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Oxidative Stress and Inflammatory Modulation of Ca<sup>2+</sup> Handling in Metabolic HFpEF-Related Left Atrial Cardiomyopathy
oleh: David Bode, Yan Wen, Niklas Hegemann, Uwe Primessnig, Abdul Parwani, Leif-Hendrik Boldt, Burkert M. Pieske, Frank R. Heinzel, Felix Hohendanner
Format: | Article |
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Diterbitkan: | MDPI AG 2020-09-01 |
Deskripsi
Metabolic syndrome-mediated heart failure with preserved ejection fraction (HFpEF) is commonly accompanied by left atrial (LA) cardiomyopathy, significantly affecting morbidity and mortality. We evaluate the role of reactive oxygen species (ROS) and intrinsic inflammation (TNF-α, IL-10) related to dysfunctional Ca<sup>2+</sup> homeostasis of LA cardiomyocytes in a rat model of metabolic HFpEF. ZFS-1 obese rats showed features of HFpEF and atrial cardiomyopathy in vivo: increased left ventricular (LV) mass, E/e’ and LA size and preserved LV ejection fraction. In vitro, LA cardiomyocytes exhibited more mitochondrial-fission (MitoTracker) and ROS-production (H2DCF). In wildtype (WT), pro-inflammatory TNF-α impaired cellular Ca<sup>2+</sup> homeostasis, while anti-inflammatory IL-10 had no notable effect (confocal microscopy; Fluo-4). In HFpEF, TNF-α had no effect on Ca<sup>2+</sup> homeostasis associated with decreased TNF-α receptor expression (western blot). In addition, IL-10 substantially improved Ca<sup>2+</sup> release and reuptake, while IL-10 receptor-1 expression was unaltered. Oxidative stress in metabolic syndrome mediated LA cardiomyopathy was increased and anti-inflammatory treatment positively affected dysfunctional Ca<sup>2+</sup> homeostasis. Our data indicates, that patients with HFpEF-related LA dysfunction might profit from IL-10 targeted therapy, which should be further explored in preclinical trials.