Clinical and molecular characterisation of hereditary dopamine transporter deficiency syndrome: an observational cohort and experimental study

doi:10.1016/S1474-4422(10)70269-6

. 2011 Jan;10(1):54-62.

doi: 10.1016/S1474-4422(10)70269-6. Epub 2010 Nov 25.

Clinical and molecular characterisation of hereditary dopamine transporter deficiency syndrome: an observational cohort and experimental study

Affiliations

Affiliation

¹ Department of Medical and Molecular Genetics, University of Birmingham School of Medicine, Institute of Biomedical Research, and Centre for Rare Diseases and Personalised Medicine, University of Birmingham, Birmingham, UK. manju_dave@hotmail.com

PMID: 21112253
PMCID: PMC3002401
DOI: 10.1016/S1474-4422(10)70269-6

Clinical and molecular characterisation of hereditary dopamine transporter deficiency syndrome: an observational cohort and experimental study

Manju A Kurian et al. Lancet Neurol. 2011 Jan.

. 2011 Jan;10(1):54-62.

doi: 10.1016/S1474-4422(10)70269-6. Epub 2010 Nov 25.

Affiliation

¹ Department of Medical and Molecular Genetics, University of Birmingham School of Medicine, Institute of Biomedical Research, and Centre for Rare Diseases and Personalised Medicine, University of Birmingham, Birmingham, UK. manju_dave@hotmail.com

PMID: 21112253
PMCID: PMC3002401
DOI: 10.1016/S1474-4422(10)70269-6

Abstract

Background: dopamine transporter deficiency syndrome is the first identified parkinsonian disorder caused by genetic alterations of the dopamine transporter. We describe a cohort of children with mutations in the gene encoding the dopamine transporter (SLC6A3) with the aim to improve clinical and molecular characterisation, reduce diagnostic delay and misdiagnosis, and provide insights into the pathophysiological mechanisms.

Methods: 11 children with a biochemical profile suggestive of dopamine transporter deficiency syndrome were enrolled from seven paediatric neurology centres in the UK, Germany, and the USA from February, 2009, and studied until June, 2010. The syndrome was characterised by detailed clinical phenotyping, biochemical and neuroradiological studies, and SLC6A3 mutation analysis. Mutant constructs of human dopamine transporter were used for in-vitro functional analysis of dopamine uptake and cocaine-analogue binding.

Findings: children presented in infancy (median age 2·5 months, range 0·5-7) with either hyperkinesia (n=5), parkinsonism (n=4), or a mixed hyperkinetic and hypokinetic movement disorder (n=2). Seven children had been initially misdiagnosed with cerebral palsy. During childhood, patients developed severe parkinsonism-dystonia associated with an eye movement disorder and pyramidal tract features. All children had raised ratios of homovanillic acid to 5-hydroxyindoleacetic acid in cerebrospinal fluid, of range 5·0-13·2 (normal range 1·3-4·0). Homozygous or compound heterozygous SLC6A3 mutations were detected in all cases. Loss of function in all missense variants was recorded from in-vitro functional studies, and was supported by the findings of single photon emission CT DaTSCAN imaging in one patient, which showed complete loss of dopamine transporter activity in the basal nuclei.

Interpretation: dopamine transporter deficiency syndrome is a newly recognised, autosomal recessive disorder related to impaired dopamine transporter function. Careful characterisation of patients with this disorder should provide novel insights into the complex role of dopamine homoeostasis in human disease, and understanding of the pathophysiology could help to drive drug development.

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Figures

**Figure 1**
Nuclear brain imaging with single photon emission CT DaTSCAN in a control patient (A), a patient with juvenile parkinsonism of unknown aetiology (B), and patient 3 (C) Patients were age-matched. (A) Normal distribution of dopamine transporter sites. (B) Bilateral symmetrical loss of dopamine transporter sites from lentiform nuclei. (C) Complete loss of dopamine transporter sites in the basal nuclei, resulting in high background counts without any activity from basal nuclei.

