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Pooled Sequencing of 531 Genes in Inflammatory Bowel Disease Identifies an Associated Rare Variant in BTNL2 and Implicates Other Immune Related Genes

机译:炎症性肠病中531个基因的集合测序确定了BTNL2的相关稀有变异并暗示了其他免疫相关基因

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Author Summary Crohn's disease and ulcerative colitis are two forms of inflammatory bowel disease which cause chronic inflammation of the gastrointestinal tract. Common genetic variants in more than 160 regions of the human genome have been associated with an altered risk of these disorders, but leave much of the estimated genetic contribution to disease risk unexplained. We sought to establish whether rare genetic variants which alter the structure or function of the proteins encoded by genes also contribute to disease susceptibility. We used high throughput DNA sequencing to screen over 500 genes for such variants in nearly 500 patients and controls, and validated interesting variants in about 10,000 patients and 7,000 controls. We detected association of a limited number of rare variants from coding regions with disease, suggesting that they do not account for a large proportion of genetic susceptibility. However, they highlight the involvement of genes of potential importance in the development of inflammatory bowel disease, including those involved in the activation of immune cells, the regulation of immune response genes, and the degradation of proteins in cells.
机译:作者摘要克罗恩病和溃疡性结肠炎是引起肠胃道慢性炎症的两种形式的炎症性肠病。在人类基因组的160多个区域中,常见的遗传变异与这些疾病的风险改变有关,但尚无法解释对疾病风险的许多估计遗传贡献。我们试图确定改变基因编码蛋白质结构或功能的罕见遗传变异是否也有助于疾病易感性。我们使用高通量DNA测序技术在近500名患者和对照中筛选了500多个基因用于此类变异,并在大约10,000名患者和7,000个对照中验证了有趣的变异。我们检测到来自编码区的有限数量的稀有变体与疾病的关联,这表明它们并未占遗传易感性的很大比例。然而,它们强调了炎症性肠病发展过程中潜在重要基因的参与,包括那些与免疫细胞活化,免疫应答基因调控和细胞蛋白质降解有关的基因。

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