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

机译:GWASdb:通过全基因组关联研究鉴定的人类遗传变异数据库

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Recent advances in genome-wide association studies (GWAS) have enabled us to identify thousands of genetic variants (GVs) that are associated with human diseases. As next-generation sequencing technologies become less expensive, more GVs will be discovered in the near future. Existing databases, such as NHGRI GWAS Catalog, collect GVs with only genome-wide level significance. However, many true disease susceptibility loci have relatively moderate P values and are not included in these databases. We have developed GWASdb that contains 20 times more data than the GWAS Catalog and includes less significant GVs (P??1.0?×?10?3) manually curated from the literature. In addition, GWASdb provides comprehensive functional annotations for each GV, including genomic mapping information, regulatory effects (transcription factor binding sites, microRNA target sites and splicing sites), amino acid substitutions, evolution, gene expression and disease associations. Furthermore, GWASdb classifies these GVs according to diseases using Disease-Ontology Lite and Human Phenotype Ontology. It can conduct pathway enrichment and PPI network association analysis for these diseases. GWASdb provides an intuitive, multifunctional database for biologists and clinicians to explore GVs and their functional inferences. It is freely available at http://jjwanglab.org/gwasdb and will be updated frequently.
机译:全基因组关联研究(GWAS)的最新进展使我们能够识别与人类疾病相关的数千种遗传变异(GV)。随着下一代测序技术变得越来越便宜,在不久的将来将会发现更多的GV。现有数据库(例如NHGRI GWAS目录)收集的GV仅具有全基因组水平的意义。但是,许多真实的疾病易感基因座具有相对中等的P值,因此未包含在这些数据库中。我们开发了GWASdb,它包含的数据比GWAS目录多20倍,并且包含从文献中手动编制的不那么重要的GV(P 1.0?×?10 ?3 )。此外,GWASdb为每个GV提供了全面的功能注释,包括基因组作图信息,调节作用(转录因子结合位点,microRNA目标位点和剪接位点),氨基酸取代,进化,基因表达和疾病关联。此外,GWASdb使用疾病本体精简版和人类表型本体论根据疾病对这些GV进行分类。它可以对这些疾病进行途径富集和PPI网络关联分析。 GWASdb为生物学家和临床医生提供了直观的多功能数据库,以探索GV及其功能推论。它可从http://jjwanglab.org/gwasdb免费获得,并将经常更新。

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