Genetic Control of Individual Differences in Gene-Specific Methylation in Human Brain

Zhang, Dandan; Cheng, Lijun; Badner, Judith A.; Chen, Chao; Chen, Qi; Luo, Wei; Craig, David W.; Redman, Margot; Gershon, Elliot S.; Liu, Chun Yu

doi:10.1016/j.ajhg.2010.02.005

Cited by 360 publications

(374 citation statements)

References 36 publications

(58 reference statements)

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“…Rather than studying genetic variants in isolation, the common disease genetic epigenetic (CDGE) hypothesis encourages the simultaneous analysis of both genetic and epigenetic variants (MVPs) to construct 'hepitypes' in order to increase the power of associations in epidemiological studies and minimise inconsistent associations [18,21]. Analysing both the genetic and epigenetic characteristics of a gene and their interaction in disease has recently been the focus of a number of studies [22][23][24]. Cis interactions between genetic and epigenetic variants involve the direct modulation of CpG methylation by SNPs [18] and the correlation of methylation with SNPs within 1 Mb of a CpG [24] while trans interactions involve regulation effects between CpGs and SNPs from more distant genomic regions, including regions from different chromosomes [24].…”

Section: Introductionmentioning

confidence: 99%

“…Analysing both the genetic and epigenetic characteristics of a gene and their interaction in disease has recently been the focus of a number of studies [22][23][24]. Cis interactions between genetic and epigenetic variants involve the direct modulation of CpG methylation by SNPs [18] and the correlation of methylation with SNPs within 1 Mb of a CpG [24] while trans interactions involve regulation effects between CpGs and SNPs from more distant genomic regions, including regions from different chromosomes [24].…”

Section: Introductionmentioning

confidence: 99%

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Vitamin D receptor gene methylation is associated with ethnicity, tuberculosis, and TaqI polymorphism

et al. 2011

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The Vitamin D Receptor (VDR) gene encodes a transcription factor which, on activation by vitamin D, modulates diverse biological processes including calcium homeostasis and immune function. Genetic variation involving VDR shows striking differences in allele frequency between populations and has been associated with disease susceptibility including tuberculosis and autoimmunity, although results have often been conflicting. We hypothesized that methylation of VDR may be population specific and that the combination of differential methylation and genetic variation may characterise TB predisposition. We use bisulphite conversion and/or pyrosequencing to analyse the methylation status of 17 CpGs of VDR and to genotype 7 SNPs in the 3′ CpG Island (CGI 1060), including the commonly studied SNPs ApaI (rs7975232) and TaqI (rs731236). We show that for lymphoblastoid cell lines from two ethnically diverse populations (Yoruba from HapMap, n=30 and Caucasians, n=30) together with TB cases (n=32) and controls (n=29) from the Venda population of South Africa there are methylation variable positions (MVPs) in the 3′ end that significantly distinguish ethnicity (9/17 CpGs) and TB status (3/17 CpGs). Moreover methylation status shows complex association with TaqI genotype highlighting the need to consider both genetic and epigenetic variants in genetic studies of VDR association with disease.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Vitamin D receptor gene methylation is associated with ethnicity, tuberculosis, and TaqI polymorphism

et al. 2011

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“…On the basis of DNA methylation analyses in blood chromatin collected across three generations from the same pedigrees, more than 92% of the differences in methylcytosine load between alleles is explained by haplotype, suggesting a dominant role of genetic variation in the establishment of epigenetic markings, as opposed to environmental influences (Gertz et al, 2011). Likewise, in the human cerebral and cerebellar cortex, methylation of several hundred CpG enriched sequences is significantly affected by genetic variations, including single-nucleotide polymorphisms (SNPs) separated from the CpG site by 41 Mb (Numata et al, 2012;Zhang et al, 2010a). An even larger number of genetic polymorphisms were linked to gene expression differences in the prefrontal cortex, including many SNP-based haplotypes within promoters and around the 5 0 ends of annotated transcripts (Colantuoni et al, 2011).…”

Section: Epigenetics and Transcriptional (Dys) Regulation In Diseasedmentioning

confidence: 99%

Epigenetics in the Human Brain

Houston

Peter

Mitchell

et al. 2012

Neuropsychopharmacol

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Many cellular constituents in the human brain permanently exit from the cell cycle during pre-or early postnatal development, but little is known about epigenetic regulation of neuronal and glial epigenomes during maturation and aging, including changes in mood and psychosis spectrum disorders and other cognitive or emotional disease. Here, we summarize the current knowledge base as it pertains to genome organization in the human brain, including the regulation of DNA cytosine methylation and hydroxymethylation, and a subset of (altogether 4100) residue-specific histone modifications associated with gene expression, and silencing and various other functional chromatin states. We propose that high-resolution mapping of epigenetic markings in postmortem brain tissue or neural cultures derived from induced pluripotent cells (iPS), in conjunction with transcriptome profiling and whole-genome sequencing, will increasingly be used to define the molecular pathology of specific cases diagnosed with depression, schizophrenia, autism, or other major psychiatric disease. We predict that these highly integrative explorations of genome organization and function will provide an important alternative to conventional approaches in human brain studies, which mainly are aimed at uncovering group effects by diagnosis but generally face limitations because of cohort size.

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“…That is, the information is encoded in the length of the telomeres, not in the repeated TTAGGG sequence. Note that there is indeed an effect of genetic variants on TL, 7 but this also the case for DNAmethylation, 12 simply implying that epigenetic(-like) features are also partially under genetic control. Importantly, together with the telomeres, a stable phenotype is inherited as well, ie, absence of replicative senescence, with associated gene expression pattern.…”

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confidence: 99%