抑制铁蛋白沉积可预防肥胖小鼠脂肪肝的恶化

IF 6 2区医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Antioxidants Pub Date : 2024-10-31 DOI:10.3390/antiox13111336

Gi Cheol Park, Soo-Young Bang, Ji Min Kim, Sung-Chan Shin, Yong-Il Cheon, Kwang Min Kim, Hanaro Park, Eui-Suk Sung, Minhyung Lee, Jin-Choon Lee, Byung-Joo Lee

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引用次数: 0

摘要

铁变态反应是一种以脂质过氧化和铁积累为特征的调节性细胞死亡形式，它与肥胖症中代谢功能障碍相关性脂肪性肝炎（MASH）的进展有关。本研究调查了铁蛋白沉积在肥胖小鼠肝脂肪变性和 MASH 发病过程中的作用，并评估了铁蛋白沉积抑制剂 ferrostatin-1 的治疗潜力。C57BL/6J 野生型小鼠（n = 8）和肥胖/肥胖小鼠（n = 16）以标准饲料饲养。小鼠被分为三组，包括 C57BL/6（n = 8）、ob/ob（n = 8）和ob/ob + ferrostatin-1 (FER)（n = 8），后一组每周三次腹腔注射 5 μM/kg ferrostatin，持续八周。治疗后，收集血清和组织样本进行分析。在肥胖/ob小鼠中观察到明显的肝脏脂肪变性和脂肪生成标志物增加，而在接受铁前列素-1治疗的肥胖/ob + FER组中，这些指标恢复到基线水平。肥胖/ob组的活性氧（ROS）和丙二醛（MDA）水平升高，表明氧化应激升高，而谷胱甘肽过氧化物酶4（GPX4）活性显著降低。铁前列素-1可降低MDA水平并恢复GPX4的活性。此外，铁前列素还能减轻铁超载，促进巨噬细胞从M1极化到M2，从而减轻肝脏炎症和纤维化。铁前列素治疗可逆转肥胖/肥胖小鼠的线粒体功能障碍。我们的研究结果表明，铁蛋白沉积症在肥胖发展为肝脂肪变性和 MASH 的过程中起着重要作用。使用铁前列素-1抑制高铁血症可有效改善肝脏组织学、减少氧化应激、使脂肪生成正常化并调节巨噬细胞极化。这项研究强调了以铁蛋白沉积为靶点作为肥胖相关肝病治疗策略的潜力，值得在临床环境中进一步研究。

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Inhibiting Ferroptosis Prevents the Progression of Steatotic Liver Disease in Obese Mice.

Ferroptosis, a form of regulated cell death characterized by lipid peroxidation and iron accumulation, has been implicated in the progression of metabolic-dysfunction-associated steatohepatitis (MASH) in obesity. This study investigated the role of ferroptosis in the development of hepatic steatosis and MASH in obese mice and assessed the therapeutic potential of ferrostatin-1, a ferroptosis inhibitor. C57BL/6J wild-type (n = 8) and ob/ob mice (n = 16) were maintained on a standard chow diet. Mice were divided into three groups that included C57BL/6 (n = 8), ob/ob (n = 8), and ob/ob + ferrostatin-1 (FER) (n = 8), with the latter group receiving an intraperitoneal injection of 5 μM/kg ferrostatin three times per week for eight weeks. Following treatment, serum and tissue samples were collected for analysis. Significant hepatic steatosis and increased lipogenesis markers were observed in ob/ob mice, which were restored to baseline levels in the ob/ob + FER group treated with ferrostatin-1. Elevated oxidative stress was indicated by increased reactive oxygen species (ROS) and malondialdehyde (MDA) levels in the ob/ob group, while glutathione peroxidase 4 (GPX4) activity was significantly reduced. Ferrostatin-1 treatment decreases MDA levels and restores GPX4 activity. Additionally, ferrostatin mitigates iron overload and promotes macrophage polarization from M1 to M2, thereby reducing liver inflammation and fibrosis. Ferrostatin treatment reversed mitochondrial dysfunction in ob/ob mice. Our findings revealed that ferroptosis plays a significant role in the progression of obesity to hepatic steatosis and MASH. Inhibiting ferroptosis using ferrostatin-1 effectively improves liver histology, reduces oxidative stress, normalizes lipogenesis, and modulates macrophage polarization. This study highlights the potential of targeting ferroptosis as a therapeutic strategy for obesity-related liver diseases, warranting further investigation in clinical settings.

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来源期刊

Antioxidants Biochemistry, Genetics and Molecular Biology-Physiology

CiteScore

10.60

自引率

11.40%

发文量

2123

审稿时长

16.3 days

期刊介绍： Antioxidants (ISSN 2076-3921), provides an advanced forum for studies related to the science and technology of antioxidants. It publishes research papers, reviews and communications. Our aim is to encourage scientists to publish their experimental and theoretical results in as much detail as possible. There is no restriction on the length of the papers. The full experimental details must be provided so that the results can be reproduced. Electronic files and software regarding the full details of the calculation or experimental procedure, if unable to be published in a normal way, can be deposited as supplementary electronic material.