Inhibition of ferroptosis by icariin treatment attenuates excessive ethanol consumption-induced atrial remodeling and susceptibility to atrial fibrillation, role of SIRT1

Inhibition of ferroptosis by icariin treatment attenuates excessive ethanol consumption-induced atrial remodeling and susceptibility to atrial fibrillation, role of SIRT1

Ferroptosis contributes to the pathogenesis of atrial fibrillation (AF), although the mechanisms are still largely uncovered. The current study was designed to explore the pharmacological effects of icariin against ethanol-induced atrial remodeling, if any, and the mechanisms involved with a focus o...

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Veröffentlicht in:Apoptosis (London) 2023-04, Vol.28 (3-4), p.607-626
Hauptverfasser: Yu, Li-Ming, Dong, Xue, Huang, Tao, Zhao, Ji-Kai, Zhou, Zi-Jun, Huang, Yu-Ting, Xu, Yin-Li, Zhao, Qiu-Sheng, Wang, Zhi-Shang, Jiang, Hui, Yin, Zong-Tao, Wang, Hui-Shan
Format: Artikel
Sprache:eng
Schlagworte:
Acetaldehyde
Alcohol
Alcohol, Denatured
Animals
Apoptosis
Atria
Atrial fibrillation
Atrial Fibrillation - chemically induced
Atrial Fibrillation - drug therapy
Atrial Remodeling
Biochemistry
Biomedical and Life Sciences
Biomedicine
Cancer Research
Cardiac arrhythmia
Cell Biology
Damage accumulation
Ethanol
Ethanol - toxicity
Ferroptosis
Fibrillation
GA-binding protein
Health aspects
Mitochondria
Myocytes
Oncology
p53 Protein
Pathogenesis
Risk factors
Signal transduction
Signaling
SIRT1 protein
Sirtuin 1 - genetics
Tumor proteins
Tumor Suppressor Protein p53
Virology
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Zusammenfassung:Ferroptosis contributes to the pathogenesis of atrial fibrillation (AF), although the mechanisms are still largely uncovered. The current study was designed to explore the pharmacological effects of icariin against ethanol-induced atrial remodeling, if any, and the mechanisms involved with a focus on SIRT1 signaling. Excessive ethanol-treated animals were administered with Ferrostatin-1, Erastin or icariin to evaluate the potential effects of icariin or ferroptosis. Then, the underling mechanisms was further explored in the in vitro experiments using HL-1 atrial myocytes. Excessive ethanol administration caused significant atrial damage as evidenced by increased susceptibility to AF, altered atrial conduction pattern, atrial enlargement, and enhanced fibrotic markers. These detrimental effects were reversed by Ferrostatin-1 or icariin treatment, while Erastin co-administration markedly abolished the beneficial actions conferred by icariin. Mechanistically, ethanol-treated atria exhibited markedly up-regulated pro-ferroptotic protein (PTGS2, ACSL4, P53) and suppressed anti-ferroptotic molecules (GPX4, FTH1). Icariin treatment inhibited ethanol-induced atrial ferroptosis by reducing atrial mitochondrial damage, ROS accumulation and iron overload. Interestingly, the in vivo and in vitro data showed that icariin activated atrial SIRT1-Nrf-2-HO-1 signaling pathway, while EX527 not only reversed these effects, but also abolished the therapeutic effects of icariin. Moreover, the stimulatory effects on GPX4, SLC7A11 and the suppressive effects on ACSL4, P53 conferred by icariin were blunted by EX527 treatment. These data demonstrate that ferroptosis plays a causative role in the pathogenesis of ethanol-induced atrial remodeling and susceptibility to AF. Icariin protects against atrial damage by inhibiting ferroptosis via SIRT1 signaling. Its role as a prophylactic/therapeutic drug deserves further clinical study.
ISSN:1360-8185
1573-675X
DOI:10.1007/s10495-023-01814-8