## Abstract Exogenous diamines and polyamines added to rat hepatoma (HTC) cells in culture rapidly decrease ornithine decarboxylase (ODC) activity. Previous evidence has suggested that these amines act either at the level of blocking new enzyme synthesis or by the induction of a non‐competitive pro
Consequences of aberrant ornithine decarboxylase regulation in rat hepatoma cells
✍ Scribed by Margaret E. Tome; Steven M. Fiser; Eugene W. Gerner
- Publisher
- John Wiley and Sons
- Year
- 1994
- Tongue
- English
- Weight
- 757 KB
- Volume
- 158
- Category
- Article
- ISSN
- 0021-9541
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✦ Synopsis
Arizona 85724 DH23A cells, an a-difluoromethylornithine (DFMO)-resistant variant of rat hepatoma tissue culture cells (HTC), contain high levels of very stable ornithine decarboxylase (ODC). In the absence of DFMO, the high ODC activity results in a large accumulation of endogenous putrescine. Concomitant with the putrescine increase is a period of cytostasis and a subsequent loss of viable cells. In contrast, HTC cells with a moderate polyamine content can be maintained in exponential growth. This suggests that a moderate polyamine concentration is necessary for both optimal cell growth and survival. The cytoxicity observed in the DH23A cells is apparently not due to byproducts of polyamine oxidation or alterations in steady state intracellular p H or free [Ca2'1. It is possible to mimic the effects of high levels of stable ODC by treatment of cells with exogenous putrescine in the presence of DFMO. This suggests that overaccumulation of putrescine is the causative agent in the observed cytotoxicity, although the mechanism is unclear. These data support the hypothesis that downregulation of ODC may be necessary to prevent accumulation of cytotoxic concentrations of the polyamines.
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