Genome-Wide Association of Familial Late-Onset Alzheimer's Disease Replicates BIN1 and CLU and Nominates CUGBP2 in Interaction with APOE

Late-onset Alzheimer's disease (LOAD) is the most common form of dementia in the elderly. The National Institute of Aging-Late Onset Alzheimer's Disease Family Study and the National Cell Repository for Alzheimer's Disease conducted a joint genome-wide association study (GWAS) of mult...

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Autores principales: Wijsman, Ellen M., Pankratz, Nathan D., Choi, Yoonha, Rothstein, Joseph H., Faber, Kelley M., Cheng, Rong, Lee, Joseph H., Bird, Thomas D., Bennett, David A., Diaz-Arrastia, Ramon, Goate, Alison M., Farlow, Martin, Ghetti, Bernardino, Sweet, Robert A., Foroud, Tatiana M., Mayeux, Richard
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3040659/
https://www.ncbi.nlm.nih.gov/pubmed/21379329
http://dx.doi.org/10.1371/journal.pgen.1001308
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author Wijsman, Ellen M.
Pankratz, Nathan D.
Choi, Yoonha
Rothstein, Joseph H.
Faber, Kelley M.
Cheng, Rong
Lee, Joseph H.
Bird, Thomas D.
Bennett, David A.
Diaz-Arrastia, Ramon
Goate, Alison M.
Farlow, Martin
Ghetti, Bernardino
Sweet, Robert A.
Foroud, Tatiana M.
Mayeux, Richard
author_facet Wijsman, Ellen M.
Pankratz, Nathan D.
Choi, Yoonha
Rothstein, Joseph H.
Faber, Kelley M.
Cheng, Rong
Lee, Joseph H.
Bird, Thomas D.
Bennett, David A.
Diaz-Arrastia, Ramon
Goate, Alison M.
Farlow, Martin
Ghetti, Bernardino
Sweet, Robert A.
Foroud, Tatiana M.
Mayeux, Richard
author_sort Wijsman, Ellen M.
collection PubMed
description Late-onset Alzheimer's disease (LOAD) is the most common form of dementia in the elderly. The National Institute of Aging-Late Onset Alzheimer's Disease Family Study and the National Cell Repository for Alzheimer's Disease conducted a joint genome-wide association study (GWAS) of multiplex LOAD families (3,839 affected and unaffected individuals from 992 families plus additional unrelated neurologically evaluated normal subjects) using the 610 IlluminaQuad panel. This cohort represents the largest family-based GWAS of LOAD to date, with analyses limited here to the European-American subjects. SNPs near APOE gave highly significant results (e.g., rs2075650, p = 3.2×10(−81)), but no other genome-wide significant evidence for association was obtained in the full sample. Analyses that stratified on APOE genotypes identified SNPs on chromosome 10p14 in CUGBP2 with genome-wide significant evidence for association within APOE ε4 homozygotes (e.g., rs201119, p = 1.5×10(−8)). Association in this gene was replicated in an independent sample consisting of three cohorts. There was evidence of association for recently-reported LOAD risk loci, including BIN1 (rs7561528, p = 0.009 with, and p = 0.03 without, APOE adjustment) and CLU (rs11136000, p = 0.023 with, and p = 0.008 without, APOE adjustment), with weaker support for CR1. However, our results provide strong evidence that association with PICALM (rs3851179, p = 0.69 with, and p = 0.039 without, APOE adjustment) and EXOC3L2 is affected by correlation with APOE, and thus may represent spurious association. Our results indicate that genetic structure coupled with ascertainment bias resulting from the strong APOE association affect genome-wide results and interpretation of some recently reported associations. We show that a locus such as APOE, with large effects and strong association with disease, can lead to samples that require appropriate adjustment for this locus to avoid both false positive and false negative evidence of association. We suggest that similar adjustments may also be needed for many other large multi-site studies.
