Homozygous loss-of-function mutations in the gene encoding the dopamine transporter are associated with infantile parkinsonism-dystonia.

Manju Kurian; J Zhen; SY Cheng; Y Li; SR Mordekar; P Jardine; Neil Morgan; Esther Meyer; Louise Tee; Shanaz Pasha; E Wassmer; SJ Heales; Paul Gissen; ME Reith; Eamonn Maher

doi:10.1172/JCI39060

Homozygous loss-of-function mutations in the gene encoding the dopamine transporter are associated with infantile parkinsonism-dystonia.

Manju Kurian, J Zhen, SY Cheng, Y Li, SR Mordekar, P Jardine, Neil Morgan, Esther Meyer, Louise Tee, Shanaz Pasha, E Wassmer, SJ Heales, Paul Gissen, ME Reith, Eamonn Maher

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Abstract

Genetic variants of the SLC6A3 gene that encodes the human dopamine transporter (DAT) have been linked to a variety of neuropsychiatric disorders, particularly attention deficit hyperactivity disorder. In addition, the homozygous Slc6a3 knockout mouse displays a hyperactivity phenotype. Here, we analyzed 2 unrelated consanguineous families with infantile parkinsonism-dystonia (IPD) syndrome and identified homozygous missense SLC6A3 mutations (p.L368Q and p.P395L) in both families. Functional studies demonstrated that both mutations were loss-of-function mutations that severely reduced levels of mature (85-kDa) DAT while having a differential effect on the apparent binding affinity of dopamine. Thus, in humans, loss-of-function SLC6A3 mutations that impair DAT-mediated dopamine transport activity are associated with an early-onset complex movement disorder. Identification of the molecular basis of IPD suggests SLC6A3 as a candidate susceptibility gene for other movement disorders associated with parkinsonism and/or dystonic features.

Original language	English
Pages (from-to)	1595-603
Number of pages	9
Journal	Journal of Clinical Investigation
Volume	119
Issue number	6
DOIs	https://doi.org/10.1172/JCI39060
Publication status	Published - 1 Jun 2009

Keywords

frameshift mutation
PANK2
PKAN
consanguineous
eye-of-the-tiger
pantothenate kinaseassociated neurodegeneration
neurodegeneration with brain iron accumulation

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10.1172/JCI39060

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Kurian, M., Zhen, J., Cheng, SY., Li, Y., Mordekar, SR., Jardine, P., Morgan, N., Meyer, E., Tee, L., Pasha, S., Wassmer, E., Heales, SJ., Gissen, P., Reith, ME., & Maher, E. (2009). Homozygous loss-of-function mutations in the gene encoding the dopamine transporter are associated with infantile parkinsonism-dystonia. Journal of Clinical Investigation, 119(6), 1595-603. https://doi.org/10.1172/JCI39060

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title = "Homozygous loss-of-function mutations in the gene encoding the dopamine transporter are associated with infantile parkinsonism-dystonia.",

abstract = "Genetic variants of the SLC6A3 gene that encodes the human dopamine transporter (DAT) have been linked to a variety of neuropsychiatric disorders, particularly attention deficit hyperactivity disorder. In addition, the homozygous Slc6a3 knockout mouse displays a hyperactivity phenotype. Here, we analyzed 2 unrelated consanguineous families with infantile parkinsonism-dystonia (IPD) syndrome and identified homozygous missense SLC6A3 mutations (p.L368Q and p.P395L) in both families. Functional studies demonstrated that both mutations were loss-of-function mutations that severely reduced levels of mature (85-kDa) DAT while having a differential effect on the apparent binding affinity of dopamine. Thus, in humans, loss-of-function SLC6A3 mutations that impair DAT-mediated dopamine transport activity are associated with an early-onset complex movement disorder. Identification of the molecular basis of IPD suggests SLC6A3 as a candidate susceptibility gene for other movement disorders associated with parkinsonism and/or dystonic features.",

keywords = "frameshift mutation, PANK2, PKAN, consanguineous, eye-of-the-tiger, pantothenate kinaseassociated neurodegeneration, neurodegeneration with brain iron accumulation",

author = "Manju Kurian and J Zhen and SY Cheng and Y Li and SR Mordekar and P Jardine and Neil Morgan and Esther Meyer and Louise Tee and Shanaz Pasha and E Wassmer and SJ Heales and Paul Gissen and ME Reith and Eamonn Maher",

