1. CSF Testing in Neurotransmitter Disorders Keith Hyland, Ph.D.
Tel, 678-597-5659
khyland@medicalneurogenetics.com
khyland@mnglab.com
2. Conflict of Interest Disclosure
3. Topics to be Covered Pathways
Methods
Neurotransmitter Disorders
Other Disorders Detected.
4. When to Perform a Lumbar Puncture Standard screening tests are likely normal
Encephalopathy of unknown etiology
Seizures of unknown etiology
“Cerebral Palsy” of unknown etiology
Unexplained movement disorder Explain that not all of these will have seizures but LP is required for diagnosisExplain that not all of these will have seizures but LP is required for diagnosis
5. Disorders of Neurotransmitter Metabolism
Catecholamine (dopamine, and norepinephrine)
Serotonin
6. Sample Collection Sample collection is critical!
Rostro - caudal gradients
Stability of metabolites (particularly tetrahydrobiopterin)
Always call the lab for instructions
(678- 597- 5658)
9. HPLC DIAGNOSIS OF GTP-CYCLOHYDROLASE DEFICIENCY
10. GTP-Cyclohydrolase Deficiency Problems with Diagnosis? No hyperphenylalaninemia
Same CSF metabolite pattern can be seen following ischemia / hypoxia
Same CSF pattern can be seen following insult to dopaminergic cells
11. Definitive Diagnosis
Fibroblast enzyme assay
Genomic sequencing
13. HPLC Diagnosis of Sepiapterin Reductase Deficiency
14. Caveats? Dihydropteridine reductase deficiency can lead to similar metabolite changes.
Definitive diagnosis:
Fibroblast enzyme assay
Genomic sequencing
Sepiapterin in CSF
16. HPLC DIAGNOSIS OF TYROSINE HYDROXYLASE DEFICIENCY
19. HPLC Diagnosis of AADC Deficiency
20. Aromatic L-Amino Acid Decarboxylase Deficiency – Definitive Diagnosis?
Plasma enzyme assay
Mutation analysis available
22. Pyridox(am)ine 5'-phosphate Oxidase Deficiency.��PNPO – Gene map locus 17q31.22�
CSF threonine, +/- glycine
CSF 3-OMD
CSF 5HIAA, CSF HVA
Urinary vanillactic acid
23. Pyridox(am)ine 5'-phosphate Oxidase Deficiency. L-dopa Dopamine
AADC
AADC requires vitamin B6 as a cofactor
Treatment with pyridoxine
NO EFFECT
26. Pyridoxal 5’-phosphate Responsive Seizures Treatment with pyridoxal 5’ phosphate
(10 – 50 mg/kg/day)
Immediate cessation of seizures
29. Pyridoxal 5’-phosphate Responsive Seizures Defect lies in the conversion of pyridoxine to pyridoxal 5’-phosphate
Pyridoxamine Phosphate Oxidase (PNPO) Deficiency
Clayton PT et al Lancet 2003
30. Pyridoxal 5’-phosphate Responsive Seizures CSF pyridoxal 5’-phosphate concentrations are low.
Ormazabal et al 2008
31. Folinic Acid Responsive Seizures� Serendipity and Science? Explain the way that the seizure disorder was first discoveredExplain the way that the seizure disorder was first discovered
32. CSF Neurotransmitter Metabolite�(HPLC – electrochemical detection)
33. Etiology
34. Serendipity and Science Explain the way that the seizure disorder was first discoveredExplain the way that the seizure disorder was first discovered
35. Pyridoxine responsive seizures� Mutations in antiquitin in individuals with pyridoxine-dependent seizures.�
Mills et al Nat Med 2006
36. Pathophysiologic mechanism in pyridoxine responsive seizures
37. Relationship between AASA and unknown
38. Pyridoxal 5’-phosphate Responsive Seizures Pyridoxal 5'-phosphate may be curative in early-onset epileptic encephalopathy.
Hoffmann et. al. J. Inherit Metab Dis 2007
39. Test To Request
40. Conclusions All neonates and infants with intractable seizures of unknown origin should have a lumbar puncture performed and neurotransmitter metabolites analyzed.
Pyridoxal 5’-phosphate responsive seizures
Folinic acid responsive seizures/Pyridoxine responsive seizures
41. The vesicular amine transporter acts via an ATP-dependent process linked to a proton pump.
VAT has a dual role :Maintain a ready supply of neurotransmitter and
Mediate release.
Action potential arrives, CA2+ channels open. Get calcium influx. The increased calcium promotes fusion of the vesicle with the neuronal membrane.
DA reuptake by the DAT is energy dependent coupled to a NA+ gradient across the neuronal membrane
Action is via G protein- coupled receptors. These are many types and en masse are termed the G protein receptor-linked superfamily.
