龙胆苦苷改善DDC诱导的小鼠胆管疾病模型中的导管反应和炎症反应。

Current molecular pharmacology Pub Date : 2023-10-19 DOI:10.2174/0118761429251911231011092145

Juan Hao, Jian Wu, Quanjun Yang, Kan Lu, Yi Xu, Yiyue Chen, Jibo Liu, Xiaohong Shao, Chunling Zhu, Yaqin Ding, Xin Xie

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引用次数: 0

摘要

背景：胆管疾病包括一系列没有治疗方法的疾病。基于胆汁酸（BA）代谢调节的药理学治疗代表了治疗胆管疾病的有前景的治疗策略。龙胆苦苷（GPS）来源于中草药龙胆，具有调节胆汁酸代谢和氧化应激的药理作用。目的：本研究旨在探讨GPS对3,5-二乙氧羰基-1,4-二氢吡啶（DDC）诱导的胆管病变的影响。方法：设计两个独立的动物实验来评估GPS对DDC饮食诱导的慢性胆管疾病的综合作用，包括胆管闭塞、导管反应、BA代谢重编程、肝纤维化、氧化应激和炎症反应。结果：在第一个药理学实验中，向喂食DDC饮食的小鼠腹膜内注射三个剂量的GPS（5、25和125mg/kg），持续14天。DDC诱导了典型的导管反应，增加了导管周围纤维化和门区混合炎症细胞浸润。GPS治疗显示出导管反应、BA代谢、纤维化、氧化应激和炎症反应的剂量依赖性改善。在第二个实验中，将高剂量的GPS腹膜内注射到对照小鼠中28天，导致肝功能没有明显的组织学变化和显著的血清学异常。然而，GPS抑制DDC诱导的氧化应激、血清和肝脏BA积累、促炎细胞因子产生和免疫细胞浸润。具体而言，GPS处理组显示单核细胞衍生的巨噬细胞、CD4+和CD8+T淋巴细胞以及保存的库普弗细胞的浸润减少。结论：GPS通过改善导管反应、导管周围纤维化、氧化应激和炎症反应，减轻了DDC饮食诱导的慢性胆管疾病。其剂量依赖性药理作用表明，GPS值得在胆管病的临床试验中进一步评估。

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Gentiopicroside Ameliorated Ductular Reaction and Inflammatory Response in DDC-induced Murine Cholangiopathies Model.

Background: Cholangiopathies comprise a spectrum of diseases without curative treatments. Pharmacological treatments based on bile acid (BA) metabolism regulation represent promising therapeutic strategies for the treatment of cholangiopathies. Gentiopicroside (GPS), derived from the Chinese medicinal herb Gentianae Radix, exerts pharmacological effects on bile acid metabolism regulation and oxidative stress.

Objective: The present study aims to investigate the effect of GPS on 3,5-diethoxycarbonyl-1,4dihydrocollidine (DDC)-induced cholangiopathy.

Methods: Two independent animal experiments were designed to evaluate the comprehensive effect of GPS on chronic DDC diet-induced cholangiopathy, including bile duct obliteration, ductular reaction, BA metabolism reprogramming, liver fibrosis, oxidative stress and inflammatory responses.

Results: In the first pharmacological experiment, three doses of GPS (5, 25 and 125 mg/kg) were injected intraperitoneally into mice fed a DDC diet for 14 days. DDC induced a typical ductular reaction, increased periductal fibrosis and mixed inflammatory cell infiltration in the portal areas. GPS treatment showed dose-dependent improvements in the ductular reaction, BA metabolism, fibrosis, oxidative stress and inflammatory response. In the second experiment, a high dose of GPS was injected intraperitoneally into control mice for 28 days, resulting in no obvious histologic changes and significant serologic abnormalities in liver function. However, GPS inhibited DDC-induced oxidative stress, serum and hepatic BA accumulation, proinflammatory cytokine production, and immunocyte infiltration. Specifically, the GPS-treated groups showed decreased infiltration of monocyte-derived macrophages and CD4+ and CD8+ T lymphocytes, as well as preserved Kupffer cells.

Conclusion: GPS alleviated chronic DDC diet-induced cholangiopathy disorder by improving the ductular reaction, periductal fibrosis, oxidative stress and inflammatory response. Its dosage-dependent pharmacological effects indicated that GPS warrants its further evaluation in clinical trials for cholangiopathy.

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Current molecular pharmacology

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