[Cimifugin通过抑制MAPK通路调节th细胞免疫平衡，改善小鼠克罗恩病样结肠炎]。

Q3 Medicine

南方医科大学学报杂志 Pub Date : 2025-03-20 DOI:10.12122/j.issn.1673-4254.2025.03.17

Lixia Yin, Minzhu Niu, Keni Zhang, Zhijun Geng, Jianguo Hu, Jiangyan Li, Jing Li

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Intestinal barrier integrity in the mice was assessed using immunofluorescence assay and Western blotting for claudin-1 and ZO-1; T-helper (Th) cell subset ratios in the mesenteric lymph nodes were analyzed with flow cytometry. Network pharmacology, KEGG enrichment analysis and molecular docking were used to predict the targets of cimifugin and analyze the key pathways and cimifugin-MAPK protein interactions, which were validated by Western blotting in the mouse models.Results: In mice with TNBS-induced colitis, cimifugin treatment significantly attenuated body weight loss and colon shortening, lowered DAI and histopathological scores, decreased IFN-γ and IL-17 levels, and increased IL-4 and IL-10 levels in the colonic mucosa. 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引用次数: 0

摘要

目的：探讨cimifugin对小鼠克罗恩病（CD）样结肠炎的治疗作用及其可能机制。方法：将30只成年雄性C57BL/6小鼠随机分为对照组、2,4,6-三硝基苯磺酸（TNBS）致cd样结肠炎模型组和cimifugin治疗组（每日12.5 mg/kg灌胃）。通过观察体重、疾病活动指数（DAI）评分、结肠长度、组织病理学炎症评分和结肠黏膜炎症细胞因子水平的变化来评价cimifugin的治疗效果。采用免疫荧光法和免疫印迹法检测小鼠肠屏障的完整性，检测claudin-1和ZO-1；流式细胞术分析肠系膜淋巴结t辅助细胞（Th）亚群比例。利用网络药理学、KEGG富集分析、分子对接等方法预测cimifugin的作用靶点，分析关键通路及cimifugin与mapk蛋白的相互作用，并在小鼠模型中进行Western blotting验证。结果：在tnbs诱导的结肠炎小鼠中，cimifugin治疗显著减轻了体重减轻和结肠缩短，降低了DAI和组织病理学评分，降低了IFN-γ和IL-17水平，增加了结肠黏膜IL-4和IL-10水平。Cimifugin还显著改善tnbs诱导的小鼠结肠杯状细胞claudin-1脱位和减少，上调claudin-1和ZO-1表达，降低Th1和Th17细胞百分比，增加Th2和Treg细胞百分比。KEGG分析提示cimifugin的作用可能与MAPK信号传导有关，分子对接显示cimifugin与MAPK核心蛋白具有较强的结合亲和力。Western blotting结果显示，cimifigin处理的小鼠模型结肠黏膜中JNK、ERK和p38的磷酸化水平显著降低。结论：Cimifugin可通过抑制MAPK通路激活，修复肠屏障损伤，恢复Th1/Th2和Th17/Treg平衡，从而减轻tnbs诱导的cd样结肠炎。

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[Cimifugin ameliorates Crohn's disease-like colitis in mice by modulating Th-cell immune balance via inhibiting the MAPK pathway].

Objectives: To investigate the therapeutic effects of cimifugin on Crohn's disease (CD)-like colitis in mice and its possible mechanism.

Methods: Thirty adult male C57BL/6 mice were randomized equally into control group, 2,4,6-trinitrobenzenesulfonic acid (TNBS)-induced CD-like colitis model group, and cimifugin treatment (daily gavage at 12.5 mg/kg) group. The therapeutic effect of cimifugin was evaluated by observing changes in body weight, disease activity index (DAI) scores, colon length, histopathological inflammation scores, and inflammatory cytokine levels in the colonic mucosa. Intestinal barrier integrity in the mice was assessed using immunofluorescence assay and Western blotting for claudin-1 and ZO-1; T-helper (Th) cell subset ratios in the mesenteric lymph nodes were analyzed with flow cytometry. Network pharmacology, KEGG enrichment analysis and molecular docking were used to predict the targets of cimifugin and analyze the key pathways and cimifugin-MAPK protein interactions, which were validated by Western blotting in the mouse models.

Results: In mice with TNBS-induced colitis, cimifugin treatment significantly attenuated body weight loss and colon shortening, lowered DAI and histopathological scores, decreased IFN-γ and IL-17 levels, and increased IL-4 and IL-10 levels in the colonic mucosa. Cimifugin treatment also significantly improved TNBS-induced claudin-1 dislocation and reduction of goblet cells, upregulated claudin-1 and ZO-1 expressions, reduced Th1 and Th17 cell percentages, and increased Th2 and Treg cell percentages in the colonic mucosa of the mice. KEGG analysis suggested a possible connection between the effect of cimifugin and MAPK signaling, and molecular docking showed strong binding affinity between cimifugin and MAPK core proteins. Western blotting demonstrated significantly decreased phosphorylation levels of JNK, ERK, and p38 in the colonic mucosa of cimifugin-treated mouse models.

Conclusions: Cimifugin alleviates TNBS-induced CD-like colitis by repairing intestinal barrier damage and restoring Th1/Th2 and Th17/Treg balance via suppressing MAPK pathway activation.

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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：