TY - JOUR
T1 - DNAJC6 Mutations Associated with Early-Onset Parkinson's Disease
AU - Olgiati, Simone
AU - Quadri, Marialuisa
AU - Fang, Mingyan
AU - Rood, Janneke P.M.A.
AU - Saute, Jonas A.
AU - Chien, Hsin Fen
AU - Bouwkamp, Christian G.
AU - Graafland, Josja
AU - Minneboo, Michelle
AU - Breedveld, Guido J.
AU - Zhang, Jianguo
AU - Verheijen, Frans W.
AU - Boon, Agnita J.W.
AU - Kievit, Anneke J.A.
AU - Jardim, Laura Bannach
AU - Mandemakers, Wim
AU - Barbosa, Egberto Reis
AU - Rieder, Carlos R.M.
AU - Leenders, Klaus L.
AU - Wang, Jun
AU - Bonifati, Vincenzo
N1 - Publisher Copyright:
© 2016 American Neurological Association.
PY - 2016/2/1
Y1 - 2016/2/1
N2 - Objective DNAJC6 mutations were recently described in two families with autosomal recessive juvenile parkinsonism (onset age < 11), prominent atypical signs, poor or absent response to levodopa, and rapid progression (wheelchair-bound within ∼10 years from onset). Here, for the first time, we report DNAJC6 mutations in early-onset Parkinson's disease (PD). Methods The DNAJC6 open reading frame was analyzed in 274 patients with early-onset sporadic or familial PD. Selected variants were followed up by cosegregation, homozygosity mapping, linkage analysis, whole-exome sequencing, and protein studies. Results We identified two families with different novel homozygous DNAJC6 mutations segregating with PD. In each family, the DNAJC6 mutation was flanked by long runs of homozygosity within highest linkage peaks. Exome sequencing did not detect additional pathogenic variants within the linkage regions. In both families, patients showed severely decreased steady-state levels of the auxilin protein in fibroblasts. We also identified a sporadic patient carrying two rare noncoding DNAJC6 variants possibly effecting RNA splicing. All these cases fulfilled the criteria for a clinical diagnosis of early-onset PD, had symptoms onset in the third-to-fifth decade, and slow disease progression. Response to dopaminergic therapies was prominent, but, in some patients, limited by psychiatric side effects. The phenotype overlaps that of other monogenic forms of early-onset PD. Interpretation Our findings delineate a novel form of hereditary early-onset PD. Screening of DNAJC6 is warranted in all patients with early-onset PD compatible with autosomal recessive inheritance. Our data provide further evidence for the involvement of synaptic vesicles endocytosis and trafficking in PD pathogenesis.
AB - Objective DNAJC6 mutations were recently described in two families with autosomal recessive juvenile parkinsonism (onset age < 11), prominent atypical signs, poor or absent response to levodopa, and rapid progression (wheelchair-bound within ∼10 years from onset). Here, for the first time, we report DNAJC6 mutations in early-onset Parkinson's disease (PD). Methods The DNAJC6 open reading frame was analyzed in 274 patients with early-onset sporadic or familial PD. Selected variants were followed up by cosegregation, homozygosity mapping, linkage analysis, whole-exome sequencing, and protein studies. Results We identified two families with different novel homozygous DNAJC6 mutations segregating with PD. In each family, the DNAJC6 mutation was flanked by long runs of homozygosity within highest linkage peaks. Exome sequencing did not detect additional pathogenic variants within the linkage regions. In both families, patients showed severely decreased steady-state levels of the auxilin protein in fibroblasts. We also identified a sporadic patient carrying two rare noncoding DNAJC6 variants possibly effecting RNA splicing. All these cases fulfilled the criteria for a clinical diagnosis of early-onset PD, had symptoms onset in the third-to-fifth decade, and slow disease progression. Response to dopaminergic therapies was prominent, but, in some patients, limited by psychiatric side effects. The phenotype overlaps that of other monogenic forms of early-onset PD. Interpretation Our findings delineate a novel form of hereditary early-onset PD. Screening of DNAJC6 is warranted in all patients with early-onset PD compatible with autosomal recessive inheritance. Our data provide further evidence for the involvement of synaptic vesicles endocytosis and trafficking in PD pathogenesis.
UR - http://www.scopus.com/inward/record.url?scp=84958106531&partnerID=8YFLogxK
U2 - 10.1002/ana.24553
DO - 10.1002/ana.24553
M3 - Article
SN - 0364-5134
VL - 79
SP - 244
EP - 256
JO - Annals of Neurology
JF - Annals of Neurology
IS - 2
ER -