Study on Mechanism of Hepatotoxicity of Triptolide Based on Hepatocyte's Microcarrier Culture
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Study on Mechanism of Hepatotoxicity of Triptolide Based on Hepatocyte's Microcarrier Culture
Chinese Journal of Experimental Traditional Medical FormulaeVol. 18, Issue 13, Pages: 248-251(2012)
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Published:2012
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LIU Zhang-pu, ZHOU Ling-ling, FENG Zhe, et al. Study on Mechanism of Hepatotoxicity of Triptolide Based on Hepatocyte's Microcarrier Culture[J]. Chinese journal of experimental traditional medical formulae, 2012, 18(13): 248-251.
DOI:
LIU Zhang-pu, ZHOU Ling-ling, FENG Zhe, et al. Study on Mechanism of Hepatotoxicity of Triptolide Based on Hepatocyte's Microcarrier Culture[J]. Chinese journal of experimental traditional medical formulae, 2012, 18(13): 248-251.DOI:
Study on Mechanism of Hepatotoxicity of Triptolide Based on Hepatocyte's Microcarrier Culture
Objective: To explore a method for high density cultivation of LO2 hepatocytes using microcarrier
and study the hepatotoxicity and its mechanism of triptolide's major toxic components. Method: With the condition of the cells restricted to attach dish
three-dimensional cultivating of LO2 hepatocytes was carried out by Cytodex-3.The cell growth was observed on the light microscope and the effect of triptolide on liver cell proliferation was detected. Concentrations of alanine aminotransferase(ALT)
aspartate aminotransferase(AST)
lactic dehydrogense(LDH)
superoxide dismutase(SOD) and malondialdehyde(MDA) in the supernatant were examined. Content of glutathione peroxidase(GSH-Px) was also examined in the cell lysate. Result: The proliferation of hepatocytes was considerably inhibited and the activity of hepatocytes was decreased by triptolide(100 μg·mL-1). On the other hand
the activity of ALT
AST
LDH was increased by triptolide(100 μg·mL-1). The content of MDA was increased
and the activities of SOD and GSH-Px were decreased by triptolide(100 μg·mL-1). Conclusion: The triptolide could do harm to hepatocytes
which may be caused by the lipid peroxidation of hepatocytes.
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