TY - JOUR
T1 - FUS Mutations in Familial Amyotrophic Lateral Sclerosis in the Netherlands
AU - Groen, Ewout J. N.
AU - van Es, Michael A.
AU - van Vught, Paul W. J.
AU - Spliet, Wim G. M.
AU - van Engelen-Lee, Jooyeon
AU - de Visser, Marianne
AU - Wokke, John H. J.
AU - Schelhaas, Helenius J.
AU - Ophoff, Roel A.
AU - Fumoto, Katsumi
AU - Pasterkamp, R. Jeroen
AU - Dooijes, Dennis
AU - Cuppen, Edwin
AU - Veldink, Jan H.
AU - van den Berg, Leonard H.
PY - 2010
Y1 - 2010
N2 - Objectives: To assess the frequency of FUS mutations in 52 probands with familial amyotrophic lateral sclerosis (FALS) and to provide careful documentation of clinical characteristics. Design: FUS mutation analysis was performed using capillary sequencing on all coding regions of the gene in a cohort of patients with FALS. The clinical characteristics of patients carrying FUS mutations were described in detail. Setting: Three university hospitals in the Netherlands (referral centers for neuromuscular diseases). Patients: Fifty-two probands from unrelated pedigrees with FALS. Main Outcome Measure: FUS mutations. Results: We identified 3 mutations in 4 of 52 probands. We observed 2 previously identified mutations (p.Arg521Cys and p.Arg521His) and 1 novel mutation (p.Ser462Phe). In addition, a p.Gln210His polymorphism was identified in 1 proband and 3 healthy control subjects. Phenotypic analysis demonstrated that patients may lack upper motor neuron signs, which was confirmed at autopsy, and disease survival was short ( <36 months for 8 of 10 patients). Conclusions: We discovered FUS mutations in Dutch patients with FALS and the occurrence of benign variations in the gene. Therefore, caution is warranted when interpreting results in a clinical setting. Although the phenotype associated with FUS mutations is variable, most patients predominantly demonstrate loss of lower motor neurons and have short disease survival
AB - Objectives: To assess the frequency of FUS mutations in 52 probands with familial amyotrophic lateral sclerosis (FALS) and to provide careful documentation of clinical characteristics. Design: FUS mutation analysis was performed using capillary sequencing on all coding regions of the gene in a cohort of patients with FALS. The clinical characteristics of patients carrying FUS mutations were described in detail. Setting: Three university hospitals in the Netherlands (referral centers for neuromuscular diseases). Patients: Fifty-two probands from unrelated pedigrees with FALS. Main Outcome Measure: FUS mutations. Results: We identified 3 mutations in 4 of 52 probands. We observed 2 previously identified mutations (p.Arg521Cys and p.Arg521His) and 1 novel mutation (p.Ser462Phe). In addition, a p.Gln210His polymorphism was identified in 1 proband and 3 healthy control subjects. Phenotypic analysis demonstrated that patients may lack upper motor neuron signs, which was confirmed at autopsy, and disease survival was short ( <36 months for 8 of 10 patients). Conclusions: We discovered FUS mutations in Dutch patients with FALS and the occurrence of benign variations in the gene. Therefore, caution is warranted when interpreting results in a clinical setting. Although the phenotype associated with FUS mutations is variable, most patients predominantly demonstrate loss of lower motor neurons and have short disease survival
U2 - https://doi.org/10.1001/archneurol.2009.329
DO - https://doi.org/10.1001/archneurol.2009.329
M3 - Article
C2 - 20142531
SN - 0003-9942
VL - 67
SP - 224
EP - 230
JO - Archives of neurology
JF - Archives of neurology
IS - 2
ER -