Mitochondrial Dysfunction in Arrhythmia and Cardiac Hypertrophy

² Collaborative Innovation Center for Birth Defect Research and Transformation of Shandong Province, Jining Medical University, 272067 Jining, Shandong, China

³ College of Second Clinical Medicine, Jining Medical University, 272067 Jining, Shandong, China

⁴ Department of Cardiology, Ruijin Hospital, Shanghai Jiao Tong University, School of Medicine, 200025 Shanghai, China

⁵ College of Basic Medical, Xuzhou Medical University, 221004 Xuzhou, Jiangsu, China

⁶ Lin He's Academician Workstation of New Medicine and Clinical Translation, Jining Medical University, 272067 Jining, Shandong, China

^*Correspondence: chun-kai-huang@outlook.com (Chun-Kai Huang); tanrubin11@126.com (Rubin Tan); yuanjinxiang18@163.com (Jinxiang Yuan)
^†These authors contributed equally.

Rev. Cardiovasc. Med. 2023, 24(12), 364; https://doi.org/10.31083/j.rcm2412364

Submitted: 27 May 2023 | Revised: 18 August 2023 | Accepted: 4 September 2023 | Published: 25 December 2023

(This article belongs to the Section Heart Diseases)

This is an open access article under the CC BY 4.0 license.

Abstract

Arrhythmia and cardiac hypertrophy are two very common cardiovascular diseases that can lead to heart failure and even sudden death, thus presenting a serious threat to human life and health. According to global statistics, nearly one million people per year die from arrhythmia, cardiac hypertrophy and other associated cardiovascular diseases. Hence, there is an urgent need to find new treatment targets and to develop new intervention measures. Recently, mitochondrial dysfunction has been examined in relation to heart disease with a view to lowering the incidence of arrhythmia and cardiac hypertrophy. The heart is the body’s largest energy consuming organ, turning over about 20 kg of adenosine triphosphate (ATP) per day in the mitochondria. Mitochondrial oxidative phosphorylation (OXPHOS) produces up to 90% of the ATP needed by cardiac muscle cells for contraction and relaxation. Dysfunction of heart mitochondria can therefore induce arrhythmia, cardiac hypertrophy and other cardiovascular diseases. Mitochondrial DNA (mtDNA) mutations cause disorders in OXPHOS and defects in the synthesis of muscle contraction proteins. These lead to insufficient production of secondary ATP, increased metabolic requirements for ATP by the myocardium, and the accumulation of reactive oxygen species (ROS). The resulting damage to myocardial cells eventually induces arrhythmia and cardiac hypertrophy. Mitochondrial damage decreases the efficiency of energy production, which further increases the production of ROS. The accumulation of ROS causes mitochondrial damage and eventually leads to a vicious cycle of mitochondrial damage and low efficiency of mitochondrial energy production. In this review, the mechanism underlying the development of arrhythmia and cardiac hypertrophy is described in relation to mitochondrial energy supply, oxidative stress, mtDNA mutation and Mitochondrial dynamics. Targeted therapy for arrhythmia and cardiac hypertrophy induced by mitochondrial dysfunction is also discussed in terms of its potential clinical value. These strategies should improve our understanding of mitochondrial biology and the pathogenesis of arrhythmia and cardiac hypertrophy. They may also identify novel strategies for targeting mitochondria in the treatment of these diseases.

Keywords

mitochondria

dysfunction

heart

arrhythmias

cardiac hypertrophy

Funding

82100522/National Natural Science Foundation of China

600791001/Research Start-up Fund of Jining Medical University

JYHL2021MS10/Research Fund for Lin He’s Academician Workstation of New Medicine and Clinical Translation in Jining Medical University

81700055/National Natural Science Foundation of China

Figures

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Fig. 1.

Mechanisms by which mitochondria are involved in regulating cardiac arrhythmias through energy control, oxidative stress, mitochondrial DNA, mitochondrial dynamics, and more: In the mouse TECRL KO model, the PI3K/AKT pathway is inhibited in cardiomyocytes, the expression of mitochondrial Mfn2 protein is decreased, the expression of OXPHOS-related proteins is decreased, ATP production is decreased, and arrhythmia is induced. In an in vitro culture model of ventricular myocytes isolated from CPVT mice, we detected excessive RyR2 channels and increased SR Ca ${}^{2+}$ leakage. After excessive Ca ${}^{2+}$ in the cytoplasm was taken up by MCU on the mitochondria, mitochondrial Ca ${}^{2+}$ overload was induced, which led to increased ROS production and further driven SR Ca ${}^{2+}$ leakage and formed a positive feedback process. It drives the onset of arrhythmias. Mitochondrial dysfunction caused by mtDNA mutations, mtDNA4977 deficiency and mtDNA damage is one of the important causes of arrhythmia. In MI rats exposed to PM2.5 followed by ISO injection, the protein expression of Mfn1 was down-regulated, and the protein expression of PINK1 and Parkin was up-regulated, which aggravated the infarct size, destroyed the normal sinus rhythm, and triggered ventricular arrhythmias. In the HL-1 cell model, Drp1 inhibitor midivi exerted anti-arrhythmia effect by inhibiting the expression of Drp1, enhancing mitochondrial membrane potential, reducing mitochondrial fission and inhibiting cell apoptosis. ATP, adenosine triphosphate; Akt, V-akt murine thymoma viral oncogene homolog; Ca ${}^{2+}$ , calcium ion; CPVT, catecholaminergic polymorphic ventricular tachycardia; Drp1, dynamin-related protein 1; ISO, isoproterenol; MCU, mitochondrial calcium uniporter protein; Mfn1, mitofusin-1; Mfn2, mitofusin-2; MtDNA, mitochondrial DNA; PI3K, phosphoinositide 3-kinase; PINK1, phosphatase and tensin homolog deleted on chromosome ten-induced putative kinase 1; RyR2, ryanodine receptor 2; SR, sarcoplasmic reticulum; TECRL KO, Trans-2,3-Enoyl-CoA Reductase-Like Knockout; OXPHOS, oxidative phosphorylation system; ROS, reactive oxygen species; MI, myocardial infarction; PM2.5, particulate matter 2.5; HL-1, mouse cardiomyocyte cell line.

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Rev. Cardiovasc. Med. Print ISSN 1530-6550 Electronic ISSN 2153-8174