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

摘要Objective:Salt-processed Psoraleae Fructus(SPF)is widely used as a phytoestrogen-like agent in the treat-ment 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 hepatotoxi-city 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 phar-macology 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 path-ways.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 gallblad-der 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 indi-cators,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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作者 Yu Wu [1] Yan Xu [2] Hao Cai [2] Zhengying Hua [2] Meimei Luo [2] Letao Hu [2] Nong Zhou [3] Xinghong Wang [4] Weidong Li [2] 学术成果认领
作者单位 Nantong Hospital of Traditional Chinese Medicine,Affiliated Traditional Chinese Medicine Hospital of Nantong University,Nantong 226000,China;Jiangsu Key Laboratory of Chinese Medicine Processing,Engineering Center of State Ministry of Education for Standardization of Chinese Medicine Processing,Nanjing University of Chinese Medicine,Nanjing 210023,China [1] Jiangsu Key Laboratory of Chinese Medicine Processing,Engineering Center of State Ministry of Education for Standardization of Chinese Medicine Processing,Nanjing University of Chinese Medicine,Nanjing 210023,China [2] Jiangsu Key Laboratory of Chinese Medicine Processing,Engineering Center of State Ministry of Education for Standardization of Chinese Medicine Processing,Nanjing University of Chinese Medicine,Nanjing 210023,China;Chongqing Engineering Laboratory of Green Planting and Deep Processing of Famous-region Drug in the Three Gorges Reservoir Region,College of Biology and Food Engineering,Chongqing Three Gorges University,Chongqing 404120,China [3] Nantong Hospital of Traditional Chinese Medicine,Affiliated Traditional Chinese Medicine Hospital of Nantong University,Nantong 226000,China [4]
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DOI 10.1016/j.chmed.2024.11.002
发布时间 2025-05-12(万方平台首次上网日期,不代表论文的发表时间)
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2025年17卷2期

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