肝星状细胞中整合素α8(ITGA8)缺乏通过抑制COL11A1减轻四氯化碳诱导的肝纤维化。
ITGA8 deficiency in hepatic stellate cells attenuates CCl-Induced liver fibrosis via suppression of COL11A1.
作者信息
Yan Xuzhen, Han Qi, Wu Wenyue, Li Hong, Zhang Wen, Wang Yiwen, Chen Wei, Yang Aiting, You Hong
机构信息
Experimental and Translational Research Center, Beijing Friendship Hospital, Capital Medical University, Beijing, PR China; Beijing Clinical Medicine Institute, Beijing, PR China; National Clinical Research Center of Digestive Diseases, Beijing, PR China.
Liver Research Center & Beijing Key Laboratory of Translational Medicine on Liver Cirrhosis, Beijing Friendship Hospital, Capital Medical University, Beijing, PR China; National Clinical Research Center of Digestive Diseases, Beijing, PR China.
出版信息
Biochem Biophys Res Commun. 2025 Apr 5;756:151522. doi: 10.1016/j.bbrc.2025.151522. Epub 2025 Feb 21.
BACKGROUND AND OBJECTIVE
Liver fibrosis is a pathological process driven by chronic liver injury, characterized by excessive extracellular matrix (ECM) deposition due to hepatic stellate cell (HSC) activation. Integrins are critical regulators of ECM remodeling and HSC activation, yet the role of integrin α8(ITGA8) in liver fibrosis remains unclear. This study aims to investigate the function and underlying mechanisms of HSC-derived ITGA8 in liver fibrosis and evaluate the therapeutic potential of ITGA8-targeted intervention.
METHODS
A CCl-induced mouse liver fibrosis model and public database analysis were used to assess ITGA8 expression and localization in liver fibrosis. AAV2/6-shItga8 was utilized to selectively silence HSC-derived ITGA8, and its effects on HSC activation and ECM accumulation were examined. In addition, in vitro ITGA8 knockdown combined with proteomic analysis was performed to explore the molecular mechanisms linking ITGA8 to ECM remodeling.
RESULTS
ITGA8 expression was significantly upregulated in fibrotic liver tissues across different etiologies, with a strong colocalization with HSCs. Silencing ITGA8 using AAV2/6-shItga8 effectively reduced liver fibrosis, as indicated by decreased hepatic inflammation, lower serum ALT levels, reduced inflammatory cell infiltration, and downregulated expression of pro-inflammatory cytokines. Fibrosis markers, including Sirius Red staining, type I collagen deposition, and α-SMA expression, were all reduced upon Itga8 silencing. Proteomic analysis revealed that ITGA8 regulates liver fibrosis through the ECM-receptor interaction pathway, with COL11A1 identified as a key downstream target. ITGA8 knockdown significantly suppressed COL11A1 expression, and reduced HSC-mediated collagen contraction, suggesting that ITGA8 contributes to ECM cross-linking and fibrosis progression via COL11A1 regulation.
CONCLUSION
This study demonstrates that HSC-derived ITGA8 promotes ECM accumulation and liver fibrosis progression by regulating COL11A1. Targeted silencing of ITGA8 via AAV2/6-shItga8 effectively alleviates liver fibrosis, providing new insights into ITGA8 as a potential therapeutic target for antifibrotic treatment.
背景与目的
肝纤维化是一种由慢性肝损伤驱动的病理过程,其特征是肝星状细胞(HSC)激活导致细胞外基质(ECM)过度沉积。整合素是ECM重塑和HSC激活的关键调节因子,但整合素α8(ITGA8)在肝纤维化中的作用仍不清楚。本研究旨在探讨HSC来源的ITGA8在肝纤维化中的功能及潜在机制,并评估ITGA8靶向干预的治疗潜力。
方法
采用CCl诱导的小鼠肝纤维化模型和公共数据库分析来评估ITGA8在肝纤维化中的表达和定位。利用AAV2/6-shItga8选择性沉默HSC来源的ITGA8,并检测其对HSC激活和ECM积累的影响。此外,进行体外ITGA8敲低并结合蛋白质组学分析,以探索将ITGA8与ECM重塑联系起来的分子机制。
结果
在不同病因的纤维化肝组织中,ITGA8表达显著上调,且与HSC有强烈的共定位。使用AAV2/6-shItga8沉默ITGA8可有效减轻肝纤维化,表现为肝脏炎症减轻、血清ALT水平降低、炎症细胞浸润减少以及促炎细胞因子表达下调。Itga8沉默后,包括天狼星红染色、I型胶原沉积和α-SMA表达在内的纤维化标志物均降低。蛋白质组学分析表明,ITGA8通过ECM-受体相互作用途径调节肝纤维化,COL11A1被确定为关键的下游靶点。ITGA8敲低显著抑制COL11A1表达,并减少HSC介导的胶原收缩,表明ITGA8通过调节COL11A1促进ECM交联和纤维化进展。
结论
本研究表明,HSC来源的ITGA8通过调节COL11A1促进ECM积累和肝纤维化进展。通过AAV2/6-shItga8靶向沉默ITGA8可有效减轻肝纤维化,为ITGA8作为抗纤维化治疗的潜在靶点提供了新的见解。
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