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Compartmentation of Lactate Originating from Glycogen and Glucose in Cultured Astrocytes
Authors:Helle?M.?Sickmann,Arne?Schousboe,Keld?Fosgerau,Helle?S.?Waagepetersen  author-information"  >  author-information__contact u-icon-before"  >  mailto:hsw@dfuni.dk"   title="  hsw@dfuni.dk"   itemprop="  email"   data-track="  click"   data-track-action="  Email author"   data-track-label="  "  >Email author
Affiliation:(1) Department of Pharmacology, Danish University of Pharmaceutical Sciences, DK-2100 Copenhagen, Denmark;(2) Pharmacology Research 1, Novo Nordisk A/S, DK-2760 Maaloev, Denmark
Abstract:Brain glycogen metabolism was investigated by employing isofagomine, an inhibitor of glycogen phosphorylase. Cultured cerebellar and neocortical astrocytes were incubated in medium containing [U-13C]glucose in the absence or presence of isofagomine and the amounts and percent labeling of intra- and extracellular metabolites were determined by mass spectrometry (MS). The percent labeling in glycogen was markedly decreased in the presence of isofagomine. Surprisingly, the percent labeling of intracellular lactate was also decreased demonstrating the importance of glycogen turnover. The decrease was limited to the percent labeling in the intracellular pool of lactate, which was considerably lower compared to that observed in the medium in which it was close to 100%. These findings indicate compartmentation of lactate derived from glycogenolysis and that derived from glycolysis. Inhibiting glycogen degradation had no effect on the percent labeling in citrate. However, the percent labeling of extracellular glutamine was slightly decreased in neocortical astrocytes exposed to isofagomine, indicating an importance of glycogen turnover in the synthesis of releasable glutamine. In conclusion, the results demonstrate that glycogen in cultured astrocytes is continuously synthesized and degraded. Moreover, it was found that lactate originating from glycogen is compartmentalized from that derived from glucose, which lends further support to a compartmentalized metabolism in astrocytes. Special issue dedicated to Dr. Bernd Hamprecht.
Keywords:Amino acid  astrocytes  cerebellar  citrate  compartmentation  energy  glucose  [U-13C]glucose  glutamate  glutamine  glycogen analysis  glycogen phosphorylase  glycogen  glycogenolysis  glycolysis  Isofagomine  lactate  LC-MS  mass spectrometry  metabolism  mitochondria  mitochondrial heterogeneity  neocortical  percent labeling  pyruvate carboxylation  TCA cycle  turnover
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