Protective Effect and Combination Proportion of 8,8Glycyrrhizic Acid on Acute Liver Injury in Mice

ZHANG Hui; PEI Zhi-dong; CHEN Ying; KANG Ting-guo

doi:10.13422/j.cnki.syfjx.2016020103

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Protective Effect and Combination Proportion of 8,8Glycyrrhizic Acid on Acute Liver Injury in Mice

更新时间：2024-01-04

- Protective Effect and Combination Proportion of 8,8Glycyrrhizic Acid on Acute Liver Injury in Mice
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 22, Issue 2, Pages: 103-106(2016)
- 作者机构：
- 作者简介：
- 基金信息：
- DOI：10.13422/j.cnki.syfjx.2016020103
  CLC： R285.5
- Published：2016
- 稿件说明：
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ZHANG Hui, PEI Zhi-dong, CHEN Ying, et al. Protective Effect and Combination Proportion of 8,8Glycyrrhizic Acid on Acute Liver Injury in Mice[J]. Chinese journal of experimental traditional medical formulae, 2016, 22(2): 103-106.
DOI：

ZHANG Hui, PEI Zhi-dong, CHEN Ying, et al. Protective Effect and Combination Proportion of 8,8Glycyrrhizic Acid on Acute Liver Injury in Mice[J]. Chinese journal of experimental traditional medical formulae, 2016, 22(2): 103-106. DOI： 10.13422/j.cnki.syfjx.2016020103.

摘要

目的:对比研究18α-甘草酸

18β-甘草酸及二者联合用药对小鼠急性肝损伤的保护作用

并筛选二者联合用药的最佳配伍比例。方法:小鼠随机被分为正常组

模型组

18α-甘草酸

18β-甘草酸低、中、高剂量组(15

60 mg·kg-1)

联合用药给药剂量均为60 mg·kg-1

联合用药1(18α-甘草酸-18β-甘草酸1:3)组、联合用药2(18α-甘草酸-18β-甘草酸2:3)组、联合用药3(18α-甘草酸:18β-甘草酸1:1)组。在造模前各治疗组ip给药7 d

1次/d

其他各组ip生理盐水;末次给药1 h后

除正常组ip生理盐水外

其他各组均ip 0.1%四氯化碳(CCl4)花生油(20 mL·kg-1)建立CCl4诱导小鼠急性肝损伤模型

观察18α-

18β-甘草酸高、中、低剂量(15

60 mg·kg-1)组

联合用药3个不同配伍比例组对急性肝损伤小鼠血清中和肝组织中丙氨酸转氨酶(ALT)

天冬氨酸转氨酶(AST)水平的影响

并检测肝组织匀浆中超氧化物歧化酶(SOD)活力及丙二醛(MDA)含量

同时筛选二者联合用药的最佳配伍比例。结果:与正常组比较

模型组血清AST

肝组织AST

ALT

MDA水平明显升高

SOD活力显著降低(P<0.01)

提示造模成功。与模型组比较

18α-甘草酸组

18β-甘草酸组均可降低小鼠血清中AST

肝组织AST

ALT活力

MDA含量

升高肝组织中SOD活力;比较二者对急性肝损伤小鼠的保护作用

结果18β-甘草酸组对肝组织中AST

ALT水平影响优于18α-甘草酸组

其他指标无显著性差异;二者联合用药的最佳配伍比例为2:3

其对肝组织中AST活力及MDA含量的影响均优于单用18α-或18β-甘草酸治疗组。结论:18α-与18β-甘草酸可保护急性肝损伤小鼠

后者保护作用比前者强

二者配伍的最佳比例是2:3

其对AST

MDA水平影响优于单用18α-或18β-甘草酸。

Abstract

Objective:To compare the protective effect of 18α-and 18β-glycyrrhizic acid on acute liver injury in mice

and screen out their optimal combination proportion. Method:The mice were randomly divided into normal group

model group

high dose group (60 mg·kg-1)

middle dose group (30 mg·kg-1)

low dose group (15 mg·kg-1) of 18α-and 18β-glycyrrhizic acid. With the drug dose of combined medication groups of 60 mg·kg-1

combined medication 1 groups (18α-glycyrrhizic acid-18β-glycyrrhizic acid 1:3)

combined medication 2 groups (18α-glycyrrhizic acid-18β-glycyrrhizic acid 2:3)

combined medication 3 groups (18α-glycyrrhizic acid-18β-glycyrrhizic acid 1:1). Before the modeling

the drugs were injected once everyday for 7 days

the same volume of saline was given to normal group and model group. At 1 h after the last administration

the treated groups and model group were ip given 0.1%CCl4 peanut oil (20 mL·kg-1) to establish mouse model of acute liver injury induced by CCl4 .The samples of blood and liver from high does group

middle dose group

low dose group and three combination proportion groups of 18α-and 18β-glycyrrhizic acid were analyzed

and level of alanine aminotransferase (ALT)

aspartate aminotransferase (AST)

superoxide dismutase (SOD) and malondialdehyde (MDA) were measured. Result:Compared with the normal group

the serum levels of AST

liver homogenate levels of AST

ALT

MDA in model group were remarkably higher (P<0.01)

levels of SOD was remarkably lower. Compared with the model group

18α-and 18β-glycyrrhizic acid remarkably reduced the serum levels of AST

reduced liver homogenate levels of AST

ALT and MDA

and increased liver homogenate content of SOD. 18β-glycyrrhizic acid had a better effect on liver homogenate levels of AST

ALT than 18α-glycyrrhizic acid

and showed no significant difference in other indexes compared with 18β-glycyrrhizic acid. The optimal combination proportion of 18α-and 18β-glycyrrhizicacid is 2:3

with a better effect on liver homogenate levels of AST

MDA than simple 18α-or 18β-glycyrrhizic acid. Conclusion:18α-and 18β-glycyrrhizic acid can protect acute liver injury in mice. The latter had a better protective effect than the former. Their optimal combination proportion is 2:3

with a better effect on liver homogenate levels of AST

MDA than simple 18α-or 18β-glycyrrhizic acid.

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