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spelling pubmed-30406592011-03-04 Genome-Wide Association of Familial Late-Onset Alzheimer's Disease Replicates BIN1 and CLU and Nominates CUGBP2 in Interaction with APOE Wijsman, Ellen M. Pankratz, Nathan D. Choi, Yoonha Rothstein, Joseph H. Faber, Kelley M. Cheng, Rong Lee, Joseph H. Bird, Thomas D. Bennett, David A. Diaz-Arrastia, Ramon Goate, Alison M. Farlow, Martin Ghetti, Bernardino Sweet, Robert A. Foroud, Tatiana M. Mayeux, Richard PLoS Genet Research Article Late-onset Alzheimer's disease (LOAD) is the most common form of dementia in the elderly. The National Institute of Aging-Late Onset Alzheimer's Disease Family Study and the National Cell Repository for Alzheimer's Disease conducted a joint genome-wide association study (GWAS) of multiplex LOAD families (3,839 affected and unaffected individuals from 992 families plus additional unrelated neurologically evaluated normal subjects) using the 610 IlluminaQuad panel. This cohort represents the largest family-based GWAS of LOAD to date, with analyses limited here to the European-American subjects. SNPs near APOE gave highly significant results (e.g., rs2075650, p = 3.2×10(−81)), but no other genome-wide significant evidence for association was obtained in the full sample. Analyses that stratified on APOE genotypes identified SNPs on chromosome 10p14 in CUGBP2 with genome-wide significant evidence for association within APOE ε4 homozygotes (e.g., rs201119, p = 1.5×10(−8)). Association in this gene was replicated in an independent sample consisting of three cohorts. There was evidence of association for recently-reported LOAD risk loci, including BIN1 (rs7561528, p = 0.009 with, and p = 0.03 without, APOE adjustment) and CLU (rs11136000, p = 0.023 with, and p = 0.008 without, APOE adjustment), with weaker support for CR1. However, our results provide strong evidence that association with PICALM (rs3851179, p = 0.69 with, and p = 0.039 without, APOE adjustment) and EXOC3L2 is affected by correlation with APOE, and thus may represent spurious association. Our results indicate that genetic structure coupled with ascertainment bias resulting from the strong APOE association affect genome-wide results and interpretation of some recently reported associations. We show that a locus such as APOE, with large effects and strong association with disease, can lead to samples that require appropriate adjustment for this locus to avoid both false positive and false negative evidence of association. We suggest that similar adjustments may also be needed for many other large multi-site studies. Public Library of Science 2011-02-17 /pmc/articles/PMC3040659/ /pubmed/21379329 http://dx.doi.org/10.1371/journal.pgen.1001308 Text en Wijsman et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Wijsman, Ellen M.
Pankratz, Nathan D.
Choi, Yoonha
Rothstein, Joseph H.
Faber, Kelley M.
Cheng, Rong
Lee, Joseph H.
Bird, Thomas D.
Bennett, David A.
Diaz-Arrastia, Ramon
Goate, Alison M.
Farlow, Martin
Ghetti, Bernardino
Sweet, Robert A.
Foroud, Tatiana M.
Mayeux, Richard
Genome-Wide Association of Familial Late-Onset Alzheimer's Disease Replicates BIN1 and CLU and Nominates CUGBP2 in Interaction with APOE
title Genome-Wide Association of Familial Late-Onset Alzheimer's Disease Replicates BIN1 and CLU and Nominates CUGBP2 in Interaction with APOE
title_full Genome-Wide Association of Familial Late-Onset Alzheimer's Disease Replicates BIN1 and CLU and Nominates CUGBP2 in Interaction with APOE
title_fullStr Genome-Wide Association of Familial Late-Onset Alzheimer's Disease Replicates BIN1 and CLU and Nominates CUGBP2 in Interaction with APOE
title_full_unstemmed Genome-Wide Association of Familial Late-Onset Alzheimer's Disease Replicates BIN1 and CLU and Nominates CUGBP2 in Interaction with APOE
title_short Genome-Wide Association of Familial Late-Onset Alzheimer's Disease Replicates BIN1 and CLU and Nominates CUGBP2 in Interaction with APOE
title_sort genome-wide association of familial late-onset alzheimer's disease replicates bin1 and clu and nominates cugbp2 in interaction with apoe
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3040659/
https://www.ncbi.nlm.nih.gov/pubmed/21379329
http://dx.doi.org/10.1371/journal.pgen.1001308
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