**Figure 2**
Expression of wild-type and mutant human dopamine transporter in HEK293 cells Protein was probed with antibodies against the C-terminal (A) and N-terminal (B) of the dopamine transporter, and with anti-β-actin antibody to show the relative equivalent loading of total protein (C). The same amount of total lysate protein was loaded in all lanes. The mutations not reported in previous studies are shown in the same sequence as in webappendix p 10, starting with patient 5.

**Figure 3**
Diagnostic algorithm for dopamine transporter deficiency syndrome and differential disorders CSF=cerebrospinal fluid. Neurometabolic investigations need to be tailored according to the clinical presentation, but could include serum assessment of lactate, ammonia, biotinidase, carnitine, acylcarnitine profile, aminoacids, thyroid function tests (including free triiodothyronine); urine assessment of organic acids, aminoacids, purines, and pyrimidines; and CSF assessment of lactate, glucose, aminoacids, and protein. Assessment of a muscle or skin biopsy sample, specialist metabolic tests, and genetic investigation might also be appropriate. A CSF neurotransmitter profile should include homovanillic acid, 5-hydroxyindoleacetic acid, and pterins.,

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Comment in

Infantile parkinsonism-dystonia due to dopamine transporter gene mutations: another genetic twist.
Blackstone C. Blackstone C. Lancet Neurol. 2011 Jan;10(1):24-5. doi: 10.1016/S1474-4422(10)70280-5. Epub 2010 Nov 25. Lancet Neurol. 2011. PMID: 21112252 No abstract available.
A specific subtype of infantile Parkinsonism-dystonia identified.
Fisher E. Fisher E. Clin Genet. 2011 Apr;79(4):332-4. doi: 10.1111/j.1399-0004.2011.01633.x. Epub 2011 Feb 18. Clin Genet. 2011. PMID: 21261603 No abstract available.

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References

1. Torres GE, Gainetdinov RR, Caron MG. Plasma membrane monoamine transporters: structure, regulation and function. Nat Rev Neurosci. 2003;4:13–25. - PubMed
1. Carlsson A. Perspectives on the discovery of central monoaminergic neurotransmission. Annu Rev Neurosci. 1987;10:19–40. - PubMed
1. Carlsson A. A paradigm shift in brain research. Science. 2001;294:1021–1024. - PubMed
1. Greengard P. The neurobiology of slow synaptic transmission. Science. 2001;294:1024–1030. - PubMed
1. Hoffmann GF, Surtees RA, Wevers RA. Cerebrospinal fluid investigations for neurometabolic disorders. Neuropediatrics. 1998;29:59–71. - PubMed

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[1] Torres GE, Gainetdinov RR, Caron MG. Plasma membrane monoamine transporters: structure, regulation and function. Nat Rev Neurosci. 2003;4:13–25. - PubMed

[2] Torres GE, Gainetdinov RR, Caron MG. Plasma membrane monoamine transporters: structure, regulation and function. Nat Rev Neurosci. 2003;4:13–25. - PubMed

[3] Carlsson A. Perspectives on the discovery of central monoaminergic neurotransmission. Annu Rev Neurosci. 1987;10:19–40. - PubMed

[4] Carlsson A. Perspectives on the discovery of central monoaminergic neurotransmission. Annu Rev Neurosci. 1987;10:19–40. - PubMed

[5] Carlsson A. A paradigm shift in brain research. Science. 2001;294:1021–1024. - PubMed

[6] Carlsson A. A paradigm shift in brain research. Science. 2001;294:1021–1024. - PubMed

[7] Greengard P. The neurobiology of slow synaptic transmission. Science. 2001;294:1024–1030. - PubMed

[8] Greengard P. The neurobiology of slow synaptic transmission. Science. 2001;294:1024–1030. - PubMed

[9] Hoffmann GF, Surtees RA, Wevers RA. Cerebrospinal fluid investigations for neurometabolic disorders. Neuropediatrics. 1998;29:59–71. - PubMed

[10] Hoffmann GF, Surtees RA, Wevers RA. Cerebrospinal fluid investigations for neurometabolic disorders. Neuropediatrics. 1998;29:59–71. - PubMed

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Clinical and molecular characterisation of hereditary dopamine transporter deficiency syndrome: an observational cohort and experimental study

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Clinical and molecular characterisation of hereditary dopamine transporter deficiency syndrome: an observational cohort and experimental study

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