Anticancer Effect of Gambogic Acid in Gastric Cancer Line SGC-7901

We investigate the anticancer effect of a traditional Chinese medicine gambogic acid (GA) in human gastric cancer line SGC-7901 and further study the mechanism of apoptosis induction of GA.Low differential human gastric cancer line SGC-7901 were treated with GA at different doses and different times, the inhibitory rates were detected by MTT assay. Apoptosis induced by GA in SGC-7901 cells was observed by Annexin-V/PI doubling staining flow cytometry assay. And T/C (%) was chosen to detect the inhibition of GA on human gastric adenocar-cinoma SGC-7901 nude mice xenografts. Apoptosis on nude mice xenografts was observed by Annexin-V/PI doubling staining flow cytometry assay and DNA fragmentation assay. To further determine the molecular mechanism of apoptosis induced by GA, the changes on the expression of bcl-2 and bax genes were detected by RT-PCR.After incubation with GA, low differential human gastric cancer line SGC-7901 was dramatically inhibited in a dose-dependent manner. After these cells were exposed to GA for 24, 48 and 72 h, the IC50 value was 1.02±±0.05, 1.41±±0.20 and 1.14±± 0.19 μmol/L, respectively. Apoptosis in SGC-7901 cells induced by GA was observed by Annexin-V/PI doubling staining flow cytome-try assay. The apoptotic population of SGC-7901 cells was about 12.96% and 24.58%, respectively, when cells were incuba-ted with 1.2 μmol/L GA for 48 and 72 h. T/C (%) of human gastric carcinoma adeno-carcinoma SGC-7901 nude mice xenografts was 44.3, when the nude mice were treated with GA (8 mg/kg). Meanwhile, apoptosis induced by GA was observed in human gastric carcinoma adenocarcinoma SGC-7901 nude mice xenografts. The increase of bax gene and the decrease of bc1-2 gene expressions were found by RT-PCR.The inhibition of GA on human gastric cancer line SGC-7901 was confirmed. This effect connects with the inducing apoptosis in SGC-7901 cells and the molecular mechanism might be related to th- - e reduction of expression of apoptosis-regulated gene bcl-2, and the improvement of the expression of apoptosis-regulated gene bax. The result was also confirmed in vivo.