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

Jeannette Simino; Zhiying Wang; Jan Bressler; Vincent Chouraki; Qiong Yang; Steven G Younkin; Sudha Seshadri; Myriam Fornage; Eric Boerwinkle; Thomas H Mosley Jr

doi:10.1371/journal.pone.0180046

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

PLoS One. 2017 Jul 13;12(7):e0180046. doi: 10.1371/journal.pone.0180046. eCollection 2017.

Authors

Jeannette Simino^{1

2}, Zhiying Wang³, Jan Bressler³, Vincent Chouraki⁴, Qiong Yang^{5

6}, Steven G Younkin⁷, Sudha Seshadri^{6

8}, Myriam Fornage^{3

9}, Eric Boerwinkle^{3

9

10}, Thomas H Mosley Jr^{1

11}

Affiliations

¹ Gertrude C. Ford MIND Center, University of Mississippi Medical Center, Jackson, Mississippi, United States of America.
² Department of Data Science, John D. Bower School of Population Health, University of Mississippi Medical Center, Jackson, Mississippi, United States of America.
³ Human Genetics Center, Department of Epidemiology, Human Genetics & Environmental Sciences, School of Public Health, University of Texas Health Science Center, Houston, Texas, United States of America.
⁴ Lille University, Inserm, CHU Lille, Institut Pasteur de Lille, U1167 - RID-AGE - Risk factors and molecular determinants of aging-related diseases; Lille, France.
⁵ Department of Biostatistics, Boston University School of Public Health, Boston, Massachusetts, United States of America.
⁶ The National Heart, Lung, and Blood Institute's Framingham Heart Study, Framingham, Massachusetts, United States of America.
⁷ Department of Neuroscience, Mayo Clinic College of Medicine, Mayo Clinic Jacksonville, Jacksonville, Florida, United States of America.
⁸ Department of Neurology, Boston University School of Medicine, Boston, Massachusetts, United States of America.
⁹ The Brown Foundation Institute of Molecular Medicine, Research Center for Human Genetics, The University of Texas Health Science Center, Houston, Texas, United States of America.
¹⁰ Human Genome Sequencing Center, Baylor College of Medicine, Houston, Texas, United States of America.
¹¹ Department of Medicine, University of Mississippi Medical Center, Jackson, Massachusetts, United States of America.

Abstract

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 aβ42 concentrations and aβ42:aβ40 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 aβ42 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 aβ42:aβ40 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 aβ42:aβ40 ratio and the fold-change in aβ42, 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.

MeSH terms

Aged
Amyloid beta-Peptides / blood*
Black or African American / genetics*
Exome
Female
Gene Regulatory Networks
Genome-Wide Association Study / methods
Humans
Male
Middle Aged
Polymorphism, Single Nucleotide*
Sequence Analysis, DNA / methods*
United States / ethnology
White People / genetics*

Substances

Amyloid beta-Peptides

Abstract

MeSH terms

Substances

Grants and funding