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A scan of chromosome 10 identifies a novel locus showing strong association with late-onset Alzheimer disease

Lookup NU author(s): Dr Christopher Morris

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Abstract

Strong evidence of linkage to late-onset Alzheimer disease ( LOAD) has been observed on chromosome 10, which implicates a wide region and at least one disease-susceptibility locus. Although significant associations with several biological candidate genes on chromosome 10 have been reported, these findings have not been consistently replicated, and they remain controversial. We performed a chromosome 10-specific association study with 1,412 genebased single-nucleotide polymorphisms ( SNPs), to identify susceptibility genes for developing LOAD. The scan included SNPs in 677 of 1,270 known or predicted genes; each gene contained one or more markers, about half (48%) of which represented putative functional mutations. In general, the initial testing was performed in a white case-control sample from the St. Louis area, with 419 LOAD cases and 377 age-matched controls. Markers that showed significant association in the exploratory analysis were followed up in several other white case-control sample sets to confirm the initial association. Of the 1,397 markers tested in the exploratory sample, 69 reached significance (P < .05). Five of these markers replicated at P < .05 in the validation sample sets. One marker, rs498055, located in a gene homologous to RPS3A ( LOC439999), was significantly associated with Alzheimer disease in four of six case-control series, with an allelic P value of .0001 for a meta-analysis of all six samples. One of the case-control samples with significant association to rs498055 was derived from the linkage sample (P = .0165). These results indicate that variants in the RPS3A homologue are associated with LOAD and implicate this gene, adjacent genes, or other functional variants ( e. g., noncoding RNAs) in the pathogenesis of this disorder.


Publication metadata

Author(s): Grupe A, Li YH, Rowland C, Nowotny P, Hinrichs AL, Smemo S, Kauwe JSK, Maxwell TJ, Cherny S, Doil L, Tacey K, van Luchene R, Myers A, Vrieze FW, Kaleem M, Hollingworth P, Jehu L, Foy C, Archer N, Hamilton G, Holmans P, Morris CM, Catanese J, Sninsky J, White TJ, Powell J, Hardy J, O'Donovan M, Lovestone S, Jones L, Morris JC, Thal L, Owen M, Williams J, Goate A

Publication type: Article

Publication status: Published

Journal: American Journal of Human Genetics

Year: 2006

Volume: 78

Issue: 1

Pages: 78-88

ISSN (print): 0002-9297

ISSN (electronic): 1537-6605

Publisher: Cell Press

URL: http://dx.doi.org/10.1086/498851

DOI: 10.1086/498851


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Funding

Funder referenceFunder name
Intramural NIH HHS
AG05128NIA NIH HHS
AG 05146NIA NIH HHS
G0300429Medical Research Council
GM065509NIGMS NIH HHS
G0701075Medical Research Council
G9810900Medical Research Council
P01 AG003991NIA NIH HHS
P01 AG03991NIA NIH HHS
P50 AG005146NIA NIH HHS
P50 AG005681NIA NIH HHS
P50 AG05681NIA NIH HHS
P50 AG16570NIA NIH HHS
P50 GM065509NIGMS NIH HHS
P50 MH060451NIMH NIH HHS
MH60451NIMH NIH HHS
NS39764NINDS NIH HHS
P50 AG005128NIA NIH HHS
P50 AG005131NIA NIH HHS
P50 AG008671NIA NIH HHS
P50 AG016570NIA NIH HHS
P50 AG05131NIA NIH HHS
P50 NS039764NINDS NIH HHS
P50-AG08671NIA NIH HHS
T32 HG000045NHGRI NIH HHS
R01 AG016208NIA NIH HHS
R01 AG16208NIA NIH HHS
U01 MH046281NIMH NIH HHS
U01 MH046373NIMH NIH HHS
U24 AG021886NIA NIH HHS
U01 MH046290NIMH NIH HHS

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