Triacetin-based acetate supplementation as a chemotherapeutic adjuvant therapy in glioma.

[canavan disease]

Cancer is associated with epigenetic (i .e ., histone hypoacetylation ) and metabolic (i .e ., aerobic glycolysis ) alterations . Levels of 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 , are reduced in glioma ; yet , few studies have investigated acetate as a potential therapeutic agent . This preclinical study sought to test the efficacy of the food additive Triacetin (glyceryl triacetate , GTA ) as a novel therapy to increase acetate bioavailability in glioma cells . The growth -inhibitory effects of GTA , compared to the histone deacetylase inhibitor Vorinostat (SAHA ), were assessed in established human glioma cell lines (HOG and Hs 683 oligodendroglioma , U 87 and U 251 glioblastoma ) and primary tumor -derived glioma stem-like cells (GSCs ), relative to an oligodendrocyte progenitor line (Oli -Neu ), normal astrocytes , and neural stem cells (NSCs ) in vitro . GTA was also tested as a chemotherapeutic adjuvant with temozolomide (TMZ ) in orthotopically grafted GSCs . GTA-induced cytostatic growth arrest in vitro comparable to Vorinostat , but , unlike Vorinostat , GTA did not alter astrocyte growth and promoted NSC expansion . GTA alone increased survival of mice engrafted with glioblastoma GSCs and potentiated TMZ to extend survival longer than TMZ alone . GTA was most effective on GSCs with a mesenchymal cell phenotype . Given that GTA has been chronically administered safely to infants with Canavan disease , a leukodystrophy due to ASPA mutation , GTA-mediated acetate supplementation may provide a novel , safe chemotherapeutic adjuvant to reduce the growth of glioma tumors , most notably the more rapidly proliferating , glycolytic and hypoacetylated mesenchymal glioma tumors .