缺血/再灌注损伤诱导的 GPX4 启动子超甲基化可调控肝细胞铁凋亡

IF 3.1 3区 医学 Q2 GASTROENTEROLOGY & HEPATOLOGY
Chen Bai, Peilun Xiao, Yuting Chen, Fangfang Chu, Yue Jiao, Jiaqi Fan, Yuexia Zhang, Jiao Liu, Jiying Jiang, Shuna Yu
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引用次数: 0

摘要

背景和目的:谷胱甘肽过氧化物酶 4(GPX4)是参与缺血再灌注损伤的铁变态反应的关键因素。然而,人们对其在肝缺血再灌注损伤(HIRI)中的作用知之甚少。本研究旨在探讨 GPX4 甲基化在 HIRI 期间的铁凋亡中的作用:在体外实验中,建立了缺氧和缺糖细胞模型。在体内实验中,通过对小鼠进行模拟 HIRI,建立了缺血再灌注模型。然后评估了铁突变的发生、GPX4 启动子甲基化和全局甲基化水平:结果:在缺氧和缺糖的情况下观察到了铁中毒,其特点是细胞活力显著下降(P < 0.05)、脂质过氧化增加(P < 0.01)、铁过载(P < 0.05)和 GPX4 下调(P < 0.05)。GPX4 基因敲除(P<0.01)会加剧这种铁变态反应,而外源性谷胱甘肽(P<0.01)则会减轻铁变态反应。同样,HIRI 对小鼠的铁变态反应也很明显,GPX4 mRNA 和蛋白质表达下调(均 P < 0.01),酰基-CoA 合成酶长链家族成员 4 mRNA 和蛋白质上调(均 P < 0.01),前列腺素内过氧化物合成酶 2 mRNA 和蛋白质表达也上调(均 P < 0.05)。甲基化水平增加,表现为DNA甲基化转移酶表达上调(P<0.05)和Ten-eleven易位家族去甲基化酶下调(P<0.01),以及GPX4启动子甲基化上调:结论:缺血再灌注损伤后肝细胞的主要细胞死亡模式可能是铁氧化。GPX4启动子的甲基化和肝脏整体甲基化水平的升高参与了铁跃迁的调控。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
GPX4 Promoter Hypermethylation Induced by Ischemia/Reperfusion Injury Regulates Hepatocytic Ferroptosis.

Background and aims: Glutathione peroxidase 4 (GPX4) is a key factor in ferroptosis, which is involved in ischemia-reperfusion injury. However, little is known about its role in hepatic ischemia-reperfusion injury (HIRI). This study aimed to investigate the role of GPX4 methylation in ferroptosis during HIRI.

Methods: For the in vitro experiments, an oxygen and glucose deprivation cell model was established. For the in vivo experiments, an ischemia-reperfusion model was created by subjecting mice to simulated HIRI. Ferroptosis occurrence, GPX4 promoter methylation, and global methylation levels were then assessed.

Results: Ferroptosis was observed in oxygen and glucose deprivation, characterized by a significant decrease in cellular viability (P < 0.05), an increase in lipid peroxidation (P < 0.01), iron overload (P < 0.05), and down-regulation of GPX4 (P < 0.05). This ferroptosis was exacerbated by GPX4 knockdown (P < 0.01) and mitigated by exogenous glutathione (P < 0.01). Similarly, ferroptosis was evident in mice subjected to HIRI, with a down-regulation of GPX4 mRNA and protein expression (all P < 0.01), and an upregulation of acyl-CoA synthetase long-chain family member 4 mRNA and protein (all P < 0.01), as well as prostaglandin-endoperoxide synthase 2 mRNA and protein expression (all P < 0.05). Methylation levels increased, evidenced by upregulation of DNA methylation transferase expression (P < 0.05) and down-regulation of Ten-eleven translocation family demethylases (P < 0.01), along with an upregulation of GPX4 promoter methylation.

Conclusions: Ferroptosis may be the primary mode of cell death in hepatocytes following ischemia-reperfusion injury. The methylation of the GPX4 promoter and elevated levels of global hepatic methylation are involved in the regulation of ferroptosis.

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来源期刊
Journal of Clinical and Translational Hepatology
Journal of Clinical and Translational Hepatology GASTROENTEROLOGY & HEPATOLOGY-
CiteScore
6.40
自引率
2.80%
发文量
496
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