myocyte electrical remodeling and spatially inhomogeneous innervation gradients synergistically worsened arrhythmogenesis. Thus, heterogeneous innervation gradients in DCM promoted arrhythmogenesis. Restoration of homogeneous sympathetic innervation in the failing heart may reduce VAs.

Authors

Al-Hassan J. Dajani, Michael B. Liu, Michael A. Olaopa, Lucian Cao, Carla Valenzuela-Ripoll, Timothy J. Davis, Megan D. Poston, Elizabeth H. Smith, Jaime Contreras, Marissa Pennino, Christopher M. Waldmann, Donald B. Hoover, Jason T. Lee, Patrick Y. Jay, Ali Javaheri, Roger Slavik, Zhilin Qu, Olujimi A. Ajijola

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Figure 2

DCM model shows decreased cardiac sympathetic innervation.

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DCM model shows decreased cardiac sympathetic innervation.
(A) Represent...
(A) Representative [11C]meta-Hydroxyephedrine PET-CT images taken at the 60-minute time point of WT (top) and DCM (bottom) mouse models scaled to units of percentage injected dose per gram of tissue (% ID/g) (head, heart, and tail labeled for orientation). (B) [11C]meta-Hydroxyephedrine time-activity curves (0–60 minutes) showing uptake in adrenergic nerve terminals of various tissues in control and DCM mice. (C) Quantification at 60 minutes to show uptake of [11C]meta-Hydroxyephedrine in adrenergic nerve terminals of various tissues in control and DCM mice: cardiac base (n = 4 for control, n = 4 for DCM, *P = 0.0286, Mann-Whitney test), cardiac apex (n = 4 for control, n = 4 for DCM, *P = 0.0286, Mann-Whitney test), cardiac ant. wall (n = 4 for control, n = 4 for DCM, *P = 0.0286, Mann-Whitney test), cardiac post. wall (n = 4 for control, n = 4 for DCM, *P = 0.0286, Mann-Whitney test), hind leg (n = 4 for control, n = 4 for DCM, P = 0.3429, Mann-Whitney test), and superior mediastinum (n = 4 for control, n = 4 for DCM, P = 0.1143, Mann-Whitney test).

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