Whole exome sequence-based association analyses of plasma amyloid-β in African and European Americans; the Atherosclerosis Risk in Communities-Neurocognitive Study

OBJECTIVE: We performed single-variant and gene-based association analyses of plasma amyloid-β (aβ) concentrations using whole exome sequence from 1,414 African and European Americans. Our goal was to identify genes that influence plasma aβ(42) concentrations and aβ(42):aβ(40) ratios in late middle...

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Autores principales: Simino, Jeannette, Wang, Zhiying, Bressler, Jan, Chouraki, Vincent, Yang, Qiong, Younkin, Steven G., Seshadri, Sudha, Fornage, Myriam, Boerwinkle, Eric, Mosley, Thomas H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5509141/
https://www.ncbi.nlm.nih.gov/pubmed/28704393
http://dx.doi.org/10.1371/journal.pone.0180046
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author Simino, Jeannette
Wang, Zhiying
Bressler, Jan
Chouraki, Vincent
Yang, Qiong
Younkin, Steven G.
Seshadri, Sudha
Fornage, Myriam
Boerwinkle, Eric
Mosley, Thomas H.
author_facet Simino, Jeannette
Wang, Zhiying
Bressler, Jan
Chouraki, Vincent
Yang, Qiong
Younkin, Steven G.
Seshadri, Sudha
Fornage, Myriam
Boerwinkle, Eric
Mosley, Thomas H.
author_sort Simino, Jeannette
collection PubMed
description OBJECTIVE: We performed single-variant and gene-based association analyses of plasma amyloid-β (aβ) concentrations using whole exome sequence from 1,414 African and European Americans. Our goal was to identify genes that influence plasma aβ(42) concentrations and aβ(42):aβ(40) ratios in late middle age (mean = 59 years), old age (mean = 77 years), or change over time (mean = 18 years). METHODS: Plasma aβ measures were linearly regressed onto age, gender, APOE ε4 carrier status, and time elapsed between visits (fold-changes only) separately by race. Following inverse normal transformation of the residuals, seqMeta was used to conduct race-specific single-variant and gene-based association tests while adjusting for population structure. Linear regression models were fit on autosomal variants with minor allele frequencies (MAF)≥1%. T5 burden and Sequence Kernel Association (SKAT) gene-based tests assessed functional variants with MAF≤5%. Cross-race fixed effects meta-analyses were Bonferroni-corrected for the number of variants or genes tested. RESULTS: Seven genes were associated with aβ in late middle age or change over time; no associations were identified in old age. Single variants in KLKB1 (rs3733402; p = 4.33x10(-10)) and F12 (rs1801020; p = 3.89x10(-8)) were significantly associated with midlife aβ(42) levels through cross-race meta-analysis; the KLKB1 variant replicated internally using 1,014 additional participants with exome chip. ITPRIP, PLIN2, and TSPAN18 were associated with the midlife aβ(42):aβ(40) ratio via the T5 test; TSPAN18 was significant via the cross-race meta-analysis, whereas ITPRIP and PLIN2 were European American-specific. NCOA1 and NT5C3B were associated with the midlife aβ(42):aβ(40) ratio and the fold-change in aβ(42), respectively, via SKAT in African Americans. No associations replicated externally (N = 725). CONCLUSION: We discovered age-dependent genetic effects, established associations between vascular-related genes (KLKB1, F12, PLIN2) and midlife plasma aβ levels, and identified a plausible Alzheimer’s Disease candidate gene (ITPRIP) influencing cell death. Plasma aβ concentrations may have dynamic biological determinants across the lifespan; plasma aβ study designs or analyses must consider age.
