Polyamine depletion delays apoptosis of rat intestinal epithelial cells

The polyamines spermidine, spermine, and their precursorputrescine are essential for cell growth and the regulation of the cellcycle. Recent studies suggest that excessive accumulation of polyaminesfavors either malignant transformation or apoptosis, depending on thecell type and the stimulus. This study examines the involvement ofpolyamines in the induction of apoptosis by the DNA topoisomerase Iinhibitor, camptothecin. In IEC-6 cells, camptothecin induced apoptosiswithin 6 h, accompanied by detachment of cells. Detached cells showedDNA laddering and caspase 3 induction, characteristic features ofapoptosis. Depletion of putrescine, spermidine, and spermine byDL--difluoromethylornithine (DFMO), a specific inhibitorof ornithine decarboxylase (ODC) that is the first rate-limiting enzymefor polyamine biosynthesis, decreased the apoptotic index. Delayedapoptosis was accompanied by a decrease in caspase 3 activity inpolyamine-depleted cells. Addition of putrescine restored the inductionof apoptosis as indicated by an increase in the number of detachedcells and caspase 3 activity. Polyamine depletion did not change thelevel of caspase 3 protein. Inhibition of S-adenosylmethioninedecarboxylase by a specific inhibitor diethylglyoxalbis-(guanylhydrazone); DEGBG] led to depletion of spermidine andspermine with a significant accumulation of putrescine and induction ofODC. The DEGBG-treated cells showed an increase in apoptosis,suggesting the importance of putrescine in the apoptotic process.Addition of putrescine to DFMO-treated cell extracts did not increasecaspase 3 activity. The above results indicate that polyamine depletiondelays the onset of apoptosis in IEC-6 cells and confers protectionagainst DNA damaging agents, suggesting that polyamines might beinvolved in the caspase activating signal cascade.