ZHANG Qian, ZHOU Qi, JIN Ruo-min, et al. Preliminary Study on Hepatotoxicity and Nephrotoxicity Induced by Rutaecarpine[J]. Chinese journal of experimental traditional medical formulae, 2011, 17(8): 221-225.
DOI:
ZHANG Qian, ZHOU Qi, JIN Ruo-min, et al. Preliminary Study on Hepatotoxicity and Nephrotoxicity Induced by Rutaecarpine[J]. Chinese journal of experimental traditional medical formulae, 2011, 17(8): 221-225. DOI: CNKI:11-3495/R.20110303.1349.009.
Preliminary Study on Hepatotoxicity and Nephrotoxicity Induced by Rutaecarpine
Objective: To study the influence of rutaecarpine (Rut) on human normal hepatic cells (HL7702) and human embryonic kidney cells (HEK293) through in virto experiments.To study the toxicity of rutaecarpine on the vitality of hepatic and renal cells by preliminary compare co-culture system with solo-culture system. Method: ①The influence of rutaecarpine on the activity of hepatic and renal cells through MTT method in solo-culture system and co-culture system was detected.②The shape of cells was observed through inverted microscope.③After giving Rut
the change of ALT
AST
ALP
BUN
Cr and LDH in cultural supernatant of hepatic and renal cells was determined.④After giving Rut by intravenous administration
the influence of Rut on hepatic and renal function and histopathology in mice was investigated. Result: ①The MTT method showed that 2 μg ·mL-1 and 4 μg ·mL-1 of Rut decreased the activity of hepatic and renal cells. The inhibitory action on hepatic cells’ activity was higher than that on renal cell activity under the same concentration of Rut.② In cultural supernatant of hepatic cells
4 μg ·mL-1 of Rut increased AST
ALP and LDT(P<0.01). ③The animal experiment showed that after giving 10 mg ·kg-1 of Rut to mice by intravenous administration for 7 days
ALP in blood serum was increased notably (P<0.01)
while ALT
AST
BUN and Cr had a trend to increase. Histopathological examination revealed that there was an increase in hepatocyte nuclear division in 1/3 mice
meanwhile
basophilic degeneration was only found in one mouse’s kidney. Conclusion: Rut may cause hepatic and renal toxicity. The toxicity to hepatic and kidney cells induced by drugs can be studied by solo-culture system and co-culture system.
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