[复方积雪草方通过调节TLR4/MyD88通路抑制炎症-纤维化级联减轻日本血吸虫诱导小鼠肝纤维化]。

Q3 Medicine

南方医科大学学报杂志 Pub Date : 2025-06-20 DOI:10.12122/j.issn.1673-4254.2025.06.20

Liping Guan, Yan Yan, Xinyi Lu, Zhifeng Li, Hui Gao, Dong Cao, Chenxi Hou, Jingyu Zeng, Xinyi Li, Yang Zhao, Junjie Wang, Huilong Fang

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For experimental validation of the results, 36 mice were divided into control group, Sj-infected model group, and CCA-treated groups. In the latter two groups, liver fibrosis was induced via abdominal infection with Sj cercariae for 8 weeks, followed by 8 weeks of daily treatment with CCA decoction or saline. Hepatic pathology of the mice was assessedwith HE and Masson staining, and hepatic expressions of collagen-I and collagen-III were detected using immunohistochemistry; serum IL-6 and TNF-α levels were determined with ELISA. Hepatic expressions of TLR4 and MyD88 proteins were analyzed with Western blotting.Results: We identified a total of 107 bioactive CCA components and 791 targets, including 37 intersection targets linked to Sj-induced fibrosis. The core targets included TNF, TP53, JUN, MMP9, and CXCL8, involving the IL-17 signaling, lipid metabolism, TLR4/MyD88 axis, and cancer pathways. 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引用次数: 0

摘要

目的：探讨复方积雪草方（CCA）减轻日本血吸虫（Sj）致小鼠肝纤维化的作用机制。方法：利用TCMSP数据库与sj相关肝纤维化靶点交叉分析，鉴定CCA的有效成分和靶点。利用Cytoscape 3.9.1构建“药物组分-靶标-通路-疾病”网络。使用DAVID进行功能富集分析（GO/KEGG）。通过分子对接研究验证核心靶点与关键化合物之间的相互作用。为验证实验结果，将36只小鼠分为对照组、sj感染模型组和cca治疗组。后两组小鼠腹腔感染Sj尾蚴诱导肝纤维化，连续8周，每日给予CCA汤或生理盐水治疗8周。采用HE、Masson染色法观察小鼠肝脏病理变化，免疫组化法检测肝脏胶原蛋白i、胶原蛋白iii的表达；ELISA法检测血清IL-6、TNF-α水平。Western blotting分析肝脏TLR4和MyD88蛋白的表达。结果：我们共鉴定出107种生物活性CCA成分和791个靶点，包括37个与sj诱导纤维化相关的交叉靶点。核心靶点包括TNF、TP53、JUN、MMP9和CXCL8，涉及IL-17信号、脂质代谢、TLR4/MyD88轴和癌症通路。分子对接研究证实槲皮素（CCA主要成分）与TNF/TP53/JUN/MMP9具有较强的结合亲和力。在sj感染小鼠模型中，CCA治疗显著减轻肝脏炎症细胞浸润，减少胶原-i和胶原- iii沉积，改善组织结构，降低血清IL-6和TNF-α水平，下调肝脏中TLR4和MyD88的表达。结论：CCA通过靶向TNF、TP53、JUN、MMP9调节TLR4/MyD88通路，从而抑制促炎细胞因子释放，抑制肝星状细胞活化，减少胶原沉积，防止肝脏肉芽肿形成，减轻sj诱导的肝纤维化。

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[Compound Centella asiatica formula alleviates Schistosoma japonicum-induced liver fibrosis in mice by inhibiting the inflammation-fibrosis cascade via regulating the TLR4/MyD88 pathway].

Objectives: To explore the therapeutic mechanism of compound Centella asiatica formula (CCA) for alleviating Schistosoma japonicum (Sj)-induced liver fibrosis in mice.

Methods: The active components and targets of CCA were identified using the TCMSP database with cross-analysis of Sj-related liver fibrosis targets. A "drug-component-target-pathway-disease" network was constructed using Cytoscape 3.9.1. Functional enrichment analysis (GO/KEGG) was performed using DAVID. Molecular docking study was carried out to validate interactions between the core targets and the key compounds. For experimental validation of the results, 36 mice were divided into control group, Sj-infected model group, and CCA-treated groups. In the latter two groups, liver fibrosis was induced via abdominal infection with Sj cercariae for 8 weeks, followed by 8 weeks of daily treatment with CCA decoction or saline. Hepatic pathology of the mice was assessedwith HE and Masson staining, and hepatic expressions of collagen-I and collagen-III were detected using immunohistochemistry; serum IL-6 and TNF-α levels were determined with ELISA. Hepatic expressions of TLR4 and MyD88 proteins were analyzed with Western blotting.

Results: We identified a total of 107 bioactive CCA components and 791 targets, including 37 intersection targets linked to Sj-induced fibrosis. The core targets included TNF, TP53, JUN, MMP9, and CXCL8, involving the IL-17 signaling, lipid metabolism, TLR4/MyD88 axis, and cancer pathways. Molecular docking study confirmed strong binding affinity between quercetin (a primary CCA component) and TNF/TP53/JUN/MMP9. In Sj-infected mouse models, CCA treatment significantly attenuated hepatic inflammatory cell infiltration, reduced collagen-I and collagen-III deposition, improved tissue architecture, reduced serum IL-6 and TNF-α levels, and downregulated TLR4 and MyD88 expressions in the liver.

Conclusions: CCA mitigates Sj-induced liver fibrosis by targeting TNF, TP53, JUN, and MMP9 to modulate the TLR4/MyD88 pathway, thereby suppressing pro-inflammatory cytokine release, inhibiting hepatic stellate cell activation, reducing collagen deposition, and preventing granuloma formation in the liver.

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来源期刊

南方医科大学学报杂志 Medicine-Medicine (all)

CiteScore

1.50

自引率

0.00%

发文量

208

期刊介绍：