Overexpression of SULT1E1 alleviates salt-processed Psoraleae Fructus-induced cholestatic liver damage

IF 4.7 4区医学 Q1 CHEMISTRY, MEDICINAL

Chinese Herbal Medicines Pub Date : 2025-04-01 DOI:10.1016/j.chmed.2024.11.002

Yu Wu , Yan Xu , Hao Cai , Zhengying Hua , Meimei Luo , Letao Hu , Nong Zhou , Xinghong Wang , Weidong Li

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引用次数: 0

Abstract

Objective

Salt-processed Psoraleae Fructus (SPF) is widely used as a phytoestrogen-like agent in the treatment of osteoporosis. However, due to improper clinical use or misuse, resulting in liver damage. In this study, network pharmacology was employed to analyze the mechanism of cholestatic liver damage. An adeno-associated virus overexpressing SULT1E1 (rAAV8-SULT1E1) was constructed and the hepatotoxicity of SPF, psoralen, and isopsoralen was determined.

Methods

By utilizing three databases inclding TCMSP, TCMID, and BATMAN- TCM, the targets of the three databases were summarized, and a total of 45 psoralen compounds were included. Network pharmacology analysis was then performed. The adenoviral vectors were injected into the tail vein of C57BL6 mice to elucidate the role of SULT1E1 in SPF-induced cholestasis-mediated hepatotoxicity in vivo. SPF (10 g/kg), psoralen, and isopsoralen (50 mg/kg each) were intragastrically administered to mice for 30 d. B-ultrasound and samples were collected and examined for follow-up experiments.

Results

A total of 854 targets were predicted for 45 active components, with 151 cholestasis-mediated hepatotoxicity-related disease targets obtained for SPF. A total of 126 pathways were enriched based on KEGG pathway analysis, with the “estrogen signaling pathway” identified as one of the top 20 pathways. In terms of pathological hepatic changes, treated mice had visually swollen hepatocytes, dilated bile ducts, and elevated serum biochemical markers, which were more prominent in mice treated with isopsoralen than in those treated with other compounds. Notably, the overexpression of SULT1E1 could reverse liver damage in each treatment group. B-ultrasound was used to observe the size of the gallbladder in vivo. The size of the gallbladder was found to significantly increase on day 30 after treatment in the SPF-, psoralen-, and isopsoralen-treated groups, especially the SPF group. Compared with the expression levels in the negative control group (rAAV8-empty + con), the expression levels of FXR, Mrp2, Bsep, SULT1E1, SULT2A1, Ntcp, and Nrf2 decreased, whereas those of CYP7a1 and IL-6 increased in the SPF-, psoralen-, and isopsoralen-treated groups.

Conclusion

The overexpression of SULT1E1 could alleviate the decreased or increased expression of indicators, indicating that SULT1E1 is an important target gene for SPF-induced liver damage. The severity of liver damage was significantly lower in the rAAV8-SULT1E1 groups than in the rAAV8-empty groups.

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SULT1E1过表达可减轻盐加工补骨脂所致的胆汁淤积性肝损伤

目的盐加工补骨脂（SPF）是一种广泛应用于骨质疏松症治疗的植物雌激素样药物。然而，由于临床使用不当或误用，造成肝脏损害。本研究采用网络药理学方法分析胆汁淤积性肝损害的机制。构建过表达SULT1E1的腺相关病毒（rAAV8-SULT1E1），测定SPF、补骨脂素和异补骨脂素的肝毒性。方法利用TCM、TCM、BATMAN- TCM 3个数据库，对3个数据库的靶点进行总结，共纳入45种补骨脂素类化合物。然后进行网络药理分析。将腺病毒载体注射到C57BL6小鼠的尾静脉，以阐明SULT1E1在spf诱导的胆汁淤积介导的体内肝毒性中的作用。小鼠灌胃SPF （10 g/kg）、补骨脂素和异补骨脂素（各50 mg/kg） 30 d。收集b超和样品，为后续实验做准备。结果共预测45种有效成分的854个靶点，其中SPF获得了151个胆汁淤积介导的肝毒性相关疾病靶点。通过KEGG通路分析，共富集了126条通路，其中“雌激素信号通路”位列前20条通路之一。在病理肝脏改变方面，治疗小鼠肝细胞明显肿胀，胆管扩张，血清生化指标升高，异补骨脂素治疗小鼠比其他化合物治疗小鼠更为突出。值得注意的是，在每个治疗组中，SULT1E1的过表达可以逆转肝损伤。用b超观察活体胆囊大小。研究发现，SPF-、补骨脂素-和异补骨脂素治疗组，尤其是SPF组，在治疗后第30天胆囊大小显著增加。与阴性对照组（rAAV8-empty + con）相比，SPF-、补骨脂素-和异补骨脂素处理组FXR、Mrp2、Bsep、SULT1E1、SULT2A1、Ntcp和Nrf2的表达水平降低，而CYP7a1和IL-6的表达水平升高。结论过表达SULT1E1可缓解spf性肝损伤相关指标表达的降低或升高，提示SULT1E1是spf性肝损伤的重要靶基因。rAAV8-SULT1E1组肝损伤严重程度明显低于raav8 -空组。

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来源期刊

Chinese Herbal Medicines CHEMISTRY, MEDICINAL-

CiteScore

4.40

自引率

5.30%

发文量

629

审稿时长

10 weeks

期刊介绍： Chinese Herbal Medicines is intended to disseminate the latest developments and research progress in traditional and herbal medical sciences to researchers, practitioners, academics and administrators worldwide in the field of traditional and herbal medicines. The journal's international coverage ensures that research and progress from all regions of the world are widely included. CHM is a core journal of Chinese science and technology. The journal entered into the ESCI database in 2017, and then was included in PMC, Scopus and other important international search systems. In 2019, CHM was successfully selected for the “China Science and Technology Journal Excellence Action Plan” project, which has markedly improved its international influence and industry popularity. CHM obtained the first impact factor of 3.8 in Journal Citation Reports (JCR) in 2023.