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Different measures of “genome-wide” DNA methylation exhibit unique properties in placental and somatic tissues
Authors:E Magda Price  Allison M Cotton  Maria S Pe?aherrera  Deborah E McFadden  Michael S Kobor  Wendy Robinson
Institution:1.Department of Obstetrics and Gynaecology; University of British Columbia; Vancouver, BC Canada;2.Department of Medical Genetics; University of British Columbia; Vancouver, BC Canada;3.Child and Family Research Institute, British Columbia; Vancouver, BC Canada;4.Department of Pathology, University of British Columbia; Vancouver, BC Canada;5.Centre for Molecular Medicine and Therapeutics, Child and Family Research Institute; Vancouver, BC Canada
Abstract:DNA methylation of CpGs located in two types of repetitive elements—LINE1 (L1) and Alu—is used to assess “global” changes in DNA methylation in studies of human disease and environmental exposure. L1 and Alu contribute close to 30% of all base pairs in the human genome and transposition of repetitive elements is repressed through DNA methylation. Few studies have investigated whether repetitive element DNA methylation is associated with DNA methylation at other genomic regions, or the biological and technical factors that influence potential associations. Here, we assess L1 and Alu DNA methylation by Pyrosequencing of consensus sequences and using subsets of probes included in the Illumina Infinium HumanMethylation27 BeadChip array. We show that evolutionary age and assay method affect the assessment of repetitive element DNA methylation. Additionally, we compare Pyrosequencing results for repetitive elements to average DNA methylation of CpG islands, as assessed by array probes classified into strong, weak and non-islands. We demonstrate that each of these dispersed sequences exhibits different patterns of tissue-specific DNA methylation. Correlation of DNA methylation suggests an association between L1 and weak CpG island DNA methylation in some of the tissues examined. We caution, however, that L1, Alu and CpG island DNA methylation are distinct measures of dispersed DNA methylation and one should not be used in lieu of another. Analysis of DNA methylation data is complex and assays may be influenced by environment and pathology in different or complementary ways.
Keywords:Alu  CpG island  DNA Methylation  L1  epigenetics  placenta  repetitive elements
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