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ISSN 1001-5256 (Print)
ISSN 2097-3497 (Online)
CN 22-1108/R
Volume 35 Issue 9
Sep.  2019
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Article Navigation >  Journal of Clinical Hepatology  > 2019  >  35(9): 1958-1964

Effect of Duxiao Ganqing Pill on liver inflammation in rats with cirrhotic endotoxemia: An analysis based on the TLR4/MyD88/NF-κB signaling pathway

DOI: 10.3969/j.issn.1001-5256.2019.09.015

  • Changchun University of Traditional Chinese Medicine

Research funding:

 

  • Received Date: 2019-05-29
  • Published Date: 2019-09-20
    Abstract
  • Objective To establish a rat model of cirrhotic endotoxemia by CCl4 compound modeling, and to investigate the protective mechanism of Duxiao Ganqing Pill against liver inflammatory injury. Methods A total of 66 rats were selected, among which 17 died during modeling. Among the remaining 49 rats, 3 were selected to measure endotoxin and observe liver structure to determine whether the model was successfully established, and the other 46 rats were randomly divided into normal group with 6 rats, model group with 8 rats, lactulose group with 8 rats, and high-, middle-, and low-dose Duxiao Ganqing Pill ( 223. 4, 111. 7, and 58. 9 mg/kg) groups with 8 rats in each group. CCl4 compound modeling was performed for 8 weeks to establish a rat model of liver cirrhosis. The rats in the normal group and the model group were given distilled water, those in the lactulose group were given lactulose, and those in the Duxiao Ganqing Pill groups were given the drug according to the above doses, once a day for 2 consecutive months. The change in the content of endotoxin was measured. HE staining was used to observe the change in liver tissue, ELISA was used to measure the content of tumor necrosis factor-α ( TNF-α) , interleukin-1β ( IL-1β) , and interleukin-6 ( IL-6) in liver tissue, and Western blot and RT-PCR were used to measure the protein and mRNA expression of TLR4, MyD88, and NF-κB. A one-way analysis of variance was used for data comparison between groups, and the least significant difference t-test was used for further comparison of data with homogeneity of variance between two groups. Results There was a significant difference in serum endotoxin level between these groups ( F = 26. 011, P < 0. 001) ; the model group had a signifi-cantly higher endotoxin level than the normal group ( P < 0. 01) ; after treatment, the lactulose group and high-, middle-, and low-dose Duxiao Ganqing Pill groups had significantly lower serum endotoxin levels than the model group ( P < 0. 01) . There were significant differences in serum levels of IL-6, IL-1β, and TNF-α between these groups ( F = 35. 390, P = 0. 002; F = 38. 271, P = 0. 001; F =40. 241, P < 0. 001) ; the model group had significantly higher serum levels of IL-6, IL-1β, and TNF-α than the normal group ( all P < 0. 01) ; after treatment, the lactulose group and high-, middle-, and low-dose Duxiao Ganqing Pill groups had significantly lower serum levels of IL-6, IL-1β, and TNF-α than the model group ( all P < 0. 01) . There were significant differences in the mRNA and protein expression of TLR4, MyD88, and NF-κB in liver tissue between these groups ( F = 24. 483, 29. 547, 19. 242, 18. 752, 22. 146, and 15. 834, all P < 0. 01) ; the model group had significantly higher mRNA and protein expression of TLR4, MyD88, and NF-κB in liver tissue than the normal group ( all P < 0. 01) ; after treatment, the lactulose group and high-, middle-, and low-dose Duxiao Ganqing Pill groups showed significant reductions in the mRNA and protein expression of TLR4, MyD88, and NF-κB in liver tissue ( all P < 0. 01) , and the middle-and high-dose Duxiao Ganqing Pill groups had significantly greater reductions than the low-dose Duxiao Ganqing Pill group ( all P < 0. 01) . Conclusion Duxiao Ganqing Pill can inhibit the transduction of inflammatory signals by downregulating the TLR4/MyD88/NF-κB signaling pathway in liver tissue, reduce the expression of the cytokines TNF-α, IL-1β, and IL-6, and thus alleviate endotoxemia and exert a protective effect on liver tissue.

