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山豆根对小鼠的肝毒性及血清胆碱酯酶升高作为肝损伤潜在补充生物标志物的研究

Hepatotoxicity induced by radix Sophorae tonkinensis in mice and increased serum cholinesterase as a potential supplemental biomarker for liver injury.

作者信息

Wang Liping, Lu Jinyao, Sun Wei, Gu Yingmin, Zhang Chaochao, Jin Ruomin, Li Lingyong, Zhang Zean, Tian Xuesong

机构信息

Center for Drug Safety Evaluation and Research, Shanghai University of Traditional Chinese Medicine, Shanghai, China.

Laboratory Animal Center, Shanghai University of Traditional Chinese Medicine, Shanghai, China.

出版信息

Exp Toxicol Pathol. 2017 Apr 4;69(4):193-202. doi: 10.1016/j.etp.2017.01.003. Epub 2017 Jan 23.

Abstract

Radix Sophorae tonkinensis (S. tonkinensis) is used in Chinese folk medicine to treat sore throats, viral hepatitis, and jaundice. However, little is known about the hepatotoxicity induced by it. This study is to investigate hepatotoxicity induced by radix S. tonkinensis and a potential supplemental biomarker for liver injury through acute toxicity, accumulative toxicity, tolerance test, and sub-chronic toxicity. The contents of cytisine (CYT), matrine (MT), and oxymatrine (OMT) in radix S. tonkinensis extracts were determined simultaneously by the method we developed. In the acute toxicity study, mice were scheduled for single oral gavage at doses of 0, 2.4, 3.2, 4.2, 5.6, 7.5g/kg of radix S. tonkinensis extracts respectively. Another three groups of mice received radix S. tonkinensis extracts orally in single doses of 0, 4.3, 5.6g/kg, while the two groups of the hepatic injury model were induced by intraperitoneal injection with 0.1% and 0.2% carbon tetrachloride (CCl). Mortality rate, analysis of serum biochemistry, and histopathological examination were used to assess the acute toxicity. In the accumulative toxicity study, mice were treated radix S. tonkinensis extracts orally by the method of dose escalation for 20days respectively. Accumulative toxicity was assessed by mortality rate. In the tolerance test, half of the mice of test group in the accumulative toxicity were administered the dose of 4.3g/kg radix S. tonkinensis extracts, and the rest of the mice in the test group were assigned to receive the dose of 5.6g/kg radix S. tonkinensis extracts. In the sub-chronic toxicity study, mice were treated with daily doses of 0, 0.25, 1.0, 2.5g/kg radix S. tonkinensis extracts for 90days. Assessments of body weights, serum biochemical analysis, and histopathological examination were performed. An enzyme-inhibition assay for butyrylcholinesterase (BuChE) and acetylcholinesterase (AChE) of CYT, MT, and OMT was also carried out. The contents of CYT, MT, and OMT in radix S. tonkinensis extracts were 5.63mg/g, 27.63mg/g, and 16.20mg/g respectively. In the acute toxicity study, LD50 of radix S. tonkinensis extracts was 4.3g/kg. No mice were found dead in the accumulative toxicity study. In the acute toxicity and tolerance test, increased ALT, AST, and CHE levels were observed in a dose-response manner, while the severity of histological changes in liver was shown in a dose-dependent mode. In the sub-chronic toxicity, though there was a decline trend of ALT and AST levels found in 0.25g/kg, 1.0g/kg, and 2.5g/kg radix S. tonkinensis extracts as compared to control, which might be related to weight loss, the severity of histopathological changes in the liver and the increased serum CHE level was shown in a dose-response manner. MT, OMT, and CYT showed inhibitory effects on BuChE and AChE in the enzyme-inhibition assay. The results of this study indicate that radix S. tonkinensis should have hepatotoxicity, and increased serum CHE is a potential supplemental biomarker for liver injury.

摘要

越南槐(S. tonkinensis)在中国民间医学中用于治疗咽喉痛、病毒性肝炎和黄疸。然而,关于其诱导的肝毒性知之甚少。本研究旨在通过急性毒性、蓄积毒性、耐受性试验和亚慢性毒性研究越南槐诱导的肝毒性以及一种潜在的肝损伤补充生物标志物。采用我们开发的方法同时测定越南槐提取物中野靛碱(CYT)、苦参碱(MT)和氧化苦参碱(OMT)的含量。在急性毒性研究中,将小鼠分别按0、2.4、3.2、4.2、5.6、7.5g/kg的剂量单次口服给予越南槐提取物。另外三组小鼠分别按0、4.3、5.6g/kg的单次剂量口服给予越南槐提取物,而两组肝损伤模型通过腹腔注射0.1%和0.2%的四氯化碳(CCl)诱导。采用死亡率、血清生化分析和组织病理学检查来评估急性毒性。在蓄积毒性研究中,分别采用剂量递增法给小鼠口服越南槐提取物20天。通过死亡率评估蓄积毒性。在耐受性试验中,将蓄积毒性试验中试验组的一半小鼠给予4.3g/kg的越南槐提取物剂量,试验组的其余小鼠给予5.6g/kg的越南槐提取物剂量。在亚慢性毒性研究中,将小鼠每天按0、0.25、1.0、2.5g/kg的剂量给予越南槐提取物,持续90天。进行体重评估、血清生化分析和组织病理学检查。还对CYT、MT和OMT进行了丁酰胆碱酯酶(BuChE)和乙酰胆碱酯酶(AChE)的酶抑制试验。越南槐提取物中CYT、MT和OMT的含量分别为5.63mg/g、27.63mg/g和16.20mg/g。在急性毒性研究中,越南槐提取物的半数致死量(LD50)为4.3g/kg。在蓄积毒性研究中未发现小鼠死亡。在急性毒性和耐受性试验中,观察到ALT、AST和CHE水平呈剂量反应性升高,而肝脏组织学变化的严重程度呈剂量依赖性。在亚慢性毒性试验中,尽管与对照组相比,0.25g/kg、1.0g/kg和2.5g/kg的越南槐提取物组的ALT和AST水平有下降趋势,这可能与体重减轻有关,但肝脏组织病理学变化的严重程度和血清CHE水平的升高呈剂量反应性。在酶抑制试验中,MT、OMT和CYT对BuChE和AChE有抑制作用。本研究结果表明越南槐具有肝毒性,血清CHE升高是肝损伤的一种潜在补充生物标志物。

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