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Abstract
In this report, we demonstrate that valproic acid (VPA), a drug that has been used for decades in the treatment of epilepsy and as a mood stabilizer, triggers replication-independent active demethylation of DNA. Thus, this drug can potentially reverse DNA methylation patterns and erase stable methylation imprints on DNA in non-dividing cells. Recent discoveries support a role for VPA in the regulation of methylated genes; however, the mechanism has been unclear because it is difficult to dissociate active demethylation from the absence of DNA methylation during DNA synthesis. We therefore took advantage of an assay that measures active DNA demethylation independently from other DNA methylation and DNA replication activities in human embryonal kidney 293 cells. We show that VPA induces histone acetylation, DNA demethylation, and expression of an ectopically methylated CMV-GFP plasmid in a dose-dependent manner. In contrast, valpromide, an analogue of VPA that does not induce histone acetylation, does not induce demethylation or expression of CMV-GFP. Furthermore, we illustrate that methylated DNA-binding protein 2/DNA demethylase (MBD2/dMTase) participates in this reaction since antisense knockdown of MBD2/dMTase attenuates VPA-induced demethylation. Taken together, our data support a new mechanism of action for VPA as enhancing intracellular demethylase activity through its effects on histone acetylation and raises the possibility that DNA methylation is reversible independent of DNA replication by commonly prescribed drugs.
Highlights
Valproic acid/Valproate/2-n-propylpentanoic acid (VPA) has been used for decades in the treatment of epilepsy and is effective as a mood stabilizer and in migraine therapy
Since we have shown that active demethylation can be induced or inhibited by modifying histone acetylation [18, 22], 1 The abbreviations used are: MBD, methylated DNA-binding protein; MBD2/dMTase, MBD2/DNA demethylase; VPA, valproate/valproic acid; VPM, valpromide; histone deacetylases (HDACs), histone deacetylase; Ac-H3, acetyl histone H3; TSA, trichostatin A; 5-aza, 2Јdeoxycytidine-5-aza-CdR; GFP, green fluorescent protein; Chromatin Immunoprecipitation (ChIP), chromatin immunoprecipitation
Since we have shown that the plasmid does not replicate during the time frame of the experiment, nor is it methylated by DNA methyltransferases, the demethylation measured by this assay is active demethylation and not passive demethylation
Summary
Valproic acid/Valproate/2-n-propylpentanoic acid (VPA) has been used for decades in the treatment of epilepsy and is effective as a mood stabilizer and in migraine therapy. It was demonstrated that the reelin gene, which encodes a neuronal protein that is down-regulated in schizophrenia, is methylated in neuronal precursor cells, accompanied by minimal expression. Following treatment of these cells by 5Ј-aza-2Ј-deoxycytidine (5-aza-CdR), a known DNA methylation inhibitor, or VPA, the expression of reelin is induced [7]. VPA can revert the down-regulation of both reelin and gad caused by L-methionine, an agent shown to increase DNA methylation [8]. Both 5-aza-CdR and VPA induce the expression of 5-lipoxygenase [9]. If VPA acts by this mechanism, it might be used to stably erase methylation of specific genes in tissues where DNA replication does not take place
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