栀子苷 F1 和瑞香素通过 PI3K/AKT 或 ERK1/2 信号通路保护血管内皮细胞免受缺氧诱导的细胞凋亡。

Kaji-Ichigoside F1 and Rosamultin Protect Vascular Endothelial Cells against Hypoxia-Induced Apoptosis via the PI3K/AKT or ERK1/2 Signaling Pathway.

机构信息

Department of Pharmacy, Logistics University of Chinese People's Armed Police Forces, Tianjin 300309, China.

Medical Team, Zhoukou Detachment of Chinese People's Armed Police Forces, Henan 466000, China.

出版信息

Oxid Med Cell Longev. 2020 Apr 12;2020:6837982. doi: 10.1155/2020/6837982. eCollection 2020.

DOI:10.1155/2020/6837982

PMID:32318240

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7153006/

Abstract

As a pair of differential isomers, Kaji-ichigoside F1 and Rosamultin are both pentacyclic triterpenoids isolated from the subterranean root of L., a plant used in folk medicine in western China as antihypoxia and anti-inflammatory treatments. We demonstrated that Kaji-ichigoside F1 and Rosamultin effectively prevented hypoxia-induced apoptosis in vascular endothelial cells. We established a hypoxia model, using EA.hy926 cells, to further explore the mechanisms. Hypoxia promoted the phosphorylation of AKT, ERK1/2, and NF-B. In hypoxic cells treated with Kaji-ichigoside F1, p-ERK1/2 and p-NF-B levels were increased, while the level of p-AKT was decreased. Treatment with Rosamultin promoted phosphorylation of ERK1/2, NF-B, and AKT in hypoxic cells. Following the addition of LY294002, the levels of p-AKT, p-ERK1/2, and p-NF-B decreased significantly. Addition of PD98059 resulted in reduced levels of p-ERK1/2 and p-NF-B, while p-AKT levels were increased. Pharmacodynamic analysis demonstrated that both LY294002 and PD98059 significantly inhibited the positive effects of Kaji-ichigoside F1 on cell viability during hypoxia, consistent with the results of hematoxylin-eosin (H&E) staining, DAPI staining, and flow cytometry. The antihypoxia effects of Rosamultin were remarkably inhibited by LY294002 but promoted by PD98059. In Kaji-ichigoside F1- and Rosamultin-treated cells, Bcl2 expression was significantly upregulated, while expression of Bax and cytochrome C and levels of cleaved caspase-9 and cleaved caspase-3 were reduced. Corresponding to pharmacodynamic analysis, LY294002 inhibited the regulatory effects of Kaji-ichigoside F1 and Rosamultin on the above molecules, while PD98059 inhibited the regulatory effects of Kaji-ichigoside F1 but enhanced the regulatory effects of Rosamultin. In conclusion, Kaji-ichigoside F1 protected vascular endothelial cells against hypoxia-induced apoptosis by activating the ERK1/2 signaling pathway, which positively regulated the NF-B signaling pathway and negatively regulated the PI3K/AKT signaling pathway. Rosamultin protected vascular endothelial cells against hypoxia-induced apoptosis by activating the PI3K/AKT signaling pathway and positively regulating ERK1/2 and NF-B signaling pathways.

摘要

作为一对差向异构体，Kaji-ichigoside F1 和 Rosamultin 均为五环三萜类化合物，从中国西部民间药物中地下根茎分离得到，用于抗缺氧和抗炎治疗。我们证明了 Kaji-ichigoside F1 和 Rosamultin 可有效预防血管内皮细胞缺氧诱导的凋亡。我们建立了缺氧模型，使用 EA.hy926 细胞，进一步探索其机制。缺氧促进 AKT、ERK1/2 和 NF-B 的磷酸化。在 Kaji-ichigoside F1 处理的缺氧细胞中，p-ERK1/2 和 p-NF-B 水平增加，而 p-AKT 水平降低。Rosamultin 处理促进缺氧细胞中 ERK1/2、NF-B 和 AKT 的磷酸化。加入 LY294002 后，p-AKT、p-ERK1/2 和 p-NF-B 的水平显著降低。加入 PD98059 后，p-ERK1/2 和 p-NF-B 的水平降低，而 p-AKT 的水平升高。药效学分析表明，LY294002 和 PD98059 均显著抑制 Kaji-ichigoside F1 在缺氧时对细胞活力的正向作用，与苏木精-伊红（H&E）染色、DAPI 染色和流式细胞术的结果一致。Rosamultin 的抗缺氧作用显著被 LY294002 抑制，但被 PD98059 促进。在 Kaji-ichigoside F1 和 Rosamultin 处理的细胞中，Bcl2 的表达显著上调，而 Bax 和细胞色素 C 的表达以及 cleaved caspase-9 和 cleaved caspase-3 的水平降低。与药效学分析一致，LY294002 抑制 Kaji-ichigoside F1 和 Rosamultin 对上述分子的调节作用，而 PD98059 抑制 Kaji-ichigoside F1 的调节作用但增强 Rosamultin 的调节作用。总之，Kaji-ichigoside F1 通过激活 ERK1/2 信号通路保护血管内皮细胞免受缺氧诱导的凋亡，该信号通路正向调节 NF-B 信号通路，负向调节 PI3K/AKT 信号通路。Rosamultin 通过激活 PI3K/AKT 信号通路并正向调节 ERK1/2 和 NF-B 信号通路来保护血管内皮细胞免受缺氧诱导的凋亡。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8eb2/7153006/bf525b655d02/OMCL2020-6837982.001.jpg

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栀子苷 F1 和瑞香素通过 PI3K/AKT 或 ERK1/2 信号通路保护血管内皮细胞免受缺氧诱导的细胞凋亡。

Kaji-Ichigoside F1 and Rosamultin Protect Vascular Endothelial Cells against Hypoxia-Induced Apoptosis via the PI3K/AKT or ERK1/2 Signaling Pathway.

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