     

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    • References(21)
  • [1] LYU Z, ZHANG YX. Current status of the clinical research on intestinal endotoxemia in patients with liver cirrhosis[J]. Chin Hepatol, 2011, 16 (3) :262-283. (in Chinese) 吕震, 张友祥.肝硬化肠源性内毒素血症临床研究现状[J].肝脏, 2011, 16 (3) :262-283.
    [2] FEROLLA SM, ARMILIATO GN, COUTO CA, et al. The role of intestinal bacteria overgrowth in obesity-related nonalcoholic fatty liver disease[J]. Nutrients, 2014, 6 (12) :5583-5599.
    [3] ZHAO SH, FAN H, SONG ZJ, et al. Morphological structure changes of small intestinal mucosa and plasma endotoxin in cirrhotic rats[J]. Chin J Gastroenterol Hepatol, 2012, 21 (7) :607-610. (in Chinese) 赵生环, 范红, 宋正己, 等.肝硬化大鼠小肠黏膜形态结构改变与内毒素血症[J].胃肠病学和肝病学杂志, 2012, 21 (7) :607-610.
    [4] FENG LL, WANG XJ. Research advances in the pathogenesis of intestinal endotoxemia in patients with liver cirrhosis[J].Chin J Integr Trad West Med Dig, 2013, 21 (9) :496-498. (in Chinese) 冯丽丽, 汪晓军.肝硬化时肠源性内毒素血症形成机制的研究进展[J].中国中西医结合消化杂志, 2013, 21 (9) :496-498.
    [5] ZAN J, ZHANG H, LU MY, et al. Isosteviol sodium injection improves outcomes by modulating TLRs/NF-κB-dependent inflammatory responses following experimental traumatic brain injury in rats[J]. Neuroreport, 2018, 29 (10) :794-803.
    [6] KAYAGAKI N, WONG MT, STOWE IB, et al. Noncanonical inflammasome activation by intracellular LPS independent of TLR4[J]. Science, 2013, 341 (6151) :1246-1249.
    [7] CHEN HW, ZHU W, LI SS. Protective effects of endotoxin pretreatment on expression of TLR-4, NF-κB and ICAM-1 in hepatic tissue of rats with endotoxemia[J]. Acta Med Univ Sci Technol Huazhong, 2011, 40 (6) :666-669. (in Chinese) 陈华文, 祝伟, 李树生.内毒素预处理对内毒素血症大鼠肝TLR-4, NF-κB和ICAM-1表达的影响[J].华中科技大学学报:医学版, 2011, 40 (6) :666-669.
    [8] XIONG Z. Effect of Duxiao Ganqing pills based on the purgation method in regulating the PI3K/Akt signaling pathway in the intestinal mucosa of rats with liver cirrhosis:An experimental study[D]. Changchun University of Chinese Medicine, 2015. (in Chinese) 熊壮.基于“下法”毒消肝清丸调控肝硬化大鼠肠粘膜PI3K/Akt信号通路的实验研究[D].长春中医药大学, 2015.
    [9] SONG BY. Effect of Duxiao Ganqing pills based on the purgation method on the protein expression of occludin and AQP-4in the brain tissue of rats with liver cirrhosis and hepatic encephalopathy[D]. Changchun University of Chinese Medicine, 2015. (in Chinese) 宋柏玉.基于“下法”毒消肝清丸对肝硬化肝性脑病大鼠脑组织occludin及AQP-4蛋白表达的影响[D].长春中医药大学, 2015.
    [10] ZHU H, PING J, XU LM. Role of the nuclear factor-kappa B signaling pathway in hepatic fibrosis and the anti-fibrotic mechanism of traditional Chinese medicine[J]. J Clin Hepatol, 2018, 34 (4) :858-861. (in Chinese) 朱慧, 平键, 徐列明. NF-κB通路在肝纤维化进展和中药抗肝纤维化机制中的作用[J].临床肝胆病杂志, 2018, 34 (4) :858-861.
