DNA methylation: conducting the orchestra from exposure to phenotype?

被引:0
|
作者
Fleur A. D. Leenen
Claude P. Muller
Jonathan D. Turner
机构
[1] Luxembourg Institute of Health,Department of Infection and Immunity
[2] University of Trier,Department of Immunology, Research Institute of Psychobiology
来源
Clinical Epigenetics | 2016年 / 8卷
关键词
DNA methylation; EWAS; Association studies; Biomarker; Transcriptional microvariability; Gene-environment interactions;
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摘要
DNA methylation, through 5-methyl- and 5-hydroxymethylcytosine (5mC and 5hmC), is considered to be one of the principal interfaces between the genome and our environment, and it helps explain phenotypic variations in human populations. Initial reports of large differences in methylation level in genomic regulatory regions, coupled with clear gene expression data in both imprinted genes and malignant diseases, provided easily dissected molecular mechanisms for switching genes on or off. However, a more subtle process is becoming evident, where small (<10 %) changes to intermediate methylation levels are associated with complex disease phenotypes. This has resulted in two clear methylation paradigms. The latter “subtle change” paradigm is rapidly becoming the epigenetic hallmark of complex disease phenotypes, although we are currently hampered by a lack of data addressing the true biological significance and meaning of these small differences.
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