Zhang Haijing, Yang Yifei, Guo Feifei, He Rong, Gao Shuangrong, Cao Chunyu, Zhao Chunhui, Xia Bing, Xu Qihua, Gong Ping, Wang Lifang, Su Ping, Liu Ting
Institute of Chinese Material Medica, China Academy of Chinese Medical Sciences, Beijing, China.
Front Pharmacol. 2022 Nov 3;13:1023379. doi: 10.3389/fphar.2022.1023379. eCollection 2022.
Danlu tongdu tablets (DLTD) is a listed Chinese patent medicine collected in the Pharmacopoeia of the People's Republic of China (version 2020). This prescription has been applied in clinics in China for lumbar spinal stenosis and lumbosacral disc herniations. The wide application of Danlu tongdu in therapy has raised some clinical adverse reactions, such as significant elevation of alanine transaminase (ALT) and aspartate transaminase (AST) in individual patients after use. The present study aimed to investigate the safety of Danlu tongdu and analyze its adverse effects on the liver. The maximum feasible dose (MFD) was used to carry out the acute toxicity tests. Mortality, adverse effects, body weight and food consumption were recorded for up to 14 days post treatment. In the 6-month chronic toxicity test, sprague-dawley rats were randomly divided into four groups according body weight, the experimental groups were administrated to rats at the concentrations of 1.67, 3.34 and 6.67 g/kg/day, whereas the control group was received the ultrapure water (vehicle) only, 10 ml/kg, once a day. The animal's body weight, food consumption was monitored weekly. In addition, their hematological and biochemical parameters, body and organ weights and histopathology, were all measured at specific observation time points. Additionally, we further explored the adverse effects mechanism of Danlu tongdu on the liver through transcriptome analysis. No deaths or substance-relative toxicity were observed in the acute toxicity study or the 6-month chronic toxicity study with doses of 1.67 g/kg and 3.34 g/kg, respectively. We found that mild hypertrophy and hyperplasia of hepatic interlobular bile ducts were detected in some rats with doses of 6.67 g/kg after repeated oral administration of Danlu tongdu for 13 and 26 weeks, but the above changes in liver were reversible. The results of transcriptome sequencing showed that Danlu tongdu had a significant effect on cytochrome P450 enzymes in rat liver, especially cytochrome P450 1 (CYP1) subtype. Therefore, the toxic target organ of Danlu tongdu is the liver and the mechanism of mild liver injury is closely related to the up-regulation of cytochrome P450 1A1 (CYP1A1) and cytochrome P450 1A2 (CYP1A2) expression.
丹鹿通督片(DLTD)是收录于《中华人民共和国药典》(2020年版)的上市中成药。该方剂在中国临床上已用于治疗腰椎管狭窄症和腰椎间盘突出症。丹鹿通督片在治疗中的广泛应用引发了一些临床不良反应,比如个别患者用药后丙氨酸转氨酶(ALT)和天冬氨酸转氨酶(AST)显著升高。本研究旨在探讨丹鹿通督片的安全性并分析其对肝脏的不良影响。采用最大可行剂量(MFD)进行急性毒性试验。记录给药后长达14天的死亡率、不良反应、体重和食物消耗量。在为期6个月的慢性毒性试验中,将斯普拉格-道利大鼠按体重随机分为四组,实验组大鼠分别按1.67、3.34和6.67 g/kg/天的浓度给药,而对照组仅给予超纯水(溶媒),10 ml/kg,每天一次。每周监测动物的体重和食物消耗量。此外,在特定观察时间点测量其血液学和生化参数、体重和器官重量以及组织病理学。此外,我们通过转录组分析进一步探究了丹鹿通督片对肝脏的不良影响机制。在急性毒性研究以及分别给予1.67 g/kg和3.34 g/kg剂量的6个月慢性毒性研究中,均未观察到死亡或与药物相关的毒性。我们发现,在丹鹿通督片连续口服给药13周和26周后,部分给予6.67 g/kg剂量的大鼠检测到肝小叶间胆管轻度肥大和增生,但上述肝脏变化是可逆的。转录组测序结果表明,丹鹿通督片对大鼠肝脏中的细胞色素P450酶有显著影响,尤其是细胞色素P450 1(CYP1)亚型。因此,丹鹿通督片的毒性靶器官是肝脏,轻度肝损伤机制与细胞色素P450 1A1(CYP1A1)和细胞色素P450 1A2(CYP1A2)表达上调密切相关。
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