CRP相关CpG位点的DNA甲基化可能介导教育成就与认知之间的途径

Meike Stoldt, Farah Ammous, Lisha Lin, Scott M Ratliff, Erin B Ware, Jessica D Faul, Wei Zhao, Sharon L R Kardia, Jennifer A Smith
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引用次数: 0

摘要

越来越多的证据表明,炎症过程与认知能力下降和痴呆症有关。这项研究探讨了 C 反应蛋白(CRP)这一常见的临床炎症生物标志物的表观遗传标志物是否可能介导教育程度与认知能力之间的关系。我们首先在健康与退休研究(HRS,平均年龄=69.7 岁)的 3298 名参与者中评估了 53 个先前报告的与 CRP 相关的 DNA 甲基化位点(CpGs)是否与 CRP 相关,包括单独评估和汇总成一个甲基化风险评分(MRSCRP)。在对年龄、性别、吸烟、体重指数、遗传血统和白细胞计数进行调整后,49 个 CpGs(92%)与 HRS 中 CRP 的自然对数相关(p
本文章由计算机程序翻译,如有差异,请以英文原文为准。
DNA Methylation at C-Reactive Protein-Associated CpG Sites May Mediate the Pathway Between Educational Attainment and Cognition.

Growing evidence has linked inflammatory processes to cognitive decline and dementia. This work examines whether an epigenetic marker of C-reactive protein (CRP), a common clinical inflammatory biomarker, may mediate the relationship between educational attainment and cognition. We first evaluated whether 53 previously reported CRP-associated DNA methylation sites (CpGs) are associated with CRP, both individually and aggregated into a methylation risk score (MRSCRP), in 3 298 participants from the Health and Retirement Study (HRS, mean age = 69.7 years). Forty-nine CpGs (92%) were associated with the natural logarithm of CRP in HRS after adjusting for age, sex, smoking, BMI, genetic ancestry, and white blood cell counts (p < .05), and each standard deviation increase in MRSCRP was associated with a 0.38 unit increase in lnCRP (p = 4.02E-99). In cross-sectional analysis, for each standard deviation increase in MRSCRP, total memory score and total cognitive score decreased, on average, by 0.28 words and 0.43 items, respectively (p < .001). Further, MRSCRP mediated 6.9% of the relationship between high school education and total memory score in a model adjusting for age, sex, and genetic ancestry (p < .05); this was attenuated to 2.4% with additional adjustment for marital status, APOE ε4 status, health behaviors, and comorbidities (p < .05). Thus, CRP-associated methylation may partially mediate the relationship between education and cognition at older ages. Further research is warranted to determine whether DNA methylation at these sites may improve current prediction models for cognitive impairment in older adults.

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