Low myo-inositol and high glutamine levels in brain are associated with neuropsychological deterioration after induced hyperammonemia

The neuropsychological effect of hyperammonemia is variable. This study tests the hypothesis that the effect of ammonia on the neuropsychological function in patients with cirrhosis is determined by the ability of the brain to buffer ammonia-induced increase in glutamine within the astrocyte by losi...

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Published in:American journal of physiology: Gastrointestinal and liver physiology 2004-09, Vol.287 (3), p.G503-G509
Main Authors: Shawcross, D L, Balata, S, Olde Damink, S W M, Hayes, P C, Wardlaw, J, Marshall, I, Deutz, N E P, Williams, R, Jalan, R
Format: Article
Language:English
Subjects:
Adult
Aged
Amino Acids - pharmacology
Ammonia - blood
Basal Ganglia - metabolism
Brain Chemistry - physiology
Choline - metabolism
Creatinine - blood
Female
Glutamine - metabolism
Humans
Hyperammonemia - metabolism
Hyperammonemia - psychology
Inositol - metabolism
Liver Cirrhosis - metabolism
Liver Cirrhosis - psychology
Liver Function Tests
Magnetic Resonance Spectroscopy
Male
Middle Aged
Neuropsychological Tests
Signal Transduction - physiology
Temporal Lobe - metabolism
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Summary:The neuropsychological effect of hyperammonemia is variable. This study tests the hypothesis that the effect of ammonia on the neuropsychological function in patients with cirrhosis is determined by the ability of the brain to buffer ammonia-induced increase in glutamine within the astrocyte by losing osmolytes like myo-inositol (mI) and not by the magnitude of the induced hyperammonemia. Fourteen cirrhotic patients with no evidence of overt hepatic encephalopathy were given a 75-g amino acid (aa) solution mimicking the hemoglobin molecule to induce hyperammonemia. Measurement of a battery of neuropsychological function tests including immediate memory, ammonia, aa, and short-echo time proton magnetic resonance spectroscopy were performed before and 4 h after administration of the aa solution. Eight patients showed deterioration in the Immediate Memory Test at 4 h. Demographic factors, severity of liver disease, change in plasma ammonia, and aa profiles after the aa solution were similar in those that showed a deterioration compared with those who did not. In patients who showed deterioration in the memory test, the mI-to-creatine ratio (mI/Cr) was significantly lower at baseline than those that did not deteriorate. In contrast, the glutamate/glutamine-to-Cr ratio was significantly greater in the patients that deteriorated. The observation that deterioration in the memory test scores was greater in those with lower mI/Cr supports the hypothesis that the neuropsychological effects of induced hyperammonemia is determined by the capacity of the brain to handle ammonia-induced increase in glutamine.
ISSN:0193-1857
1522-1547
DOI:10.1152/ajpgi.00104.2004