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Characterization of DCTN1 genetic variability in neurodegeneration.

Authors :: Vilariño-Güell C
Wider C
Soto-Ortolaza AI
Cobb SA
Kachergus JM
Keeling BH
Dachsel JC
Hulihan MM
Dickson DW
Wszolek ZK
Uitti RJ
Graff-Radford NR
Boeve BF
Josephs KA
Miller B
Boylan KB
Gwinn K
Adler CH
Aasly JO
Hentati F
Destée A
Krygowska-Wajs A
Chartier-Harlin MC
Ross OA
Rademakers R
Farrer MJ
Source :: Neurology [Neurology] 2009 Jun 09; Vol. 72 (23), pp. 2024-8.
Publication Year :: 2009
Abstract: Objective: Recently, mutations in DCTN1 were found to cause Perry syndrome, a parkinsonian disorder with TDP-43-positive pathology. Previously, mutations in DCTN1 were identified in a family with lower motor neuron disease, in amyotrophic lateral sclerosis (ALS), and in a family with ALS/frontotemporal dementia (FTD), suggesting a central role for DCTN1 in neurodegeneration.<br />Methods: In this study we sequenced all DCTN1 exons and exon-intron boundaries in 286 samples diagnosed with Parkinson disease (PD), frontotemporal lobar degeneration (FTLD), or ALS.<br />Results: This analysis revealed 36 novel variants (9 missense, 5 silent, and 22 noncoding). Segregation analysis in families and association studies in PD, FTLD, and ALS case-control series did not identify any variants segregating with disease or associated with increased disease risk.<br />Conclusions: This study suggests that pathogenic mutations in DCTN1 are rare and do not play a common role in the development of Parkinson disease, frontotemporal lobar degeneration, or amyotrophic lateral sclerosis.