Abstract
The treatment of transformed rat cells with micromolar amounts of 5′deoxy 5′methyl thioadenosine induces rapid effects on the rate of methylation of DNA concomitantly with alterations of intracellular pools of S-adenosyl methionine and S-adenosyl homocysteine. Pulse chase labelling experiments indicate that 5′deoxy 5′methylthioadenosine does not inhibit the degradation of S-adenosyl homocysteine but inhibits the comsumption of S-adenosyl methionine. In vitro transmethylation assays performed with heterologous DNA show that low doses of the thioethernucleoside do not significantly affect the DNA methyltransferase activity of cellular extracts. The biological role of 5′deoxy 5′methylthioadenosine, a natural molecule formed during the synthesis of polyamines is discussed.
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