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
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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