A multi-incident, Old-Order Amish family with PD

Authors

B A. Racette, Department of Neurology and Neurological, Washington University School of Medicine, St. Louis, MO 63110, USA. racetteb@neuro.wustl.edu
M Rundle
J C. Wang
A Goate
N L. Saccone
M Farrer
S Lincoln
J Hussey
S Smemo
J Lin
B Suarez
A Parsian
J S. Perlmutter

Document Type

Article

Abstract

BACKGROUND: PD is largely a sporadic condition of unknown etiology, but specific inherited mutations are a cause of PD. OBJECTIVE: To describe a large, multi-incident Amish pedigree with PD. METHODS: Case ascertainment, calculation of population prevalence, and calculation of kinship coefficients (a measure of relatedness between two individuals) for affecteds and subjects in a large kindred with PD were conducted. Sequencing of genes with known mutations sufficient to cause PD and marker-by-marker haplotype analysis in chromosomal regions flanking previously described genes with known mutations were performed. RESULTS: The authors have examined 113 members of this pedigree and classified 67 as normal (no evidence of PD), 17 as clinically definite PD, 6 as clinically probable PD, and 23 as clinically possible PD. The mean age at onset of the clinically definite subjects was 56.7 years. The phenotype in this family is typical of idiopathic PD, including rest tremor, rigidity, bradykinesia, postural instability, and response to levodopa. In addition, dementia occurred in six of the clinically definite subjects, and many subjects experienced levodopa-related motor complications including wearing off and dopa-induced dyskinesias. In the index Amish community, a minimum prevalence of PD in the population 40 years and older of 552/100,000 was calculated. The mean kinship coefficient in the subjects with PD and those with PD by history (0.036) was higher (p = 0.007) than in a group of age-matched normal Amish control subjects (0.016), providing evidence that PD is inherited in this family. Sequence analysis did not detect any mutations in known PD genes. No single haplotype cosegregates with the disease in any of the chromosomal regions previously found to be linked to PD, and no marker in these regions exhibits increased homozygosity among definite PD cases. CONCLUSIONS: PD in this community is more common than in the general population, and this increased prevalence may be due in part to a novel gene(s).

Medical Subject Headings

Adult; Aged; Aged, 80 and over; Chi-Square Distribution; Ethnicity (genetics); Female; Genetic Linkage (genetics); Humans; Incidence; Male; Middle Aged; Parkinson Disease (epidemiology, genetics); Pedigree; Prevalence; Religion

Publication Date

2-26-2002

Publication Title

Neurology

ISSN

0028-3878

Volume

58

Issue

4

First Page

568

Last Page

74

PubMed ID

11865134

Digital Object Identifier (DOI)

10.1212/wnl.58.4.568

Recommended Citation

Racette, B A.; Rundle, M; Wang, J C.; Goate, A; Saccone, N L.; Farrer, M; Lincoln, S; Hussey, J; Smemo, S; Lin, J; Suarez, B; Parsian, A; and Perlmutter, J S., "A multi-incident, Old-Order Amish family with PD" (2002). Neurology. 1094.
https://scholar.barrowneuro.org/neurology/1094