An EWAS of dementia biomarkers and their associations with age, African ancestry, and PTSD

Mark W. Miller; Erika J. Wolf; Xiang Zhao; Mark W. Logue; Sage E. Hawn

doi:10.1186/s13148-024-01649-3

Clinical Epigenetics (Mar 2024)

An EWAS of dementia biomarkers and their associations with age, African ancestry, and PTSD

Mark W. Miller,
Erika J. Wolf,
Xiang Zhao,
Mark W. Logue,
Sage E. Hawn

Affiliations

Mark W. Miller: National Center for PTSD, VA Boston Healthcare System (116B-2)
Erika J. Wolf: National Center for PTSD, VA Boston Healthcare System (116B-2)
Xiang Zhao: National Center for PTSD, VA Boston Healthcare System (116B-2)
Mark W. Logue: National Center for PTSD, VA Boston Healthcare System (116B-2)
Sage E. Hawn: National Center for PTSD, VA Boston Healthcare System (116B-2)

DOI: https://doi.org/10.1186/s13148-024-01649-3
Journal volume & issue: Vol. 16, no. 1
pp. 1 – 13

Abstract

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Abstract Background Large-scale cohort and epidemiological studies suggest that PTSD confers risk for dementia in later life but the biological mechanisms underlying this association remain unknown. This study examined this question by assessing the influences of PTSD, APOE ε4 genotypes, DNA methylation, and other variables on the age- and dementia-associated biomarkers Aβ40, Aβ42, GFAP, NfL, and pTau-181 measured in plasma. Our primary hypothesis was that PTSD would be associated with elevated levels of these markers. Methods Analyses were based on data from a PTSD-enriched cohort of 849 individuals. We began by performing factor analyses of the biomarkers, the results of which identified a two-factor solution. Drawing from the ATN research framework, we termed the first factor, defined by Aβ40 and Aβ42, “Factor A” and the second factor, defined by GFAP, NfL and pTau-181, “Factor TN.” Next, we performed epigenome-wide association analyses (EWAS) of the two-factor scores. Finally, using structural equation modeling (SEM), we evaluated (a) the influence of PTSD, age, APOE ε4 genotype and other covariates on levels of the ATN factors, and (b) tested the mediating influence of the EWAS-significant DNAm loci on these associations. Results The Factor A EWAS identified one significant locus, cg13053408, in FANCD2OS. The Factor TN analysis identified 3 EWAS-significant associations: cg26033520 near ASCC1, cg23156469 in FAM20B, and cg15356923 in FAM19A4. The SEM showed age to be related to both factors, more so with Factor TN (β = 0.581, p < 0.001) than Factor A (β = 0.330, p < 0.001). Genotype-determined African ancestry was associated with lower Factor A (β = 0.196, p < 0.001). Contrary to our primary hypothesis, we found a modest negative bivariate correlation between PTSD and the TN factor scores (r = − 0.133, p < 0.001) attributable primarily to reduced levels of GFAP (r = − 0.128, p < 0.001). Conclusions This study identified novel epigenetic associations with ATN biomarkers and demonstrated robust age and ancestral associations that will be essential to consider in future efforts to develop the clinical applications of these tests. The association between PTSD and reduced GFAP, which has been reported previously, warrants further investigation.

Published in Clinical Epigenetics

ISSN: 1868-7083 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General): Genetics
Website: https://clinicalepigeneticsjournal.biomedcentral.com/

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