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spelling pubmed-55091412017-08-07 Whole exome sequence-based association analyses of plasma amyloid-β in African and European Americans; the Atherosclerosis Risk in Communities-Neurocognitive Study Simino, Jeannette Wang, Zhiying Bressler, Jan Chouraki, Vincent Yang, Qiong Younkin, Steven G. Seshadri, Sudha Fornage, Myriam Boerwinkle, Eric Mosley, Thomas H. PLoS One Research Article OBJECTIVE: We performed single-variant and gene-based association analyses of plasma amyloid-β (aβ) concentrations using whole exome sequence from 1,414 African and European Americans. Our goal was to identify genes that influence plasma aβ(42) concentrations and aβ(42):aβ(40) ratios in late middle age (mean = 59 years), old age (mean = 77 years), or change over time (mean = 18 years). METHODS: Plasma aβ measures were linearly regressed onto age, gender, APOE ε4 carrier status, and time elapsed between visits (fold-changes only) separately by race. Following inverse normal transformation of the residuals, seqMeta was used to conduct race-specific single-variant and gene-based association tests while adjusting for population structure. Linear regression models were fit on autosomal variants with minor allele frequencies (MAF)≥1%. T5 burden and Sequence Kernel Association (SKAT) gene-based tests assessed functional variants with MAF≤5%. Cross-race fixed effects meta-analyses were Bonferroni-corrected for the number of variants or genes tested. RESULTS: Seven genes were associated with aβ in late middle age or change over time; no associations were identified in old age. Single variants in KLKB1 (rs3733402; p = 4.33x10(-10)) and F12 (rs1801020; p = 3.89x10(-8)) were significantly associated with midlife aβ(42) levels through cross-race meta-analysis; the KLKB1 variant replicated internally using 1,014 additional participants with exome chip. ITPRIP, PLIN2, and TSPAN18 were associated with the midlife aβ(42):aβ(40) ratio via the T5 test; TSPAN18 was significant via the cross-race meta-analysis, whereas ITPRIP and PLIN2 were European American-specific. NCOA1 and NT5C3B were associated with the midlife aβ(42):aβ(40) ratio and the fold-change in aβ(42), respectively, via SKAT in African Americans. No associations replicated externally (N = 725). CONCLUSION: We discovered age-dependent genetic effects, established associations between vascular-related genes (KLKB1, F12, PLIN2) and midlife plasma aβ levels, and identified a plausible Alzheimer’s Disease candidate gene (ITPRIP) influencing cell death. Plasma aβ concentrations may have dynamic biological determinants across the lifespan; plasma aβ study designs or analyses must consider age. Public Library of Science 2017-07-13 /pmc/articles/PMC5509141/ /pubmed/28704393 http://dx.doi.org/10.1371/journal.pone.0180046 Text en © 2017 Simino et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Simino, Jeannette
Wang, Zhiying
Bressler, Jan
Chouraki, Vincent
Yang, Qiong
Younkin, Steven G.
Seshadri, Sudha
Fornage, Myriam
Boerwinkle, Eric
Mosley, Thomas H.
Whole exome sequence-based association analyses of plasma amyloid-β in African and European Americans; the Atherosclerosis Risk in Communities-Neurocognitive Study
title Whole exome sequence-based association analyses of plasma amyloid-β in African and European Americans; the Atherosclerosis Risk in Communities-Neurocognitive Study
title_full Whole exome sequence-based association analyses of plasma amyloid-β in African and European Americans; the Atherosclerosis Risk in Communities-Neurocognitive Study
title_fullStr Whole exome sequence-based association analyses of plasma amyloid-β in African and European Americans; the Atherosclerosis Risk in Communities-Neurocognitive Study
title_full_unstemmed Whole exome sequence-based association analyses of plasma amyloid-β in African and European Americans; the Atherosclerosis Risk in Communities-Neurocognitive Study
title_short Whole exome sequence-based association analyses of plasma amyloid-β in African and European Americans; the Atherosclerosis Risk in Communities-Neurocognitive Study
title_sort whole exome sequence-based association analyses of plasma amyloid-β in african and european americans; the atherosclerosis risk in communities-neurocognitive study
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5509141/
https://www.ncbi.nlm.nih.gov/pubmed/28704393
http://dx.doi.org/10.1371/journal.pone.0180046
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