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NeurotransmitterMetabolites
and Pterins in CSF
Impaired hydroxylation of tyrosine and tryptophan due to
deficiency of BH4 reduces the formation of catecholamine
and serotonin. The measurement of CSF neurotransmitter metabolites
is of capital importance for clinical and treatment follow-up,
as it allows to separate typical from atypical cases of BH4
deficiency (the latter are phenotypically defined by the
absence of clinical signs and symptoms and do not need any
treatment for biogenic amine deficiency).
Metabolism of tyrosine and tryptophan:
Following the hydroxylation
of tyrosine and tryptophan to L-DOPA and 5-hydroxytryptophan,
these products are decarboxylated by the aromatic amino
acid decarboxylase to form the active neurotransmitters dopamine
and serotonin. Dopamine is further hydroxylated by b-hydroxylase
to noradrenaline, which can be methylated to form adrenaline.
The main routes of catabolism of the catecholamines and
serotonin
involve either methylation by O-methyltransferase or formation
of homovanillic acid (HVA) and 5-hydroxyindoleacetic acid
(5HIAA) through the action of aldehyde dehydrogenase and
monoamine oxidase. Depending on the type of HPA, the turnover
of tyrosine and tryptophan can be influenced by different
factors: e.g. actual plasma and CSF phenylalanine levels,
transport of aromatic amino acids across the blood-brain
barrier, residual activity of the defective enzyme in the
brain, or gene dosage effects. Metabolites:
In order to distinguish between the different
variants of BH4 deficiency, i.e. typical (severe, general)
and atypical (mild, peripheral, partial) forms, quantification
of the neurotransmitter metabolites, 5HIAA and HVA, is
essential. Quantification is easily performed using HPLC
with electrochemical
detection. Simultaneously, 3-O-methyl-DOPA, a metabolite
of L-DOPA, and a marker of decarboxylation, can be measured. Differential diagnosis:
Except for the atypical (mild, peripheral,
partial) forms of GTPCH, PTPS, and PCD deficiencies, 5HIAA
and HVA are dramatically decreased in the CSF of patients
with the severe form of BH4 deficiency. The levels of both
metabolites decrease with age in all BH4 deficiencies and
a similar correlation was found in control children. In
the mild forms of DHPR deficiency, 5HIAA is usually decreased,
while HVA levels are normal. In addition to BH4 deficiencies, neurotransmitter metabolites
analysis is essential in disorders presenting without hyperphenylalaninemia:
- Dopa-responsive dystonia; (DRD, Segawa disease),
dominant GTPCH def.; OMIM#600225
- Sepiapterinreductase (SR) deficiency (no OMIM)
- Tyrosine hydroxylase (TH) deficiency; OMIM#191290
- Aromatic L-amino acid decarboxylase (AADC) deficiency;
OMIM#107930
- Dopamine b-hydroxylase (DbH) deficiency; OMIM#223360
Collection of CSF specimen:
Discard the first 0.5 ml of CSF
and collect the next 1-2 ml in a small tube. Keep immediately
frozen at -70°C. There is no need for any additives
or to collect additional CSF fractions. Preconditions:
Before medication, preferably between 8
and 10 h in the morning. Pitfalls:
Unstable in blood-contaminated samples
(centrifuge immediately). Interference by some drugs
in some HPLC systems
(e.g., Panadol, ...). Reference values are age dependent.
Our and most other reference values are established for
the first 1-3 ml of CSF. Some laboratories use higher
CSF fractions
and other reference values which may lead to misinterpretation
of results.
Reference and pathological values
(click on image for larger view)
5HIAA = 5-hydroxyindoleacetic acid; HVA
= homovanillic acid; 3OMD = 3-O-methyldopa; MHPG = 3-methoxy-4-hydroxyphenylglycol;
5MTHF = 5-methyltetrahydrofolic acid
- Hyland K, Biaggioni I, Elpeleg
ON, Nyggard TG, Gibson KM. Disorders of neurotransmitter
metabolism. In: Blau
N, Duran M, Blaskovics M, eds. Physician's Guide
to the Laboratory Diagnosis of Metabolic Diseases.
London: Chapman & Hall,
1996: 79-98.
- Blau N, Barnes I, Dhondt JL. International
database of tetrahydrobiopterin deficiencies. J Inherit
Metab Dis
1996;19:8-14.
- Blau N, Blaskovics M. Hyperphenylalaninemia.
In: Blau N, Duran M, Blaskovics M, eds. Physician's
Guide to the
Laboratory Diagnosis of Metabolic Diseases. London:
Chapman & Hall,
1996: 65-78.
REFERENCES
- Blau N, Thöny B, Cotton RGH, Hyland
K. Disorders of tetrahydrobiopterin and related biogenic
amines. In: Scriver
CR, Beaudet AL, Sly WS, Valle D, Childs B, Vogelstein
B, eds. The Metabolic and Molecular Bases of Inherited
Disease.
8th ed. New York: McGraw-Hill, 2001: 1725-1776.
- Hyland K, Biaggio I, Elpeleg ON, Nyggard
TG, Gibson KM. Disorders of neurotransmitter metabolism.
In: Blau N, Duran M, Blaskovics
M, eds. Physician's Guide to the Laboratory Diagnosis
of Metabolic Diseases. London: Chapman & Hall, 1996:
79-98.
- Blau N, Blaskovics M. Hyperphenylalaninemia.
In: Blau N, Duran M, Blaskovics M, eds. Physician's Guide
to the Laboratory
Diagnosis of Metabolic Diseases. London: Chapman & Hall,
1996: 65-78.
- Bonafé, L., B. Thöny, W. Leimbacher, L. Kierat
and N. Blau (2001). "Diagnosis of Dopa-responsive dystonia
and other tetrahydrobiopterin disorders by the study of biopterin
metabolism in fibroblasts." Clin Chem 47: 477-485.
- Blau,
N., L. Bonafé and B. Thöny (2001). "Tetrahydrobiopterin
deficiencies without hyperphenylalaninemia: Diagnosis and
genetics of Dopa-responsive dystonia and sepiapterin reductase
deficiency." Mol Genet Metab 72: 172-185
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