Effects of (2R, 5R)‐6‐heptyne‐2,5‐diamine, a potent inhibitor of l‐ornithine decarboxylase, on rat hepatoma cells cultured in vitro

Abstract

Dl‐α‐Difluoromethylornithine (F₂MeOrn), the most widely‐used inhibitor of l‐ornithine decarboxylase, has been a useful tool to demonstrate that polyamine biosynthesis is required to maintain maximum rates of cell proliferation. However, in most eukaryotic cell systems, F₂MeOrn exerts cytostatic rather than cytotoxic effects. This may be due to the fact that this inhibitor creates only incomplete polyamine deficiency. In particular, F₂MeOrn scarcely depletes intracellular spermine levels.We now demonstrate in rat hepatoma tissue culture (HTC) cells that (2R, 5R)‐6‐heptyne‐2,5‐diamine, a more potent irreversible inhibitor of l‐ornithine decarboxylase than F₂MeOrn, decreases the concentrations of all polyamines including spermine. In parallel with the depletion of these amines, there is a progressive decrease in the rate of cell proliferation and in cell viability. Restoration of the intracellular polyamine content, by addition to the medium of polyamines or a high concentration of l‐ornithine, the substrate of l‐ornithine decarboxylase, further demonstrates that the antiproliferative effects of (2R, 5R)‐6‐heptyne‐2,5‐diamine do result from polyamine deficiency.These findings support the concept that polyamines play an essential function in the cell division processes and emphasize the vital function of spermine in mammalian cells.