[Prophylactic and therapeutic effect of oxymatrine on D-galactosamine-induced rat liver fibrosis]

Wenzhuo Yang; Minde Zeng; Zhuping Fan; Yimin Mao; Yulin Song; Yitao Jia; Lungen Lu; Cheng Wei Chen; Yan Shen Peng; Hong Yin Zhu

[Prophylactic and therapeutic effect of oxymatrine on D-galactosamine-induced rat liver fibrosis]

Zhonghua Gan Zang Bing Za Zhi. 2002 Jun;10(3):193-6.

[Article in Chinese]

Authors

Wenzhuo Yang¹, Minde Zeng, Zhuping Fan, Yimin Mao, Yulin Song, Yitao Jia, Lungen Lu, Cheng Wei Chen, Yan Shen Peng, Hong Yin Zhu

Affiliation

¹ Shanghai Digestive Disease Institute, Renji Hospital, Shanghai 200001, China.

PMID: 12113677

Abstract

Objective: To investigate the prophylactic and therapeutic effect of oxymatrine on experimental liver fibrosis and to reveal its mechanism.

Methods: By establishing D-galactosamine-induced rat liver fibrosis model, we observed the effect of oxymatrine on serum and tissue biochemical indexes, content of liver hydroxyline, expression of TGF?1 mRNA and changes of tissue pathology.

Results: There was a decline of liver hydroxyline and serum AST and ALT in oxymatrine group compared to those of the D-GalN group. The hydroxyline content in oxymatrine pretreatment group was (0.50 0.11)mug/mg compared with (0.99 0.14)mug/mg in D-GalN group (t=8.366, P<0.01). The content in oxymatrine treatment group was (0.44 0.04)mug/mg compared with 0.70 0.06 in D-GalN group (t=9.839, P<0.01). The SOD activity was (149.81 15.28) NU/mg in oxymatrine pretreatment group and (95.22 16.33) NU/mg in the model group (t=7.309, P<0.01); (157.68 19.54) NU/mg in the treatment group compared with (119.88 14.94) NU/mg in the model group (t=4.348, P<0.01). MDA in the pretreatment group was (2.06 0.17) nmol/mg, lower than (4.57 0.37) nmol/mg in the model group (t=17.529, P<0.01). In the treatment group, it was (1.76 0.24)nmol/mg, lower than (3.10 0.17) nmol/mg in the model group (t=12.697, P<0.01). TGF?1 mRNA reduced in the pretreatment and treatment groups as compared with that in the model group (0.21 0.01 vs 0.50 0.01, t=48.665, P<0.01; 0.18 0.02 vs 0.38 0.01, t=22.464, P<0.01). Electron microscopy showed that oxymatrine group had milder hepatocyte degeneration and less fibrosis accumulation than did the model group. Microscopy revealed wide septa expansion from the portal area to the central venous, piecemeal and confluent necrosis and pseudo-nodular formation in part of the lobular in the model group. While in oxymatrine group these lesions were much improved.

Conclusions: Oxymatrine shows prophylactic and therapeutic effect in D-galactosamine induced rat liver fibrosis. This is partly by protecting hepatocyte and suppressing fibrosis accumulation through anti-lipoperoxidation.

MeSH terms

Alkaloids / therapeutic use*
Animals
Anti-Arrhythmia Agents / therapeutic use
Calcium Hydroxide / metabolism
Chemoprevention
Disease Models, Animal
Galactosamine
Liver Cirrhosis / chemically induced
Liver Cirrhosis / drug therapy*
Liver Cirrhosis / metabolism
Liver Cirrhosis / pathology
Liver Cirrhosis / prevention & control
Liver Function Tests
Male
Quinolizines
RNA, Messenger / metabolism
Rats
Rats, Wistar
Superoxide Dismutase / metabolism
Transforming Growth Factor beta / genetics
Transforming Growth Factor beta / metabolism

Substances

Alkaloids
Anti-Arrhythmia Agents
Quinolizines
RNA, Messenger
Transforming Growth Factor beta
Galactosamine
Hydroxyline
oxymatrine
Superoxide Dismutase
Calcium Hydroxide