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February 28, 2012; 78 (9) Articles

Variant ataxia-telangiectasia presenting as primary-appearing dystonia in Canadian Mennonites

R. Saunders-Pullman, D. Raymond, A.J. Stoessl, D. Hobson, T. Nakamura, S. Pullman, D. Lefton, M.S. Okun, R. Uitti, R. Sachdev, K. Stanley, M. San Luciano, J. Hagenah, R. Gatti, L.J. Ozelius, S.B. Bressman
First published February 15, 2012, DOI: https://doi.org/10.1212/WNL.0b013e3182494d51
R. Saunders-Pullman
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D. Raymond
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A.J. Stoessl
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D. Hobson
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T. Nakamura
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S. Pullman
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D. Lefton
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M.S. Okun
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R. Uitti
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R. Sachdev
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K. Stanley
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M. San Luciano
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J. Hagenah
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R. Gatti
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L.J. Ozelius
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S.B. Bressman
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Citation
Variant ataxia-telangiectasia presenting as primary-appearing dystonia in Canadian Mennonites
R. Saunders-Pullman, D. Raymond, A.J. Stoessl, D. Hobson, T. Nakamura, S. Pullman, D. Lefton, M.S. Okun, R. Uitti, R. Sachdev, K. Stanley, M. San Luciano, J. Hagenah, R. Gatti, L.J. Ozelius, S.B. Bressman
Neurology Feb 2012, 78 (9) 649-657; DOI: 10.1212/WNL.0b013e3182494d51

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This article has a correction. Please see:

  • Variant ataxia-telangiectasia presenting as primary-appearing dystonia in Canadian Mennonites - March 27, 2012
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Abstract

Objective: To compare the phenotype of primary-appearing dystonia due to variant ataxia-telangiectasia (A-T) with that of other dystonia ascertained for genetics research.

Methods: Movement disorder specialists examined 20 Canadian Mennonite adult probands with primary-appearing dystonia, as well as relatives in 4 families with parent-child transmission of dystonia. We screened for the exon 43 c.6200 C>A (p. A2067D) ATM mutation and mutations in DYT1 and DYT6. Clinical features of the individuals with dystonia who were harboring ATM mutations were compared with those of individuals without mutations.

Result: Genetic analysis revealed a homozygous founder mutation in ATM in 13 members from 3 of the families, and no one harbored DYT6 or DYT1 mutations. Dystonia in ATM families mimicked other forms of early-onset primary torsion dystonia, especially DYT6, with prominent cervical, cranial, and brachial involvement. Mean age at onset was markedly younger in the patients with variant A-T (n = 12) than in patients with other dystonia (n = 23), (12 years vs 40 years, p < 0.05). The patients with A-T were remarkable for the absence of notable cerebellar atrophy on MRI, lack of frank ataxia on examination, and absence of ocular telangiectasias at original presentation, as well as the presence of prominent myoclonus-dystonia in 2 patients. Many also developed malignancies.

Conclusion: Ataxia and telangiectasias may not be prominent features of patients with variant A-T treated for dystonia in adulthood, and variant A-T may mimic primary torsion dystonia and myoclonus-dystonia.

GLOSSARY

AFP=
α-fetoprotein;
A-T=
ataxia-telangiectasia;
PD=
Parkinson disease

Footnotes

  • Study funding: Supported by NIH (NS26636 to S.B.B., K23NS047256 to R.S.-P.), the Bachmann-Strauss Dystonia & Parkinson Foundation, and the Parkinson's Disease Foundation (to S.P.).

  • Supplemental data at www.neurology.org

  • Received April 4, 2011.
  • Accepted October 26, 2011.
  • Copyright © 2012 by AAN Enterprises, Inc.
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