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Genome-wide association analyses identify 39 new susceptibility loci for diverticular disease

机译:基因组关联分析识别39个憩室疾病的新易感位点

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Diverticular disease is common and has a high morbidity. Treatments are limited owing to the poor understanding of its pathophysiology. Here, to elucidate its etiology, we performed a genome-wide association study of diverticular disease (27,444cases; 382,284 controls) from the UK Biobank and tested for replication in the Michigan Genomics Initiative (2,572 cases; 28,649 controls). We identified 42 loci associated with diverticular disease; 39 of these loci are novel. Using data-driven expression-prioritized integration for complex traits (DEPICT), we show that genes in these associated regions are significantly enriched for expression in mesenchymal stem cells and multiple connective tissue cell types and are co-expressed with genes that have a role in vascular and mesenchymal biology. Genes in these associated loci have roles in immunity, extracellular matrix biology, cell adhesion, membrane transport and intestinal motility. Phenome-wide association analysis of the 42 variants shows a common etiology of diverticular disease with obesity and hernia. These analyses shed light on the genomic landscape of diverticular disease.
机译:憩室疾病是常见的并且具有高发病率。由于对其病理生理学的理解差,治疗有限。在这里,为了阐明其病因,我们从英国Biobank进行了憩室疾病(27,444例; 382,​​284个对照)的基因组 - 宽协会研究,并在密歇根基因组学倡议中进行了复制(2,572例; 28,649个控制)。我们确定了42个与憩室疾​​病相关的基因座;这些基因座中的39个是新颖的。使用数据驱动的表达优先考虑的复杂性状的整合(描绘),我们表明这些相关区域中的基因在间充质干细胞和多种结缔组织细胞类型中显着富集,并且与具有作用的基因共表达血管和间充质生物学。这些相关基因座中的基因具有免疫的作用,细胞外基质生物学,细胞粘附,膜运输和肠蠕动。 42个变体的苯齐范围的关联分析显示出肥胖和疝气的憩室疾病的常见病因。这些分析了卵子疾病基因组景观的棚光。

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