Disorders of creatine synthesis


 * The synthesis of creatine occurs in two steps:


 * 1) Reaction catalyzed by L-argininglycinamide diffease (AGAT) – transfer of the amidine group from arginine to glycine to form guanidinoacetate
 * 2) Raction catalyzed by guanidin acetate methyl transformerase (GAMT) – methylation of the amidine group of the guanidinoacetate molecule by the action of S-adenosylmethionine N-guanidinoacetate methyltransferase


 * The synthesis of creatine takes place mainly in the kidneys and pancreas, which have high AGAT activity, and then in the liver, which have high GAMT activity.
 * Creatine from these organs gets through the blood to the organs where it is used (mainly muscles and brain)
 * When creatine enters tissue utilization, the human form of Cl-dependent creatine carrier (CRTR), SLC6A8
 * Part of the intracellular creatine is reversibly converted to high-energy creatine phospahte by the action of creatine kinase (CK), which exists in three cytosol isoforms, the brain type BB-CK, the muscle type MM-CK and the heterodimer MB-CK creatine phosphate turn into creatinine non-enzymate in the muscle

Creatine synthesis disorders

 * Common features are mental retardation, speech delay and epilepsy due to creatine deficiency in the brain
 * They are diagnosable magnetic resonance spectroscopy of the brain, then in the blood, urine and amniotic fluid
 * L-argininglycinamide aminotransferase deficiency (AGAT)
 * Guanidine acetate deficiency methyltransferase (GAMT) – guanidinoacetate accumulates, the most severe clinical manifestations, convulsions, extrapyramidal symptoms
 * SLC6A8 deficiency - increased creatine/creatinine ratio

Inheritance:
 * AGAT and GAMT deficit are autosomal recessive inherited
 * SLC6A8 deficiency is X-linked hereditary

Treatment:
 * Oral creatine supplementation in the form of creatine monohydrate in AGAT and GAMT deficiency
 * Dietary restriction of arginine n GAMT deficiency
 * In patients with SLC6A8 deficiency, no effective treatment has yet been found, the application of extremely high doses of creatine is being tried, glycine and arginine are also administered.

Literature
Category: Pathobiochemistry
 * FERNANDES, John. Diagnosis and treatment of hereditary metabolic disorders. 1st edition. Praha : Triton, 2008. s. 576-580. ISBN 978-80-7387-096-6.