GWASdb: a database for human genetic variants identified by genome-wide association studies

Plewczynski, Dariusz; Wang, Panwen; Liu, Xiaorong; Lim, Ee Lyn; Wang, Zhangyong; Yeager, Meredith; Wong, Maria Pik; Sham, Pak C.; Chanock, Stephen J.; Wang, Junwen

doi:10.1093/nar/gkr1182

Cited by 195 publications

(170 citation statements)

References 42 publications

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“…In this respect, DNA methylation might display a potent intermediate event that could be useful to interpret the GWAS results. For this reason, we performed model-based gene set analysis (Bauer et al 2011) to compare SNPs directly associated with popCpGs and GWA studies available at GWASdb (Li et al 2012). We found some interesting associations related to age of menarche, and HIV control; in particular, we determined highly significant enrichment for hepatitis B infection through the detection of six SNPs directly related to CpG sites that were differentially methylated between populations (Enrichment score: 0.99) (Supplemental Table S7; Bauer et al 2011).…”

Section: Cross Talk Between Population-specific Epigenetic and Genetimentioning

confidence: 99%

“…To establish a causal relationship between genetic variability, DNA methylation level, and distinct phenotypes, we determined enrichment of meQTL-related SNPs in the entire set of GWA studies available at GWASdb (Li et al 2012) using model-based gene set analysis (Bauer et al 2011). The method analyzes all categories at once by embedding them in a Bayesian network.…”

Section: Enrichment Analysis Of Gwas-associated Polymorphismsmentioning

confidence: 99%

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DNA methylation contributes to natural human variation

et al. 2013

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DNA methylation patterns are important for establishing cell, tissue, and organism phenotypes, but little is known about their contribution to natural human variation. To determine their contribution to variability, we have generated genome-scale DNA methylation profiles of three human populations (Caucasian-American, African-American, and Han Chinese-American) and examined the differentially methylated CpG sites. The distinctly methylated genes identified suggest an influence of DNA methylation on phenotype differences, such as susceptibility to certain diseases and pathogens, and response to drugs and environmental agents. DNA methylation differences can be partially traced back to genetic variation, suggesting that differentially methylated CpG sites serve as evolutionarily established mediators between the genetic code and phenotypic variability. Notably, one-third of the DNA methylation differences were not associated with any genetic variation, suggesting that variation in population-specific sites takes place at the genetic and epigenetic levels, highlighting the contribution of epigenetic modification to natural human variation.

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Section: Cross Talk Between Population-specific Epigenetic and Genetimentioning

confidence: 99%

Section: Enrichment Analysis Of Gwas-associated Polymorphismsmentioning

confidence: 99%

DNA methylation contributes to natural human variation

et al. 2013

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“…In the past few years, GWAS have been conducted for hundreds of complex diseases and traits ( 80 ). Several bioinformatic strategies have been developed to map GWAS-derived disease-associated variants, as well as SNPs in strong linkage disequilibrium (LD), onto predicted miRNA target sites (81)(82)(83)(84)(85)(86). A very recent approach uncovered 87 such SNPs ( 84 ).…”

Section: Genetic Variation In Mirna Transcriptional Control Elementsmentioning

confidence: 99%

Needles in the genetic haystack of lipid disorders: single nucleotide polymorphisms in the microRNA regulome

Sethupathy

2013

Journal of Lipid Research

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This article is available online at http://www.jlr.org inhibits protein translation. Although mammalian miRNAs were not discovered until a decade ago ( 2 ), they have rapidly emerged as important posttranscriptional regulators of gene expression in a wide variety of biological pathways ( 3 ). Moreover, miRNAs have been demonstrated to be i ) stable plasma biomarkers of physiological status ( 4,5 ), ii ) novel intercellular signaling molecules ( 6 ), iii ) etiological factors in complex diseases ( 7 ), and iv ) promising therapeutic targets ( 8,9 ).In 2002, miR-122 was found to be the most abundant miRNA in the liver, accounting for greater than 70% of all hepatic miRNA expression ( 2 ). More recent, high-throughput small RNA sequencing (smRNA-seq) studies have confi rmed this fi nding and, notably, have not detected miR-122 in any other cell type ( 10 ). Circulating levels of miR-122 have been identifi ed as a clinically relevant biomarker of liver injury ( 11, 12 ), cirrhosis ( 13 ), necroinfl ammation ( 14 ), and hyperlipidemia ( 15 ). In 2005, miR-122 was also shown to directly promote the replication of the hepatitis C virus (HCV) ( 16 ). Subsequently, it was demonstrated that inhibition of miR-122 by a locked nucleic acid (LNA) antisense oligonucleotide diminishes HCV viremia in chimpanzees ( 17 ). The anti-miR-122 LNA molecule (known as Miravirsen) has since advanced to phase II human clinical trials for hepatitis C treatment, and it appears to induce a potent antiviral effect in the absence of evident liver or cardiac toxicities ( 18 ).miR-122 was also the fi rst miRNA identifi ed as a regulator of lipid metabolism ( 19 ). In 2006, antisense oligonucleotide-mediated inhibition of miR-122 (ASO-miR-122) in mice reduced plasma cholesterol levels, decreased hepatic lipid synthesis, and enhanced hepatic fatty acid oxidation ( 19 ). Moreover, the ASO-miR-122 was also able to reverse the effects of diet-induced obesity by reducing hepatic steatosis. Abbreviations: LRE, long-range regulatory element; miRNA (miR), microRNA; miR-122, miRNA-122; pre-miRNA, miRNA precursor; primiRNA, primary miRNA; ORF, open reading frame; RISC, RNA-induced silencing complex; SNP, single nucleotide polymorphism; TF, transcriptional factor; UTR, untranslated region.

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“…These contain a wealth of information highlighting the organisation, structure and function of the genome. Other specialist resources provide a dense functional annotation of regions that border GWAS hits (http://jjwanglab.org:8080/gwasdb/) 120 .…”

Section: Gxewas: the Systematically Tractable Meets The Biologically mentioning

confidence: 99%

Old Obstacles on New Horizons: The Challenge of Implementing Gene X Environment Discoveries in Schizophrenia Research

Iyegbe

Modinos

Sanchez³

2012

Public Health - Methodology, Environmental and Systems Issues

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GWASdb: a database for human genetic variants identified by genome-wide association studies

Cited by 195 publications

References 42 publications

DNA methylation contributes to natural human variation

DNA methylation contributes to natural human variation

Needles in the genetic haystack of lipid disorders: single nucleotide polymorphisms in the microRNA regulome

Old Obstacles on New Horizons: The Challenge of Implementing Gene X Environment Discoveries in Schizophrenia Research

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