The slide depicts dopamine binding to two different receptors leading to either the inhibition (D2,3,4) or stimulation (D1, D5) of adenylate cyclase.
Mechanism in both cases involves GTP binding to the G protein, change in activity of adenylate cyclase and a change in intracellular cyclic AMP levels which in turn regulate the activity of protein kinase A.
G protein coupled receptors can also act by altering phosphoinositide hydrolysisleading to protein kinase C activation and release of CA2+.
HOW DO RELEASE MODULATING AUTORECEPTORS WORK?
The vesicular amine transporter acts via an ATP-dependent process linked to a proton pump.
VAT has a dual role :Maintain a ready supply of neurotransmitter and
Mediate release.
Action potential arrives, CA2+ channels open. Get calcium influx. The increased calcium promotes fusion of the vesicle with the neuronal membrane.
DA reuptake by the DAT is energy dependent coupled to a NA+ gradient across the neuronal membrane
Action is via G protein- coupled receptors. These are many types and en masse are termed the G protein receptor-linked superfamily.
The slide depicts dopamine binding to two different receptors leading to either the inhibition (D2,3,4) or stimulation (D1, D5) of adenylate cyclase.
Mechanism in both cases involves GTP binding to the G protein, change in activity of adenylate cyclase and a change in intracellular cyclic AMP levels which in turn regulate the activity of protein kinase A.
G protein coupled receptors can also act by altering phosphoinositide hydrolysisleading to protein kinase C activation and release of CA2+.
HOW DO RELEASE MODULATING AUTORECEPTORS WORK?
42. Many CSF samples have unexplained low HVA and 5-HIAA concentrations? Defective VMAT2 ?
VMAT2 knockout shows low levels of dopamine, serotonin and metabolites
Genomic sequencing of VMAT2 is available.
No mutations found to date.
Only 3 samples examined
43. The vesicular amine transporter acts via an ATP-dependent process linked to a proton pump.
VAT has a dual role :Maintain a ready supply of neurotransmitter and
Mediate release.
Action potential arrives, CA2+ channels open. Get calcium influx. The increased calcium promotes fusion of the vesicle with the neuronal membrane.
DA reuptake by the DAT is energy dependent coupled to a NA+ gradient across the neuronal membrane
Action is via G protein- coupled receptors. These are many types and en masse are termed the G protein receptor-linked superfamily.
The slide depicts dopamine binding to two different receptors leading to either the inhibition (D2,3,4) or stimulation (D1, D5) of adenylate cyclase.
Mechanism in both cases involves GTP binding to the G protein, change in activity of adenylate cyclase and a change in intracellular cyclic AMP levels which in turn regulate the activity of protein kinase A.
G protein coupled receptors can also act by altering phosphoinositide hydrolysisleading to protein kinase C activation and release of CA2+.
HOW DO RELEASE MODULATING AUTORECEPTORS WORK?
The vesicular amine transporter acts via an ATP-dependent process linked to a proton pump.
VAT has a dual role :Maintain a ready supply of neurotransmitter and
Mediate release.
Action potential arrives, CA2+ channels open. Get calcium influx. The increased calcium promotes fusion of the vesicle with the neuronal membrane.
DA reuptake by the DAT is energy dependent coupled to a NA+ gradient across the neuronal membrane
Action is via G protein- coupled receptors. These are many types and en masse are termed the G protein receptor-linked superfamily.
The slide depicts dopamine binding to two different receptors leading to either the inhibition (D2,3,4) or stimulation (D1, D5) of adenylate cyclase.
Mechanism in both cases involves GTP binding to the G protein, change in activity of adenylate cyclase and a change in intracellular cyclic AMP levels which in turn regulate the activity of protein kinase A.
G protein coupled receptors can also act by altering phosphoinositide hydrolysisleading to protein kinase C activation and release of CA2+.
HOW DO RELEASE MODULATING AUTORECEPTORS WORK?
44. Many CSF samples have isolated low HVA concentrations Defective dopamine transporter (DAT)? DAT knockout shows low levels of dopamine and HVA
Genomic sequencing of DAT is available.
No mutations found.
6 samples examined
45. Dopamine transporter (DAT1) Homozygous loss-of-function mutations
in the gene encoding the dopamine
transporter are associated with infantile parkinsonism-dystonia.
CSF HVA LEVELS ARE ELEVATED!!
Kurian et al J Clin Invest 2009
47. Dopamine Transporter (DAT1) Deficiency Early onset Parkinsonian symptoms
Pyramidal tract features
Dystonia
Global Developmental delay
Normal MRI
HVA/5HIAA ratio 5 to 13.4
Normal < 2.5
5HIAA within normal range.
48. Future Directions Serotonin transporter (SERT)
Elevated 5HIAA??
Receptors – Pre and Post Synaptic
Serotonin
Dopamine
Norepinephrine
Next generation sequencing
