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Potential anticancer effect of sodium caprate on human gastric cancer cells.

Nam-Hee KimJung Ho ParkDong-Hoe KooTaeheon LeeJeong-Yoon YangHee-Young Lee
Published in: Human & experimental toxicology (2022)
The role of sodium caprate (C 10 ) in enhancing drug absorption is well established; however, little information is available on its role as an anticancer drug. This study aimed to evaluate the anticancer effect of C 10 in gastric cancer cells. The mechanism of cytotoxicity of C 10 was evaluated by western blotting following treatment of the gastric cancer cells with various concentrations of C 10 . C 10 cytotoxicity was measured via MTS (3-(4, 5-dimethylthiazol-2-yl)-5-(3-carboxymethoxyphenyl)-2-(4-sulfophenyl)-2H tetrazolium), lactate dehydrogenase (LDH), cAMP, and ATP assays. Gastric cancer cells were observed by electron microscopy following treatment with C 10 . Then, xenograft mice that were inoculated with gastric cancer cells were treated with C 10 for 4 weeks, after which the changes in tumor size were measured. C 10 triggered apoptosis in the gastric cancer cells through the mitochondrial pathway at concentrations of more than 0.2 mM. However, 15 mM of C 10 induced necrosis in gastric cancer cells by causing cellular swelling and the formation of holes in the cell membrane. Levels of cAMP and ATP decreased significantly following exposure to 15 mM C 10 for 1 h. Additionally, the size of the xenograft tumors was significantly reduced by 24% after 4 weeks of C 10 treatment ( p < 0.05). This study indicates that C 10 induces apoptosis and necrosis in a concentration-dependent manner and has clear anticancer effects on gastric cancer cells.
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