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A genome-wide scan in an Amish pedigree with parkinsonism.


ABSTRACT: The identification of familial Parkinson Disease (PD) genes is yielding important molecular pathogenetic insights. In an effort to identify additional PD genes, we studied an eight generation Amish pedigree with apparent autosomal dominant parkinsonism with incomplete penetrance. Phenotypic variability ranged from idiopathic PD to progressive supranuclear palsy (PSP), with the average age at onset 53 years (range of 39 to 74 years). We identified markers on chromosome 3 and 7 that were significant at a genome-wide level by parametric and nonparametric criteria, lod > 3 and non-parametric P-value < 0.10, respectively. We also identified markers on chromosomes 10 and 22 with lod > 3. These data suggest that parkinsonism in this pedigree is genetically complex, with contributions from several loci.

SUBMITTER: Lee SL 

PROVIDER: S-EPMC2764120 | biostudies-literature | 2008 Sep

REPOSITORIES: biostudies-literature

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A genome-wide scan in an Amish pedigree with parkinsonism.

Lee S L SL   Murdock D G DG   McCauley J L JL   Bradford Y Y   Crunk A A   McFarland L L   Jiang L L   Wang T T   Schnetz-Boutaud N N   Haines J L JL  

Annals of human genetics 20080521 Pt 5


The identification of familial Parkinson Disease (PD) genes is yielding important molecular pathogenetic insights. In an effort to identify additional PD genes, we studied an eight generation Amish pedigree with apparent autosomal dominant parkinsonism with incomplete penetrance. Phenotypic variability ranged from idiopathic PD to progressive supranuclear palsy (PSP), with the average age at onset 53 years (range of 39 to 74 years). We identified markers on chromosome 3 and 7 that were significa  ...[more]

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