Establishment of Simultaneous Liver and Kidney Lesion Model Induced by Concanavalin A in Mice

CUI Jia-li; SHAN Li-mei; ZHANG Ping; WANG Jia-bo; LI Bao-cai; XIAO Xiao-he

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Establishment of Simultaneous Liver and Kidney Lesion Model Induced by Concanavalin A in Mice

更新时间：2024-01-04

- Establishment of Simultaneous Liver and Kidney Lesion Model Induced by Concanavalin A in Mice
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 18, Issue 22, Pages: 210-214(2012)
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- Published：2012
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CUI Jia-li, SHAN Li-mei, ZHANG Ping, et al. Establishment of Simultaneous Liver and Kidney Lesion Model Induced by Concanavalin A in Mice[J]. Chinese journal of experimental traditional medical formulae, 2012, 18(22): 210-214.
DOI：

CUI Jia-li, SHAN Li-mei, ZHANG Ping, et al. Establishment of Simultaneous Liver and Kidney Lesion Model Induced by Concanavalin A in Mice[J]. Chinese journal of experimental traditional medical formulae, 2012, 18(22): 210-214. DOI：

摘要

目的: 筛选并初步建立能够诱导小鼠肝肾同时损伤的实验动物模型

为评价肝肾损伤治疗药物提供实验动物模型。方法: 考察尾静脉注射刀豆蛋白A(Con A)10

40 mg·kg-1

造模时间12 h; ig给药D-半乳糖胺(D-Gal)1 g·kg-1及腹腔注射0.3%四氯化碳(CCl4

20 mL·kg-1) 60 mg·kg-1

造模时间24 h;药物对模型小鼠肝脏、肾脏的损伤作用

通过检测肝肾功能相关的生化指标

肝脏及肾脏病理组织学改变

确定有效的造模方案。为进一步确定该模型是否能有效评价治疗肝肾损伤药物的药效

考察了大黄甘草汤对小鼠肝肾损伤模型的保护作用。结果: 给予小鼠1 g·kg-1 D-Gal

CCl4 60 mL·kg-1造模后

其血清直接胆红素(DBIL)、总胆红素(TBIL)、丙氨酸转氨酶(ALT)、天冬氨酸转氨酶(AST)活性与对照组比较均显著升高(P<0.05或P<0.01)

而尿素氮(BUN)、肌酐(CRE)、总胆固醇(TC)、甘油三脂(TG)

血清总蛋白(TP)、白蛋白(ALB)含量无明显变化

组织病理变化与血清生化指标结果相同

说明上述两种药物可诱发小鼠肝损伤模型

但未检测到肾损伤相关生化指标及病理变化;给予小鼠Con A 20 mg·kg-1造模后

小鼠血清DBIL

TBIL

ALT

AST

BUN

CRE

ALB值与对照组相比较差异显著(P<0.01

P <0.05)

说明Con A 20 mg·kg-1可诱发小鼠肝肾同时损伤

进一步优化模型

确定15 mg·kg-1 Con A为诱发小鼠肝肾损伤的最佳剂量;给予模型验证方药大黄甘草汤干预后

肝肾损伤小鼠的生化和组织学检查均有显著改善。结论: 初步建立尾静脉注射Con A 15 mg·kg-1诱导小鼠实验性肝肾同时损伤模型

用大黄甘草汤验证说明模型建立成功。

Abstract

Objective:To screen and establish the experimental animal model of simultaneous liver and kidney lesion in mice

and to provide experimental animal models for screening drugs which used to cure kidney and liver damage. Method: We investigated the damage effect of concanavalin A (Con A)

D-galactosamine (D-Gal) and carbon tetrachloride (CCl4) in the mouse liver and kidney

and we established the effective modeling method by determing the biochemical indicators and the histopathological changes related to the liver and kidney function. To further inspect if the model is able to effectively evaluate the efficacy of drugs for kidney and liver damage

we study the protective effect of Dahuang Gancao decoction on liver and kidney damage using the established model. Result: 1 g·kg-1 D-Gal

CCl4(60 mg·kg-1) could induce liver injury in mice

but there is no evident about the renal injury; 20 mg·kg-1 Con A could induce liver and kidney damage simultaneously

and we determine the best dose of Con A to built simultaneous liver and kidner damage model as 15 mg·kg-1 after further optimization. The biochemical index and histological examination of kidney and liver damage mice were significantly improved after giving the prescription Dahuang Gancao decoction. Conclusion: We initially established the experimental model of simultaneous liver and kidney damage by injecting Con A 15 mg·kg-1 through tail vein

and proved to be successful by verification of Dahuang Gancao docoction.

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