Effect of Yong-dam-sa-gan-tang on apoptosis in human hepatoma HepG2

용담사간탕(龍膽瀉肝湯)에 의해 유도된 MAP kinases 활성화를 통한 간암 세포주 HepG2의 세포사멸

  • Yun, Hyun-Jeong (Department of Prescriptionology, College of Oriental Medicine, Dongguk University) ;
  • Kim, Han-Seong (Department of Prescriptionology, College of Oriental Medicine, Dongguk University) ;
  • Heo, Sook-Kyoung (Department of Prescriptionology, College of Oriental Medicine, Dongguk University) ;
  • Hwang, Seong-Goo (Department of Prescriptionology, College of Oriental Medicine, Dongguk University) ;
  • Park, Won-Hwan (Department of Prescriptionology, College of Oriental Medicine, Dongguk University) ;
  • Park, Sun-Dong (Department of Prescriptionology, College of Oriental Medicine, Dongguk University)
  • 윤현정 (동국대학교 한의과대학 방제학교실) ;
  • 김한성 (동국대학교 한의과대학 방제학교실) ;
  • 허숙경 (동국대학교 한의과대학 방제학교실) ;
  • 황성구 (동국대학교 한의과대학 방제학교실) ;
  • 박원환 (동국대학교 한의과대학 방제학교실) ;
  • 박선동 (동국대학교 한의과대학 방제학교실)
  • Published : 2007.12.30

Abstract

The purpose of this study was to investigate the effect of Yong-dam-sa-gan-tang (YST) on apoptosis in HepG2 cells, First of all. to study the cytotoxic effect of methanol extract of YST on HepG2 cells, the cells were treated with various concentrations of YST and then cell viability was determined by XTT reduction method and trypan blue exclusion assay. YST reduced proliferation of HepG2 cells in a dose-dependent manner. To confirm the induction of apoptosis, HepG2 cells were treated with various concentrations of YST. The cleavage of poly AD P-ribose polymerase (P ARP), a substrate for caspase-3 and a typical sign of apoptosis, and the activation of caspase-3, procaspase-8 and procaspase-8 were examined by western blot analysis. YST decreased procaspase-3, procaspase-8 and procaspase-9 levels in a dose-dependent manner and induced the clevage of PARP. YST triggered the mitochondrial apoptotic signaling by increasing the release of cytochrome c from mitochondria to cytosol. Furthermore, YST also downregulated the anti-apoptotic Bcl-2 and upregulated the pro-apoptotic-Bax. Therefore, this result suggest that YST induced HepG2 cell death through the mitochondrial pathway. Sustained activation of the Ras/Raf/MEK/ERK cascade in cells results in a cell cycle arrest and has been implicated in the differentiation of certain cell types, in many cases acting to promote differentiation. YST decreased the activation of Ras/Raf/MEK/ERK cascade in a dose-dependent manner. These results suggest that YST is potentially useful as a chemo-therapeutic agent in HepG2.

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