京尼平甙调节GSK3β以抑制Th17分化并减轻颅内动脉瘤的内皮损伤

IF 6.1 2区 医学 Q1 CHEMISTRY, MEDICINAL Phytotherapy Research Pub Date : 2024-08-24 DOI:10.1002/ptr.8320
Qian Zhang, Lu-Feng Shi, Run-Dong Chen, He-He Zhao, Cong Yu, Yi-Rong Wang, Peng Lu
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引用次数: 0

摘要

颅内动脉瘤(IA)是一种常见的脑血管疾病。免疫系统紊乱和内皮功能障碍是其发病的重要机制。吉尼泊苷对内皮细胞和心脑血管疾病具有保护作用,本研究旨在探讨吉尼泊苷对颅内动脉瘤的治疗效果和机制。在右脑基底节注射弹性蛋白酶进行干预后,对IA小鼠模型腹腔注射基尼泊苷2周。通过对威利斯环血管组织进行病理测试和转录组测序分析,评估了基尼泊甙治疗内脏癌的疗效。其主要作用机制与 Th17 细胞中 GSK3β 的表达有关。Gen能显著抑制IA小鼠脾脏Th17细胞的分化比例,GSK3β/STAT3和其他通路蛋白的表达水平也受到Gen的显著抑制。这些结果表明,Gen能明显抑制Th17细胞的分化比例,而在过表达GSK3B基因后,这种效应被逆转。此外,经Gen处理的Th17分化诱导细胞条件培养基能显著上调小鼠主动脉内皮细胞中紧密连接蛋白ZO-1、Occludin和Claudin-5的表达。给 IA 小鼠服用 GSK3β 抑制剂 Tideglusib 可减轻 IA 疾病的严重程度,并上调主动脉紧密连接蛋白的表达。总之,Gen可通过GSK3β抑制Th17细胞分化,从而减轻内皮细胞损伤并上调紧密连接蛋白的表达。
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Geniposide modulates GSK3β to inhibit Th17 differentiation and mitigate endothelial damage in intracranial aneurysm.

Intracranial aneurysm (IA) is a common cerebrovascular disease. Immune system disorders and endothelial dysfunction are essential mechanisms of its pathogenesis. This study aims to explore the therapeutic effect and mechanism of Geniposide (Gen) on IA, which has a protective impact on endothelial cells and cardiovascular and cerebrovascular diseases. IA mouse models were administered intraperitoneal injections of geniposide for 2 weeks following elastase injection into the right basal ganglia of the brain for intervention. The efficacy of Gen in treating IA was evaluated through pathological testing and transcriptome sequencing analysis of Willis ring vascular tissue. The primary mechanism of action was linked to the expression of GSK3β in Th17 cells. The percentage of splenic Th17 cell differentiation in IA mice was significantly inhibited by Gen. GSK3β/STAT3, and other pathway protein expression levels were also significantly inhibited by Gen. Additionally, TNF-α and IL-23 cytokine contents were significantly downregulated after Gen treatment. These results indicated that Gen significantly inhibited the percentage of Th17 cell differentiation, an effect that was reversed upon overexpression of the GSK3B gene. Furthermore, Gen-treated, Th17 differentiation-inducing cell-conditioned medium significantly up-regulated the expression of tight junction proteins ZO-1, Occludin, and Claudin-5 in murine aortic endothelial cells. Administering the GSK3β inhibitor Tideglusib to IA mice alleviated the severity of IA disease pathology and up-regulated aortic tight junction protein expression. In conclusion, Gen inhibits Th17 cell differentiation through GSK3β, which reduces endothelial cell injury and up-regulates tight junction protein expression.

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来源期刊
Phytotherapy Research
Phytotherapy Research 医学-药学
CiteScore
12.80
自引率
5.60%
发文量
325
审稿时长
2.6 months
期刊介绍: Phytotherapy Research is an internationally recognized pharmacological journal that serves as a trailblazing resource for biochemists, pharmacologists, and toxicologists. We strive to disseminate groundbreaking research on medicinal plants, pushing the boundaries of knowledge and understanding in this field. Our primary focus areas encompass pharmacology, toxicology, and the clinical applications of herbs and natural products in medicine. We actively encourage submissions on the effects of commonly consumed food ingredients and standardized plant extracts. We welcome a range of contributions including original research papers, review articles, and letters. By providing a platform for the latest developments and discoveries in phytotherapy, we aim to support the advancement of scientific knowledge and contribute to the improvement of modern medicine.
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