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Epigenetic signatures of smoking associate with cognitive function brain structure and mental and physical health outcomes in the Lothian Birth Cohort 1936

机译:吸烟的表观遗传学特征与认知功能脑部结构以及心理健康状况有关(Lothian Birth Cohort 1936)

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摘要

Recent advances in genome-wide DNA methylation (DNAm) profiling for smoking behaviour have given rise to a new, molecular biomarker of smoking exposure. It is unclear whether a smoking-associated DNAm (epigenetic) score has predictive value for ageing-related health outcomes which is independent of contributions from self-reported (phenotypic) smoking measures. Blood DNA methylation levels were measured in 895 adults aged 70 years in the Lothian Birth Cohort 1936 (LBC1936) study using the Illumina 450K assay. A DNA methylation score based on 230 CpGs was used as a proxy for smoking exposure. Associations between smoking variables and health outcomes at age 70 were modelled using general linear modelling (ANCOVA) and logistic regression. Additional analyses of smoking with brain MRI measures at age 73 (n = 532) were performed. Smoking-DNAm scores were positively associated with self-reported smoking status (P < 0.001, eta-squared ɳ2 = 0.63) and smoking pack years (r = 0.69, P < 0.001). Higher smoking DNAm scores were associated with variables related to poorer cognitive function, structural brain integrity, physical health, and psychosocial health. Compared with phenotypic smoking, the methylation marker provided stronger associations with all of the cognitive function scores, especially visuospatial ability (P < 0.001, partial eta-squared ɳp2 = 0.022) and processing speed (P < 0.001, ɳp2 = 0.030); inflammatory markers (all P < 0.001, ranges from ɳp2 = 0.021 to 0.030); dietary patterns (healthy diet (P < 0.001, ɳp2 = 0.052) and traditional diet (P < 0.001, ɳp2 = 0.032); stroke (P = 0.006, OR 1.48, 95% CI 1.12, 1.96); mortality (P < 0.001, OR 1.59, 95% CI 1.42, 1.79), and at age 73; with MRI volumetric measures (all P < 0.001, ranges from ɳp2 = 0.030 to 0.052). Additionally, education was the most important life-course predictor of lifetime smoking tested. Our results suggest that a smoking-associated methylation biomarker typically explains a greater proportion of the variance in some smoking-related morbidities in older adults, than phenotypic measures of smoking exposure, with some of the accounted-for variance being independent of phenotypic smoking status.
机译:吸烟行为的全基因组DNA甲基化(DNAm)谱分析的最新进展已引起吸烟暴露的新的分子生物学标记。尚不清楚吸烟相关的DNAm(表观遗传学)评分是否具有与衰老相关的健康结果的预测价值,而该结果与自我报告(表型)吸烟措施的贡献无关。在Lothian Birth Cohort 1936(LBC1936)研究中,使用Illumina 450K测定法测量了895名70岁的成年人的血液DNA甲基化水平。基于230 CpGs的DNA甲基化评分被用作吸烟暴露的代表。使用一般线性模型(ANCOVA)和Logistic回归对70岁时吸烟变量与健康结果之间的关联进行建模。对年龄73岁(n = 532)的脑部MRI吸烟进行了进一步分析。吸烟-DNAm评分与自我报告的吸烟状况(P <0.001,eta-平方ɳ 2 = 0.63)和吸烟年数呈正相关(r = 0.69,P <0.001)。较高的吸烟DNAm分数与与较差的认知功能,大脑的结构完整性,身体健康和社会心理健康有关的变量相关。与表型吸烟相比,甲基化标志物与所有认知功能评分,尤其是视觉空间能力(P <0.001,偏方平方ɳp 2 = 0.022)和处理速度(P <0.001)之间的关联更强。 ,ɳp 2 = 0.030);炎性标志物(所有P <0.001,范围从ɳp 2 = 0.021到0.030);饮食模式(健康饮食(P <0.001,ɳp 2 = 0.052)和传统饮食(P <0.001,ɳp 2 = 0.032);中风( P < / em> = 0.006,或1.48,95%CI 1.12,1.96);死亡率( P <0.001,或1.59,95%CI 1.42,1.79),年龄73岁;采用MRI体积测量(所有 P <0.001,范围从ɳ p 2 = 0.030到0.052)。此外,教育是最重要的人生过程预测指标我们的结果表明,吸烟相关的甲基化生物标志物通常可以解释老年人某些与吸烟相关的发病率方差的比例,这比吸烟暴露的表型指标大,而某些考虑到的方差与表型吸烟状态。

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