AI Article Synopsis

  • Neocryptolepine derivatives, especially 8-Fluoroneocryptolepine (8FNC), have shown promising cytotoxic effects against gastric cancer, demonstrating greater potency than traditional treatments like cisplatin and fluorouracil.
  • 8FNC's effectiveness was enhanced through structural modifications, allowing it to selectively target AGS gastric cancer cells while reducing harm to healthy gastric mucosa cells (GES-1).
  • The compound induces apoptosis in AGS cells by disrupting the cell cycle and influencing the PI3K/AKT signaling pathway, indicating its potential as a lead candidate for gastric cancer treatment.

Article Abstract

Neocryptolepine derivatives have attracted great interest because of their unique cytotoxic activity. 8-Fluoroneocryptolepine (8FNC) was synthesized, and its cytotoxicity was evaluated by MTT assay in AGS gastric cancer cells and gastric mucosa GES-1 cells. 8-Fluoroneocryptolepine showed greater selectivity and cytotoxicity to AGS cells than the cisplatin (CIS) and fluorouracil (5-Fu) commonly used in clinical treatment of gastric cancer. Most importantly, we significantly improved the cytotoxic effect of 8FNC against AGS cells by structural modification and reduced the cytotoxicity against GES-1 cells compared with neocryptolepine. We further evaluated the activity of 8FNC against AGS cells . Our results indicate that 8FNC arrests the AGS cell cycle in the G2/M phase, reduces the mitochondrial membrane potential of AGS cells, and drives the initiation of apoptotic body formation in 8FNC-induced apoptosis. Moreover, 8FNC exhibits strong inhibitory effects on AGS cell migration. Studies on the molecular mechanisms of the cytotoxic activities of 8FNC revealed that it may play a significant role in the inhibitory effect on AGS human gastric cancer cells through the PI3K/AKT signaling pathway. In conclusion, 8FNC may become a promising lead compound in the development of potential clinical drug candidates for the treatment of gastric cancer.

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Source
http://dx.doi.org/10.1021/acs.jnatprod.1c01078DOI Listing

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