Integrated hepatic ferroptosis gene signature dictates pathogenic features of ferroptosis.

IF 5.6 2区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Hepatology Communications Pub Date : 2025-05-29 eCollection Date: 2025-06-01 DOI:10.1097/HC9.0000000000000721

Takashi Matsumoto, Akihiro Nita, Yohei Kanamori, Ayato Maeda, Tomomi Nita, Noriko Yasuda-Yoshihara, Kosuke Mima, Hirohisa Okabe, Katsunori Imai, Hiromitsu Hayashi, Yuta Matsuoka, Katsuya Nagaoka, Keiichi I Nakayama, Yuki Sugiura, Yasuhito Tanaka, Hideo Baba, Toshiro Moroishi

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Abstract

Background: Ferroptosis, a distinctive form of cell death induced by iron-dependent lipid peroxidation, is implicated in various biological processes, including liver diseases. Establishing an iron overload-induced ferroptosis model and identifying hepatic gene signatures associated with ferroptosis are crucial for understanding its role in liver pathogenesis.

Methods: F-box and leucine-rich repeat protein 5 (FBXL5) is a substrate-recognition component of the SCF E3 ligase complex that restricts intracellular iron levels. In this study, we used liver-specific Fbxl5-null mice to establish an iron overload-induced ferroptosis model. Transcriptome analysis identified genes involved in hepatic ferroptosis. Integrating these gene signatures with another ferroptosis model enabled the assessment of ferroptosis-related pathology in murine liver injury models and in 174 patients undergoing liver resection surgery.

Results: Iron overload induced severe liver damage in liver-specific Fbxl5-null mice, characterized by elevated liver enzymes, histopathological changes, and lipid peroxidation. Transcriptome analysis revealed a distinct set of genes associated with hepatic ferroptosis response. Generating a gene signature for evaluating ferroptosis enhanced the understanding of ferroptosis-related pathologies in liver diseases. Iron overload exacerbated liver damage in murine ischemia-reperfusion injury models via ferroptosis induction. In human patients, elevated serum iron levels correlated with sustained postoperative liver damage, indicating heightened susceptibility to ferroptosis.

Conclusions: Here, a murine model of iron overload-induced hepatic ferroptosis was established, and a gene signature indicative of hepatic ferroptosis response in both mice and humans was identified. These findings underscore the role of ferroptosis in liver injury progression and suggest potential therapeutic targets for liver disease intervention.

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整合的肝铁下垂基因特征决定了铁下垂的致病特征。

背景：铁下垂是由铁依赖性脂质过氧化引起的一种独特的细胞死亡形式，涉及多种生物过程，包括肝脏疾病。建立铁超载诱导的铁下垂模型并确定与铁下垂相关的肝脏基因特征对于了解其在肝脏发病机制中的作用至关重要。方法：F-box和富亮氨酸重复蛋白5 （FBXL5）是限制细胞内铁水平的SCF E3连接酶复合物的底物识别成分。在本研究中，我们使用肝脏特异性fbx15缺失小鼠建立铁超载诱导的铁下垂模型。转录组分析确定了与肝铁下垂有关的基因。将这些基因特征与另一种铁下垂模型相结合，可以在小鼠肝损伤模型和174例肝切除手术患者中评估铁下垂相关病理。结果：铁超载导致肝脏特异性fbx15缺失小鼠严重肝损伤，表现为肝酶升高、组织病理改变和脂质过氧化。转录组分析揭示了一组与肝铁下垂反应相关的独特基因。产生一个用于评估铁中毒的基因标记增强了对肝脏疾病中铁中毒相关病理的理解。铁超载通过诱导铁下垂加重小鼠缺血再灌注损伤模型的肝损伤。在人类患者中，血清铁水平升高与术后持续肝损伤相关，表明对铁下垂的易感性增加。结论：本研究建立了铁超载诱导的小鼠肝铁下垂模型，并鉴定了小鼠和人类肝铁下垂反应的基因标记。这些发现强调了铁下垂在肝损伤进展中的作用，并提出了肝脏疾病干预的潜在治疗靶点。

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来源期刊

Hepatology Communications GASTROENTEROLOGY & HEPATOLOGY-

CiteScore

8.00

自引率

2.00%

发文量

248

审稿时长

8 weeks

期刊介绍： Hepatology Communications is a peer-reviewed, online-only, open access journal for fast dissemination of high quality basic, translational, and clinical research in hepatology. Hepatology Communications maintains high standard and rigorous peer review. Because of its open access nature, authors retain the copyright to their works, all articles are immediately available and free to read and share, and it is fully compliant with funder and institutional mandates. The journal is committed to fast publication and author satisfaction.