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Literature DB >> 26723542

(13)C metabolic flux analysis in neurons utilizing a model that accounts for hexose phosphate recycling within the pentose phosphate pathway.

Hoda M Gebril¹, Bharathi Avula², Yan-Hong Wang³, Ikhlas A Khan⁴, Mika B Jekabsons⁵.

Abstract

Glycolysis, mitochondrial substrate oxidation, and the pentose phosphate pathway (PPP) are critical for neuronal bioenergetics and oxidation-reduction homeostasis, but quantitating their fluxes remains challenging, especially when processes such as hexose phosphate (i.e., glucose/fructose-6-phosphate) recycling in the PPP are considered. A hexose phosphate recycling model was developed which exploited the rates of glucose consumption, lactate production, and mitochondrial respiration to infer fluxes through the major glucose consuming pathways of adherent cerebellar granule neurons by replicating [(13)C]lactate labeling from metabolism of [1,2-(13)C2]glucose. Flux calculations were predicated on a steady-state system with reactions having known stoichiometries and carbon atom transitions. Non-oxidative PPP activity and consequent hexose phosphate recycling, as well as pyruvate production by cytoplasmic malic enzyme, were optimized by the model and found to account for 28 ± 2% and 7.7 ± 0.2% of hexose phosphate and pyruvate labeling, respectively. From the resulting fluxes, 52 ± 6% of glucose was metabolized by glycolysis, compared to 19 ± 2% by the combined oxidative/non-oxidative pentose cycle that allows for hexose phosphate recycling, and 29 ± 8% by the combined oxidative PPP/de novo nucleotide synthesis reactions. By extension, 62 ± 6% of glucose was converted to pyruvate, the metabolism of which resulted in 16 ± 1% of glucose oxidized by mitochondria and 46 ± 6% exported as lactate. The results indicate a surprisingly high proportion of glucose utilized by the pentose cycle and the reactions synthesizing nucleotides, and exported as lactate. While the in vitro conditions to which the neurons were exposed (high glucose, no lactate or other exogenous substrates) limit extrapolating these results to the in vivo state, the approach provides a means of assessing a number of metabolic fluxes within the context of hexose phosphate recycling in the PPP from a minimal set of measurements.

Entities: CellLine Chemical Disease Gene Species

Keywords: Bioenergetics; Glycolysis; Malic enzyme; Mitochondria; Oxidative stress; Pentose phosphate pathway

Mesh：

Substances：
Carbon Isotopes
Hexoses

Year: 2015 PMID： 26723542 PMCID： PMC4762749 DOI： 10.1016/j.neuint.2015.12.008

Source DB: PubMed Journal: Neurochem Int ISSN： 0197-0186 Impact factor: 3.921

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(13)C metabolic flux analysis in neurons utilizing a model that accounts for hexose phosphate recycling within the pentose phosphate pathway.

1. The use of glucose-C14 for the evaluation of the pathways of glucose metabolism.

2. Complex glutamate labeling from [U-13C]glucose or [U-13C]lactate in co-cultures of cerebellar neurons and astrocytes.

3. Assessment at the single-cell level identifies neuronal glutathione depletion as both a cause and effect of ischemia-reperfusion oxidative stress.

4. Metabolic shifts by nutrient manipulation in continuous cultures of BHK cells.

5. Increased pentose phosphate pathway flux after clinical traumatic brain injury: a [1,2-13C2]glucose labeling study in humans.

6. Systems-level metabolic flux profiling identifies fatty acid synthesis as a target for antiviral therapy.

7. Rapid glycation with D-ribose induces globular amyloid-like aggregations of BSA with high cytotoxicity to SH-SY5Y cells.

8. A glucose transporter can mediate ribose uptake: definition of residues that confer substrate specificity in a sugar transporter.

9. Failure to increase glucose consumption through the pentose-phosphate pathway results in the death of glucose-6-phosphate dehydrogenase gene-deleted mouse embryonic stem cells subjected to oxidative stress.

Review 10. Redox regulation of antioxidants, autophagy, and the response to stress: implications for electrophile therapeutics.

1. Updates to a ¹³C metabolic flux analysis model for evaluating energy metabolism in cultured cerebellar granule neurons from neonatal rats.

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3. Current Status of Our Understanding for Brain Integrated Functions and its Energetics.

Review 4. Towards an Understanding of Energy Impairment in Huntington's Disease Brain.

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Review 6. ¹³C metabolic flux analysis: Classification and characterization from the perspective of mathematical modeling and application in physiological research of neural cell.

Review 10. Redox regulation of antioxidants, autophagy, and the response to stress: implications for electrophile therapeutics.

Review 2. Astrocyte Bioenergetics and Major Psychiatric Disorders.

Review 4. Towards an Understanding of Energy Impairment in Huntington's Disease Brain.

Review 5. Glucose as a Major Antioxidant: When, What for and Why It Fails?

Review 6. 13C metabolic flux analysis: Classification and characterization from the perspective of mathematical modeling and application in physiological research of neural cell.

Review 6. ¹³C metabolic flux analysis: Classification and characterization from the perspective of mathematical modeling and application in physiological research of neural cell.