Characterisation of an inflammation-related epigenetic score and its association with cognitive ability

表观遗传学 DNA甲基化 C反应蛋白 生物标志物 医学 队列 表观基因组 内科学 全身炎症 炎症 认知 肿瘤科 生物信息学 认知功能衰退 痴呆 免疫学 生物 遗传学 基因 疾病 精神科 基因表达
作者
Anna Stevenson,Daniel L McCartney,Robert F. Hillary,Archie Campbell,Stewart W. Morris,Mairead Lesley Bermingham,Rosie M. Walker,Kathryn Evans,Thibaud Boutin,Caroline Hayward,Allan F. McRae,Barry W. McColl,Tara L. Spires‐Jones,Andrew M. McIntosh,Ian J. Deary,Riccardo E. Marioni
出处
期刊:Clinical Epigenetics [BioMed Central]
卷期号:12 (1) 被引量:36
标识
DOI:10.1186/s13148-020-00903-8
摘要

Abstract Background Chronic systemic inflammation has been associated with incident dementia, but its association with age-related cognitive decline is less clear. The acute responses of many inflammatory biomarkers mean they may provide an unreliable picture of the chronicity of inflammation. Recently, a large-scale epigenome-wide association study identified DNA methylation correlates of C-reactive protein (CRP)—a widely used acute-phase inflammatory biomarker. DNA methylation is thought to be relatively stable in the short term, marking it as a potentially useful signature of exposure. Methods We utilise a DNA methylation-based score for CRP and investigate its trajectories with age, and associations with cognitive ability in comparison with serum CRP and a genetic CRP score in a longitudinal study of older adults ( n = 889) and a large, cross-sectional cohort ( n = 7028). Results We identified no homogeneous trajectories of serum CRP with age across the cohorts, whereas the epigenetic CRP score was consistently found to increase with age (standardised β = 0.07 and 0.01) and to do so more rapidly in males compared to females. Additionally, the epigenetic CRP score had higher test-retest reliability compared to serum CRP, indicating its enhanced temporal stability. Higher serum CRP was not found to be associated with poorer cognitive ability (standardised β = − 0.08 and − 0.05); however, a consistent negative association was identified between cognitive ability and the epigenetic CRP score in both cohorts (standardised β = − 0.15 and − 0.08). Conclusions An epigenetic proxy of CRP may provide a more reliable signature of chronic inflammation, allowing for more accurate stratification of individuals, and thus clearer inference of associations with incident health outcomes.
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