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基因启动子甲基化与老年人肺功能有关:正常衰老研究。

Gene promoter methylation is associated with lung function in the elderly: the Normative Aging Study.

机构信息

Exposure, Epidemiology and Risk Program, Department of Environmental Health, Harvard School of Public Health, Boston, MA, USA.

出版信息

Epigenetics. 2012 Mar;7(3):261-9. doi: 10.4161/epi.7.3.19216.

Abstract

Lung function is a strong predictor of mortality. While inflammatory markers have been associated with lung function decrease, pathways are still poorly understood and epigenetic changes may participate in lung function decline mechanisms. We studied the cross-sectional association between DNA methylation in nine inflammatory genes and lung function in a cohort of 756 elderly men living in the metropolitan area of Boston. Participants donated a blood sample for DNA methylation analysis and underwent spirometry at each visit every 3 to 5 y from 1999-2006. We used separate multivariate mixed effects regression models to study the association between each lung function measurement and DNA methylation within each gene. Decreased CRAT, F3 and TLR2 methylation was significantly associated with lower lung function. One interquartile range (IQR) decrease in DNA methylation was associated with lower forced vital capacity (FVC) and forced expiratory volume in one second (FEV 1), respectively by 2.94% (p < 10 (-4)) and 2.47% (p < 10 (-3)) for F3, and by 2.10% (p < 10 (-2)) and 2.42% (p < 10 (-3)) for TLR2. Decreased IFNγ and IL6 methylation was significantly associated with better lung function. One IQR decrease in DNA methylation was associated with higher FEV 1 by 1.75% (p = 0.02) and 1.67% (p = 0.05) for IFNγ and IL6, respectively. These data demonstrate that DNA methylation may be part of the biological processes underlying the lung function decline and that IFNγ and IL6 may have ambivalent roles through activation of negative feedback.

摘要

肺功能是死亡率的一个强有力的预测因子。虽然炎症标志物与肺功能下降有关,但相关通路仍不清楚,表观遗传变化可能参与肺功能下降机制。我们研究了居住在波士顿大都市区的 756 名老年男性队列中,9 个炎症基因的 DNA 甲基化与肺功能之间的横断面关联。参与者在 1999 年至 2006 年期间每 3 至 5 年进行一次随访,每次都捐献血液样本进行 DNA 甲基化分析和肺功能检查。我们使用单独的多变量混合效应回归模型来研究每个基因中每个肺功能测量值与 DNA 甲基化之间的关联。CRAT、F3 和 TLR2 甲基化减少与肺功能降低显著相关。DNA 甲基化每降低一个四分位距(IQR),分别与用力肺活量(FVC)和 1 秒用力呼气量(FEV1)降低 2.94%(p<10(-4))和 2.47%(p<10(-3))有关,F3 降低 2.10%(p<10(-2))和 TLR2 降低 2.42%(p<10(-3))。IFNγ和 IL6 甲基化减少与肺功能改善显著相关。DNA 甲基化每降低一个 IQR,FEV1 分别增加 1.75%(p=0.02)和 1.67%(p=0.05),IFNγ 和 IL6 分别增加。这些数据表明,DNA 甲基化可能是肺功能下降的生物学过程的一部分,IFNγ 和 IL6 可能通过激活负反馈而具有矛盾的作用。

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