Protective Effect and Mechanism of Methyl Helicteres on Chronic Liver Injury Induced by CCl in Rats

LU Chun-yuan; LIN Xing; HUANG Quan-fang; WEI Jin-bin

doi:10.13422/j.cnki.syfjx.2017070141

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Protective Effect and Mechanism of Methyl Helicteres on Chronic Liver Injury Induced by CCl in Rats

更新时间：2024-01-04

- Protective Effect and Mechanism of Methyl Helicteres on Chronic Liver Injury Induced by CCl in Rats
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 23, Issue 7, Pages: 141-147(2017)
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- DOI：10.13422/j.cnki.syfjx.2017070141
  CLC： R285.5
- Published：2017
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LU Chun-yuan, LIN Xing, HUANG Quan-fang, et al. Protective Effect and Mechanism of Methyl Helicteres on Chronic Liver Injury Induced by CCl in Rats[J]. Chinese journal of experimental traditional medical formulae, 2017, 23(7): 141-147.
DOI：

LU Chun-yuan, LIN Xing, HUANG Quan-fang, et al. Protective Effect and Mechanism of Methyl Helicteres on Chronic Liver Injury Induced by CCl in Rats[J]. Chinese journal of experimental traditional medical formulae, 2017, 23(7): 141-147. DOI： 10.13422/j.cnki.syfjx.2017070141.

摘要

目的：研究山芝麻酸甲酯对四氯化碳（CCl4）诱发的大鼠肝损伤的保护作用及其机制。方法：将大鼠随机分为正常组、模型组、水飞蓟素组（50 mg·kg-1）及山芝麻酸甲酯低、高剂量组（50，200 mg·kg-1）。除正常组外，其余各组大鼠灌胃给予20% CCl4，每周2次，总共8周，制备大鼠慢性损伤模型，与此同时，治疗组每日给大鼠灌胃山芝麻酸甲酯或水飞蓟素1次，共8周。实验结束后，酶联免疫吸附（ELISA）试剂盒检测血清丙氨酸氨基转移酶（ALT），天门冬氨酸氨基转移酶（AST），白蛋白（ALB）活性及血浆中白细胞介素-6（IL-6），肿瘤坏死因子-α（TNF-α）含量。肝组织苏木素-伊红（HE）染色，观察各组大鼠肝脏病变情况。酶联免疫吸附试验（ELISA）试剂盒检测肝组织超氧化物歧化酶（SOD），谷胱甘肽过氧化物酶（GSH-Px），谷胱甘肽还原酶（GSH-Rd），细胞核转录因子-κB p65（NF-κB p65）含量。蛋白免疫印迹法（Western blot）法检测肝组织中诱导型一氧化氮合酶（iNOS），环氧合酶-2（COX-2），半胱氨酸天冬氨酸特异性蛋白酶-3（Caspase-3），半胱氨酸天冬氨酸特异性蛋白酶-8（Caspase-8），以及凋亡相关蛋白Fas，FasL蛋白表达的变化。结果：山芝麻酸甲酯明显改善CCl4引起的严重病理性肝损伤；降低大鼠血清ALT，AST和ALB的水平，提高肝脏SOD，GSH-Px和GSH-Rd的活力；明显降低血浆中炎症因子IL-6和TNF-α的含量。进一步的研究发现，山芝麻酸甲酯明显抑制了与炎症反应调节相关的信号通路NF-κB，以及重要酶iNOS和COX-2的活力。此外，山芝麻酸甲酯明显抑制Caspase-3，Caspase-8，Fas和FasL蛋白的表达，减少肝细胞凋亡。结论：山芝麻酸甲酯对CCl4致大鼠肝损伤具有保护作用，其机制可能与抑制NF-κB信号通路减轻炎症反应以及减少细胞凋亡有关。

Abstract

Objective: To study the protective effect and mechanism of methyl helicterate isolated from Helicteres Radix on chronic liver injury induced by carbon tetrachloride (CCl4) in rats. Method: The rats were randomly divided into 5 groups

including normal control group

model group

silymarin positive control group(50 mg·kg-1)

and high and low-dose methyl helicterate (200

50 mg·kg-1) groups. Except for the normal control group

all of the other groups were intragastrically administrated with 20% CCl4 for 8 weeks

twice a week. Meanwhile

the animals in the positive control group and methyl helicterate-treated groups were given silymarin (50 mg·kg-1) and methyl helicterate (200

50 mg·kg-1) by gavage once a day for 8 weeks. After the experiment

the levels of serum alanine aminotransferase (ALT)

aspartate aminotransferase (AST)

albumin (ALB) and plasma interleukin-6 (IL-6)

tumor necrosis factor -α (TNF-α) were detected by enzyme-linked immuno sorbent assay(ELISA) kits. The hepatic pathological changes were observed by HE staining. And the levels of superoxide dismutase (SOD)

glutathione peroxidase (GSH-Px)

glutathione reductase (GSH-Rd)

NF-κB p65 in liver tissues were detected by ELISA kits. Western blot assay was performed to detect the expression of nitric oxide synthase (iNOS)

cyclooxygenase-2 (COX-2)

Caspase-3

Caspase-8 Fas and FasL in liver tissues. Result: Methyl helicterate significantly alliviated CCl4-induced serious liver injury

decreased the levels of serum ALT

AST and ALB

while increased the activities of hepatic SOD

GSH-Px and GSH-Rd. Methyl helicterate also reduced the contents of inflammatory cytokines TNF-α and IL-6 in liver tissues. The further study showed that methyl helicterate significantly inhibited the vitality of NF-κB

iNOS and COX-2

which played a crucial role in regulat inginflammatory response.In addition

methyl helicterate significantly suppressed the expressions of Caspase-3

Caspase-8

Fas and FasL

and reduced the hepatocytes apoptosis. Conclusion: Methyl helicterate alleviates liver injury induced by CCl4 in rats

the mechanism may be associated with the inhibition of NF-κB signaling pathway and the decrease in cell apoptosis.

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