Unit Converter
Glutamic Acid (Glu)

SI UNITS (recommended)

CONVENTIONAL UNITS

(Non-Essential Amino Acid – Central to Nitrogen Metabolism, Neurotransmission & IEM Screening)

Synonyms

  • Glutamate (when ionized)
  • Glutamic acid
  • L-Glutamate
  • Glu
  • Plasma glutamate

Units of Measurement

  • µmol/L
  • mg/L
  • mg/dL
  • mg/100 mL
  • mg%
  • µg/mL

Key Conversions

(Molecular Weight ≈ 147.13 g/mol)

1 mg/L = 6.80 µmol/L
 1 mg/dL = 68.0 µmol/L
 1 µg/mL = 1 mg/L
 mg/dL = mg% = mg/100 mL
 1 µmol/L = 0.147 mg/L

Description

Glutamic acid (glutamate) is a non-essential amino acid and the body’s most abundant excitatory neurotransmitter.

It plays essential roles in:

  • Nitrogen transport
  • Amino acid metabolism
  • Ammonia detoxification
  • Urea cycle linkage
  • Brain neurotransmission
  • Precursor to γ-aminobutyric acid (GABA)

Plasma glutamate levels are clinically relevant mainly in inborn errors of metabolism, liver disease, and nutritional assessment.

Physiological Role

1. Neurotransmitter Function

Glutamate is the primary excitatory neurotransmitter in the CNS.
 Involved in:

  • Learning & memory (NMDA receptor)
  • Synaptic plasticity
  • Neuronal development

2. Amino Acid Metabolism

  • Central molecule in amino group transamination
  • Precursor for alanine, aspartate, proline, glutamine
  • Key part of the glutamate–glutamine cycle

3. Detoxification

  • Converts ammonia to glutamine (glutamine synthetase)
  • Helps maintain nitrogen balance

4. Energy Pathways

Converted to:

  • α-ketoglutarate → enters Krebs cycle

Clinical Significance

High Glutamic Acid (Hyperglutamatemia)

Seen in metabolic and hepatic disorders.

1. Inborn Errors of Metabolism (IEM)

Most significant diagnostic use.

  • Glutamate dehydrogenase deficiency (rare)
  • Pyridoxine-dependent epilepsy
  • Urea cycle defects (e.g., CPS, OTC deficiencies)
  • Hyperinsulinism-hyperammonemia (HI/HA) syndrome
  • Maple syrup urine disease (indirect effect)
  • Mitochondrial disorders

2. Liver Disease

Impaired urea cycle → accumulation of glutamate.

3. Hyperammonemia

Ammonia accumulation increases conversion to glutamate and glutamine.

4. Neurologic Disorders

Some cases of:

  • Epilepsy
  • Traumatic brain injury
  • Neurodegeneration
     have altered glutamate levels.

5. Dietary Supplementation

Excessive intake (e.g., monosodium glutamate) rarely causes clinically measurable plasma elevation.

Low Glutamic Acid

  • Severe malnutrition
  • Vitamin B6 (pyridoxine) deficiency
  • Chronic liver failure
  • Impaired transamination activity
  • Some mitochondrial diseases

Reference Intervals

(Tietz 8E + Mayo + ARUP + IEM guidelines)

Plasma Glutamate

  • 20 – 80 µmol/L (adults)
  • Higher in newborns: 40–120 µmol/L
  • CSF glutamate: Much lower and tightly regulated

Critical Values

  • >200 µmol/L → strongly suggest metabolic disorder or severe hepatic dysfunction
  • <10 µmol/L → rare; suggests malnutrition or transamination defects

Diagnostic Uses

1. Inborn Errors of Metabolism

Essential in the workup of:

  • Urea cycle disorders
  • Hyperinsulinism-hyperammonemia syndrome
  • Organic acidemias
  • Pyridoxine-dependent epilepsy

Often measured alongside:

  • Glutamine
  • Ammonia
  • Alanine
  • Citrulline
  • Ornithine

2. Liver Function & Hyperammonemia

Elevations correlate with:

  • Hepatic encephalopathy
  • Ammonia toxicity

3. Nutrition Assessment

Part of amino acid profile in malnutrition or parenteral nutrition monitoring.

4. Neurological Research

(Glutamate measured in plasma or CSF for research; limited clinical application.)

Analytical Notes

  • Use fasting plasma (EDTA or heparin)
  • Sample must be kept on ice immediately
  • Deproteinization required to prevent post-collection metabolism
  • Not reliable in serum (platelet release)
  • Amino acid analysis by HPLC or tandem mass spectrometry

Clinical Pearls

  • Plasma glutamate is a marker of nitrogen load and urea cycle stress.
  • High glutamate with high ammonia → think urea cycle defect.
  • In neonates, elevated glutamate + seizures → consider pyridoxine-dependent epilepsy.
  • Glutamine:glutamate ratio often more informative than glutamate alone.
  • Liver disease increases both glutamate and glutamine due to impaired detoxification.

Interesting Fact

Glutamate is the most abundant excitatory neurotransmitter in the human brain, yet high plasma levels do not necessarily reflect CNS levels due to tight blood-brain barrier control.

References

  1. Tietz Clinical Chemistry & Molecular Diagnostics, 8th Edition - Amino Acids.
  2. ACMG Guidelines - Inborn Errors of Metabolism.
  3. Mayo Clinic Laboratories - Amino Acid Profile.
  4. ARUP Consult - Urea Cycle Disorders.
  5. NIH Genetics - Glutamate Metabolism.
  6. MedlinePlus / NIH - Amino Acid Testing.

Last updated: January 26, 2026

Reviewed by : Medical Review Board

Change language

Other Convertors