Acetate supplementation induces growth arrest of NG2/PDGFRα-positive oligodendroglioma-derived tumor-initiating cells.

[canavan disease]

Cancer is associated with globally hypoacetylated chromatin and considerable attention has recently been focused on epigenetic therapies . N-acetyl-L-aspartate (NAA ), the primary storage form of acetate in the brain , and aspartoacylase (ASPA ), the enzyme responsible for NAA catalysis to generate acetate and ultimately acetyl-Coenzyme A for histone acetylation , are reduced in oligodendroglioma . The short chain triglyceride glyceryl triacetate (GTA ), which increases histone acetylation and inhibits histone deacetylase expression , has been safely used for acetate supplementation in Canavan disease , a leukodystrophy due to ASPA mutation . We demonstrate that GTA induces cytostatic G 0 growth arrest of oligodendroglioma -derived cells in vitro , without affecting normal cells . Sodium acetate , at doses comparable to that generated by complete GTA catalysis , but not glycerol also promoted growth arrest , whereas long chain triglycerides promoted cell growth . To begin to elucidate its mechanism of action , the effects of GTA on ASPA and acetyl-CoA synthetase protein levels and differentiation of established human oligodendroglioma cells (HOG and Hs 683 ) and primary tumor -derived oligodendroglioma cells that exhibit some features of cancer stem cells (grade II OG 33 and grade III OG 35 ) relative to an oligodendrocyte progenitor line (Oli -Neu ) were examined . The nuclear localization of ASPA and acetyl-CoA synthetase-1 in untreated cells was regulated during the cell cycle . GTA-mediated growth arrest was not associated with apoptosis or differentiation , but increased expression of acetylated proteins . Thus , GTA-mediated acetate supplementation may provide a safe , novel epigenetic therapy to reduce the growth of oligodendroglioma cells without affecting normal neural stem or oligodendrocyte progenitor cell proliferation or differentiation .