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doi = "10.1172/JCI39060",

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Kurian, M, Zhen, J, Cheng, SY, Li, Y, Mordekar, SR, Jardine, P, Morgan, N, Meyer, E, Tee, L, Pasha, S, Wassmer, E, Heales, SJ, Gissen, P, Reith, ME & Maher, E 2009, 'Homozygous loss-of-function mutations in the gene encoding the dopamine transporter are associated with infantile parkinsonism-dystonia.', Journal of Clinical Investigation, vol. 119, no. 6, pp. 1595-603. https://doi.org/10.1172/JCI39060

TY - JOUR

T1 - Homozygous loss-of-function mutations in the gene encoding the dopamine transporter are associated with infantile parkinsonism-dystonia.

AU - Kurian, Manju

AU - Zhen, J

AU - Cheng, SY

AU - Li, Y

AU - Mordekar, SR

AU - Jardine, P

AU - Morgan, Neil

AU - Meyer, Esther

AU - Tee, Louise

AU - Pasha, Shanaz

AU - Wassmer, E

AU - Heales, SJ

AU - Gissen, Paul

AU - Reith, ME

AU - Maher, Eamonn

PY - 2009/6/1

Y1 - 2009/6/1

N2 - Genetic variants of the SLC6A3 gene that encodes the human dopamine transporter (DAT) have been linked to a variety of neuropsychiatric disorders, particularly attention deficit hyperactivity disorder. In addition, the homozygous Slc6a3 knockout mouse displays a hyperactivity phenotype. Here, we analyzed 2 unrelated consanguineous families with infantile parkinsonism-dystonia (IPD) syndrome and identified homozygous missense SLC6A3 mutations (p.L368Q and p.P395L) in both families. Functional studies demonstrated that both mutations were loss-of-function mutations that severely reduced levels of mature (85-kDa) DAT while having a differential effect on the apparent binding affinity of dopamine. Thus, in humans, loss-of-function SLC6A3 mutations that impair DAT-mediated dopamine transport activity are associated with an early-onset complex movement disorder. Identification of the molecular basis of IPD suggests SLC6A3 as a candidate susceptibility gene for other movement disorders associated with parkinsonism and/or dystonic features.

AB - Genetic variants of the SLC6A3 gene that encodes the human dopamine transporter (DAT) have been linked to a variety of neuropsychiatric disorders, particularly attention deficit hyperactivity disorder. In addition, the homozygous Slc6a3 knockout mouse displays a hyperactivity phenotype. Here, we analyzed 2 unrelated consanguineous families with infantile parkinsonism-dystonia (IPD) syndrome and identified homozygous missense SLC6A3 mutations (p.L368Q and p.P395L) in both families. Functional studies demonstrated that both mutations were loss-of-function mutations that severely reduced levels of mature (85-kDa) DAT while having a differential effect on the apparent binding affinity of dopamine. Thus, in humans, loss-of-function SLC6A3 mutations that impair DAT-mediated dopamine transport activity are associated with an early-onset complex movement disorder. Identification of the molecular basis of IPD suggests SLC6A3 as a candidate susceptibility gene for other movement disorders associated with parkinsonism and/or dystonic features.

KW - frameshift mutation

KW - PANK2

KW - PKAN

KW - consanguineous

KW - eye-of-the-tiger

KW - pantothenate kinaseassociated neurodegeneration

KW - neurodegeneration with brain iron accumulation

U2 - 10.1172/JCI39060

DO - 10.1172/JCI39060

M3 - Article

C2 - 19478460

SN - 1558-8238

VL - 119

SP - 1595

EP - 1603

JO - Journal of Clinical Investigation

JF - Journal of Clinical Investigation

IS - 6

ER -

Homozygous loss-of-function mutations in the gene encoding the dopamine transporter are associated with infantile parkinsonism-dystonia.

Abstract

Keywords

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