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参与MARK-AGE研究的大量欧洲人群外周血单个核细胞中DNMT1和DNMT3B的年龄依赖性表达。

Age-dependent expression of DNMT1 and DNMT3B in PBMCs from a large European population enrolled in the MARK-AGE study.

作者信息

Ciccarone Fabio, Malavolta Marco, Calabrese Roberta, Guastafierro Tiziana, Bacalini Maria Giulia, Reale Anna, Franceschi Claudio, Capri Miriam, Hervonen Antti, Hurme Mikko, Grubeck-Loebenstein Beatrix, Koller Bernhard, Bernhardt Jürgen, Schӧn Christiane, Slagboom P Eline, Toussaint Olivier, Sikora Ewa, Gonos Efstathios S, Breusing Nicolle, Grune Tilman, Jansen Eugène, Dollé Martijn, Moreno-Villanueva María, Sindlinger Thilo, Bürkle Alexander, Zampieri Michele, Caiafa Paola

机构信息

Faculty of Pharmacy and Medicine, Department of Cellular Biotechnologies and Hematology, Sapienza University of Rome, Rome, 00161, Italy.

Pasteur Institute-Fondazione Cenci Bolognetti, Rome, 00161, Italy.

出版信息

Aging Cell. 2016 Aug;15(4):755-65. doi: 10.1111/acel.12485. Epub 2016 May 11.

Abstract

Aging is associated with alterations in the content and patterns of DNA methylation virtually throughout the entire human lifespan. Reasons for these variations are not well understood. However, several lines of evidence suggest that the epigenetic instability in aging may be traced back to the alteration of the expression of DNA methyltransferases. Here, the association of the expression of DNA methyltransferases DNMT1 and DNMT3B with age has been analysed in the context of the MARK-AGE study, a large-scale cross-sectional study of the European general population. Using peripheral blood mononuclear cells, we assessed the variation of DNMT1 and DNMT3B gene expression in more than two thousand age-stratified women and men (35-75 years) recruited across eight European countries. Significant age-related changes were detected for both transcripts. The level of DNMT1 gradually dropped with aging but this was only observed up to the age of 64 years. By contrast, the expression of DNMT3B decreased linearly with increasing age and this association was particularly evident in females. We next attempted to trace the age-related changes of both transcripts to the influence of different variables that have an impact on changes of their expression in the population, including demographics, dietary and health habits, and clinical parameters. Our results indicate that age affects the expression of DNMT1 and DNMT3B as an almost independent variable in respect of all other variables evaluated.

摘要

几乎在整个人类寿命期间,衰老都与DNA甲基化的含量和模式改变相关。这些变化的原因尚不清楚。然而,几条证据表明衰老过程中的表观遗传不稳定性可能追溯到DNA甲基转移酶表达的改变。在此,在MARK-AGE研究(一项针对欧洲普通人群的大规模横断面研究)的背景下,分析了DNA甲基转移酶DNMT1和DNMT3B的表达与年龄的关联。我们使用外周血单核细胞,评估了在八个欧洲国家招募的两千多名按年龄分层的男女(35 - 75岁)中DNMT1和DNMT3B基因表达的变化。两种转录本均检测到与年龄相关的显著变化。DNMT1的水平随衰老逐渐下降,但仅在64岁之前观察到这种情况。相比之下,DNMT3B的表达随年龄增长呈线性下降,这种关联在女性中尤为明显。接下来,我们试图将两种转录本与年龄相关的变化追溯到不同变量的影响,这些变量会影响它们在人群中表达的变化,包括人口统计学、饮食和健康习惯以及临床参数。我们的结果表明,就所有其他评估变量而言,年龄几乎作为一个独立变量影响DNMT1和DNMT3B的表达。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fa5c/4933658/60a1c0db1036/ACEL-15-755-g001.jpg

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