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Pyrogallol inhibits the growth of gastric cancer SNU-484 cells via induction of apoptosis

Authors:
Woo Hyun Park, Mee Na Park, Yong Hwan Han, Sang Woo Kim

Affiliations:
Department of Physiology, Medical School, Research Institute of Clinical Medicine, Chonbuk National University, JeonJu 561-180, Korea. parkwh71@chonbuk.ac.kr

Doi:
10.3892/ijmm_00000018

Pages:
263-268

Abstract:

Pyrogallol (PG) is a polyphenol compound and is known to be an O2·− generator. We evaluated the effects of PG on the growth of human gastric cancer SNU-484 cells in relation to the cell cycle and apoptosis. Dose-dependent inhibition of cell growth was observed in SNU-484 cells with an IC50 of ≈50 μM following treatment with PG for 72 h. DNA flow cytometric analysis indicated that treatment with PG generally did not induce the specific cell cycle phase arrest. Treatment with 50 μM PG induced apoptosis ≈20%, as evidenced by sub-G1 cells and annexin V-staining cells. Treatment with PG also induced the loss of mitochondrial membrane potential (Δψm) in SNU-484 cells. The intracellular reactive oxygen species (ROS) levels including O·− were significantly increased in PG-treated cells. Furthermore, the depletion of the intracellular glutathione (GSH) content was observed in cells treated with 50 or 80 μM PG. In conclusion, PG inhibited the growth of human gastric cancer SNU-484 cells by inducing cell cycle arrest as well as triggering apoptosis. The changes in ROS and GSH by PG were closely related to apoptosis in SNU-484 cells.

International Journal of Molecular Medicine

August 2008
Volume 22 Number 2


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