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Literature DB >> 20844285

Personalized epigenomic signatures that are stable over time and covary with body mass index.

Andrew P Feinberg¹, Rafael A Irizarry, Delphine Fradin, Martin J Aryee, Peter Murakami, Thor Aspelund, Gudny Eiriksdottir, Tamara B Harris, Lenore Launer, Vilmundur Gudnason, M Daniele Fallin.

Abstract

The epigenome consists of non-sequence-based modifications, such as DNA methylation, that are heritable during cell division and that may affect normal phenotypes and predisposition to disease. Here, we have performed an unbiased genome-scale analysis of ~4 million CpG sites in 74 individuals with comprehensive array-based relative methylation (CHARM) analysis. We found 227 regions that showed extreme interindividual variability [variably methylated regions (VMRs)] across the genome, which are enriched for developmental genes based on Gene Ontology analysis. Furthermore, half of these VMRs were stable within individuals over an average of 11 years, and these VMRs defined a personalized epigenomic signature. Four of these VMRs showed covariation with body mass index consistently at two study visits and were located in or near genes previously implicated in regulating body weight or diabetes. This work suggests an epigenetic strategy for identifying patients at risk of common disease.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Year: 2010 PMID： 20844285 PMCID： PMC3137242 DOI： 10.1126/scitranslmed.3001262

Source DB: PubMed Journal: Sci Transl Med ISSN： 1946-6234 Impact factor: 17.956

34 in total

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7. Positional cloning of Sorcs1, a type 2 diabetes quantitative trait locus.

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8. Sex-specific findings from a genome-wide linkage analysis of human fatness in non-Hispanic whites and African Americans: the HyperGEN study.

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9. Overweight, obesity, and mortality in a large prospective cohort of persons 50 to 71 years old.

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156 in total

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4. Associations with early-life socio-economic position in adult DNA methylation.

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