    [11] SHEN H, SHENG L, CHEN Z, et al. Mouse hepatocyte overexpression of NF–κB-inducing kinase (NIK) triggers fatal macrophage-dependent liver injury and fibrosis[J]. Hepatology, 2014, 60 (6) :2065-2076.
    [12] SUN K, XU L, JING Y, et al. Autophagy-deficient Kupffer cellspromote tumorigenesis by enhancing mtROS-NF-κBIL1α/β-dependent inflammation and fibrosis during the preneoplastic stage of hepatocarcinogenesis[J]. Cancer Lett, 2017, 388:198-207.
    [13] XIONG Z, YANG HH, LIU YY, et al. Analysis on medication rules of prof Liu Tiejun’s prescriptions with hepatic cirrhosis based on data mining[J]. Asia-Pacific Tradit Med, 2018, 7 (14) :85-88. (in Chinese) 熊壮, 杨洪辉, 刘扬扬, 等.基于数据挖掘的刘铁军教授治疗肝硬化用药规律研究[J].亚太传统医药, 2018, 7 (14) :85-88.
    [14] LI T, WANG XJ. Liu Tiejun’s experience in treating spleen and stomach diseases with purgative method[J]. J Changchun Univ Chin Med, 2019, 35 (1) :30-32. (in Chinese) 李婷, 王雪娇.刘铁军运用“下法”治疗脾胃病[J].长春中医药大学学报, 2019, 35 (1) :30-32.
    [15] XIONG Z, LIU YY, LIU YZ, et al. Professor Liu Tiejun’s ideas of the application of the purgation method in treatment of liver diseases[J]. Lishizhen Med Mater Med Res, 2017, 28 (3) :716-717. (in Chinese) 熊壮, 刘扬扬, 刘亚洲, 等.刘铁军教授应用“下法”治疗肝病思想解析[J].时珍国医国药, 2017, 28 (3) :716-717.
    [16] XING HX, CHAI GW. Promoting blood circulation and eliminating blood stasis on chronic hepatic disease[J]. J Shanxi College Tradit Chin Med, 2007, 8 (5) :44-46. (in Chinese) 邢华旭, 柴根旺.活血化瘀法在慢性肝病治疗中的应用体会[J].山西中医学院学报, 2007, 8 (5) :44-46.
    [17] CAO HH, LI XL. Effect of Rheum officinale on plasma level of endotoxin in patients with liver cirrhosis[J]. Zhejiang J Integr Tradit Chin West Med, 2012, 12 (22) :987-988. (in Chinese) 曹红华, 李晓玲.大黄对肝硬化患者血浆内毒素水平的影响[J].浙江中西医结合杂志, 2012, 12 (22) :987-988.
    [18] MA CY, PENG CR, GENG Y, et al. Experimental study on protective effects of rhein treating endotoxemia in rats[J]. Chin Arch Tradit Chin Med, 2012, 30 (2) :288-289. (in Chinese) 马超英, 彭春荣, 耿耘, 等.大黄酸对内毒素血症小鼠保护作用的实验研究[J].中华中医药学刊, 2012, 30 (2) :288-289.
    [19] HAN HY. Research progress of chronic kidney disease treated by Astragaloside IV[J]. J Changchun Univ Chin Med, 2017, 33 (4) :678-680. (in Chinese) 韩海燕.黄芪甲苷治疗慢性肾脏疾病研究进展[J].长春中医药大学学报, 2017, 33 (4) :678-680.
    [20] ZHOU XF, XUE Y, CAO ZQ. Regulation of Astragaloside IV on TLRs/NF-κB signaling pathway in rats with ulcerative colitis[J/OL]. Chin J Exp Med Formul, 2019. (in Chinese) 周晓凤, 薛晔, 曹志群.黄芪甲苷对溃疡性结肠炎大鼠TLRs/NF-κB信号通路的调节作用[J/OL].中国实验方剂学杂志, 2019.
    [21] ZHOU XH, WANG QL, ZHU XM, et al. Effects of angelica sinensis polysaccharide on TLR4/My D88/NF-κB pathway in rats with diabetic neuropathy[J]. Chin J Clin Pharmacol Ther, 2018, 23 (12) :1340-1347. (in Chinese) 周夏慧, 王庆来, 朱雪梅, 等.当归多糖对DPN大鼠TLR4/MyD88/NF-κB通路抑制影响[J].中国临床药理学与治疗学, 2018, 23 (12) :1340-1347.
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