ISG15 deficiency in hepatic stellate cells promotes TGFβ2-induced liver fibrosis by counteracting CREB1 ISGylation.

IF 25.8 1区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Gut Pub Date : 2025-08-17 DOI:10.1136/gutjnl-2025-335327

Yue Yuan, Jiaxuan Li, Dean Rao, Xun Lu, Min Chen, Xiaoping Chen, Xin Long, Bixiang Zhang, Huifang Liang, Qian Chen, Jianping Zhao

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Abstract

Background: Interferon (IFN)-stimulated gene 15 (ISG15) is a downstream molecule of the IFN pathways central to many cellular processes. ISG15 mainly exerts its function through a post-translational modification process known as ISGylation.

Objective: In this study, the role of ISG15 in the activation of hepatic stellate cells (HSCs) and liver fibrosis was examined.

Design: Liver fibrosis was established by carbon tetrachloride (CCl4), bile duct ligation (BDL) surgery and metabolic dysfunction-associated steatohepatitis (MASH) diet between HSC-specific deletion of ISG15 (ISG15cKO) and wild type mice. Using genetic strategies in vitro, the role of ISG15 in HSCs was established. Immunoprecipitation, luciferase reporter assays and chromatin-immunoprecipitation assays (ChIP) in combination with proteomics sequencing in HSCs were used to study the associated downstream mechanisms.

Results: ISG15 was underexpressed in activated HSCs and fibrotic livers, showing an inverse correlation with α-smooth muscle actin in patients with liver fibrosis. ISG15cKO mice developed spontaneous hepatic fibrosis and showed exacerbated CCl4/BDL-induced fibrogenesis. In vitro, ISG15 modulated HSC activation, proliferation and excessive extracellular matrix production. ISG15 deficiency in HSCs promoted transforming growth factorβ2 (TGFβ2) transcription by enhancing phosphorylated cAMP responsive element binding protein 1 (CREB1) activity, thereby inducing CREB1 binding on TGFβ2 promoter regions to activate TGFβ2/SMAD2 signalling. ISGylation directly binds CREB1 on Lys-304 and Lys-305 to inhibit p-CREB1 activity. Overexpression of ISG15 in HSCs or pharmacological inhibition of CREB1 by 666-15 could abolish ISG15 deficiency-induced liver fibrosis in CCl4-treated mice.

Conclusions: ISG15 regulated HSC activation and liver fibrosis in part via the CREB1/TGFβ2/SMAD2 regulatory pathway. Utilisation of ISG15-CREB1 signalling may be a potential therapeutic target for liver fibrosis.

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肝星状细胞ISG15缺乏通过对抗CREB1 isg酰化促进tgf - β2诱导的肝纤维化。

背景：干扰素（IFN）刺激基因15 （ISG15）是IFN通路的下游分子，对许多细胞过程至关重要。ISG15主要通过翻译后修饰过程isg酰化发挥作用。目的：探讨ISG15在肝星状细胞（HSCs）活化及肝纤维化中的作用。设计：通过四氯化碳（CCl4）、胆管结扎（BDL）手术和代谢功能障碍相关脂肪性肝炎（MASH）饮食，在造血干细胞特异性缺失ISG15 （ISG15cKO）和野生型小鼠之间建立肝纤维化。利用体外遗传策略，我们确定了ISG15在造血干细胞中的作用。利用免疫沉淀法、荧光素酶报告基因法和染色质免疫沉淀法（ChIP）结合造血干细胞的蛋白质组学测序，研究相关的下游机制。结果：ISG15在活化的hsc和纤维化肝中低表达，与肝纤维化患者α-平滑肌肌动蛋白呈负相关。ISG15cKO小鼠发生自发性肝纤维化，并表现出CCl4/ bdl诱导的纤维化加剧。在体外，ISG15可调节HSC的活化、增殖和过量的细胞外基质生成。hsc中ISG15缺失通过增强磷酸化cAMP响应元件结合蛋白1 （CREB1）活性，促进转化生长因子β2 （tgf - β2）转录，从而诱导CREB1结合tgf - β2启动子区域，激活tgf - β2/SMAD2信号传导。ISGylation直接结合Lys-304和Lys-305上的CREB1抑制p-CREB1活性。在造血干细胞中过度表达ISG15或666-15对CREB1的药理学抑制可以消除ccl4处理小鼠中ISG15缺陷诱导的肝纤维化。结论：ISG15部分通过CREB1/ tgf - β2/SMAD2调控途径调控HSC活化和肝纤维化。利用ISG15-CREB1信号可能是肝纤维化的潜在治疗靶点。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Gut 医学-胃肠肝病学

CiteScore

45.70

自引率

2.40%

发文量

284

审稿时长

1.5 months

期刊介绍： Gut is a renowned international journal specializing in gastroenterology and hepatology, known for its high-quality clinical research covering the alimentary tract, liver, biliary tree, and pancreas. It offers authoritative and current coverage across all aspects of gastroenterology and hepatology, featuring articles on emerging disease mechanisms and innovative diagnostic and therapeutic approaches authored by leading experts. As the flagship journal of BMJ's gastroenterology portfolio, Gut is accompanied by two companion journals: Frontline Gastroenterology, focusing on education and practice-oriented papers, and BMJ Open Gastroenterology for open access original research.