Traumatic brain injury alters methionine metabolism: implications for pathophysiology

Pramod K Dash; Georgene eHergenroeder; Cameron eJeter; Alex eChoi; Nobuhide eKobori; Anthony eMoore

doi:10.3389/fnsys.2016.00036

Frontiers in Systems Neuroscience (Apr 2016)

Traumatic brain injury alters methionine metabolism: implications for pathophysiology

Pramod K Dash,
Georgene eHergenroeder,
Cameron eJeter,
Alex eChoi,
Nobuhide eKobori,
Anthony eMoore

Affiliations

Pramod K Dash: UTHealth McGovern Medical School
Georgene eHergenroeder: University of Texas School of Dentistry
Cameron eJeter: UTHealth McGovern Medical School
Alex eChoi: UTHealth McGovern Medical School
Nobuhide eKobori: UTHealth McGovern Medical School
Anthony eMoore: UTHealth McGovern Medical School

DOI: https://doi.org/10.3389/fnsys.2016.00036
Journal volume & issue: Vol. 10

Abstract

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Methionine is an essential proteinogenic amino acid that is obtained from the diet. In addition to its requirement for protein biosynthesis, methionine is metabolized to generate metabolites that play key roles in a number of cellular functions. Metabolism of methionine via the transmethylation pathway generates S-adenosylmethionine (SAM) that serves as the principal methyl (-CH3) donor for DNA and histone methyltransferases to regulate epigenetic changes in gene expression. SAM is also required for methylation of other cellular proteins that serve various functions and phosphatidylcholine synthesis that participate in cellular signaling.. Under conditions of oxidative stress, homocysteine (which is derived from SAM) enters the transsulfuration pathway to generate glutathione, an important cytoprotective molecule against oxidative damage. As both experimental and clinical studies have shown that traumatic brain injury (TBI) alters DNA and histone methylation and causes oxidative stress, we examined if TBI alters the plasma levels of methionine and its metabolites in human patients. Blood samples were collected from healthy volunteers (n = 20) and patients with mild TBI (GCS > 12; n = 20) or severe TBI (GCS < 8; n = 20) within the first 24 hours of injury. The levels of methionine and its metabolites in the plasma samples were analyzed by either liquid chromatography-mass spectrometry or gas chromatography-mass spectrometry (LC-MS or GC-MS). Severe TBI decreased the levels of methionine, SAM, betaine and 2-methylglycine as compared to healthy volunteers, indicating a decrease in metabolism through the transmethylation cycle. In addition, precursors for the generation of glutathione, cysteine and glycine were also found to be decreased as were intermediate metabolites of the gamma-glutamyl cycle (gamma-glutamyl amino acids and 5-oxoproline). Mild TBI also decreased the levels of methionine, α-ketobutyrate, 2 hydroxybutyrate and glycine, albeit to lesser degrees than detected in the severe TBI group. Taken together, these results suggest that decreased levels of methionine and its metabolic products are likely to alter cellular function in the injured brain and other body systems.

Published in Frontiers in Systems Neuroscience

ISSN: 1662-5137 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry
Website: https://www.frontiersin.org/journals/systems-neuroscience/

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