β-lapachone induced cell death in human hepatoma (HepA2) cells

• Lai, C. C. ^[1] ; Liu, T. J. ^[2] ; Ho, L. K. ^[3] ; Don, M. J. ^[4] ; Chau, Y. P. ^[1]
  1. [1] Institute of Anatomy
  2. [2] 0epartment of Physical Medicine and Rehabititation
  3. [3] Department of Pharmacology, National Yang-Ming Universit
  4. [4] National Research Institute of Chine Medicine, Taipei, Republic of China

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• Localización: Histology and histopathology: cellular and molecular biology, ISSN-e 1699-5848, ISSN 0213-3911, Vol. 13, Nº. 1, 1998, págs. 89-97
• Idioma: inglés
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  • In present study we studied the cytotoxic effects of B-lapachone, a potent anticancer drug, on the human hepatoma cell line (HepA2) under serum-free condition. Most cells died after 2 ,uM B-Iapachone addition at 48 hours. No apoptotic characteristics of DNA ladder was documented by agarose DNA electrophoresis. The blockage of cell cycle at S phase and unscheduled DNA synthesis were demonstrated by flow cytometric analysis and anti-bromodeoxyuridine immunocytochemistry. Ultrastructural observation showed that the swollen mitochondria, dilatation and vesiculation of rER and proliferation of peroxisome-like granules appeared within the cytoplasm of HepA2 cells following drug treatment. Using enzyme cytochemistry, both peroxidase and acid phosphatase activities but not catalase activity were localised in these peroxisome-like granules. Therefore, these results suggested that (a) 13- lapachone has a novel cytotoxic effect on human hepatoma cell; (2) B-lapachone induces the interruption of the cell cycle and unscheduled DNA synthesis in HepA2 cells; and (3) B-lapachone promotes the proliferation of peroxisome-like granules containing peroxidase and acid phosphatase activities without evidence of catalase activity in hepatoma cell line.