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A review of genome-wide association studies for multiple sclerosis: classical and hypothesis-driven approaches

机译:多发性硬化症的全基因组关联研究综述:经典和假设驱动的方法

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Multiple sclerosis (MS) is a common complex neurodegenerative disease of the central nervous system. It develops with autoimmune inflammation and demyelination. Genome-wide association studies (GWASs) serve as a powerful tool for investigating the genetic architecture of MS and are generally used to identify the genetic factors of disease susceptibility, clinical phenotypes, and treatment response. This review considers the main achievements and challenges of using GWAS to identify the genes involved in MS. It also describes hypothesis-driven studies with extensive genome coverage of the selected regions, complementary to GWASs. To date, over 100 MS risk loci have been identified by the combination of both approaches; 40 of them were found in at least two GWASs and meet genome-wide significance threshold (p a parts per thousand currency sign 5 x 10(-8)) in at least one GWAS, whereas the threshold for the rest of GWASs was set in our review at p < 1 x 10(-5). Yet, MS risk loci identified to date explain only a part of the total heritability, and the reasons of "missing heritability" are discussed. The functions of MS-associated genes are described briefly; the majority of them encode immune-response proteins involved in the main stages of MS pathogenesis.
机译:多发性硬化症(MS)是中枢神经系统常见的复杂神经退行性疾病。随着自身免疫炎症和脱髓鞘而发展。全基因组关联研究(GWAS)是研究MS遗传结构的有力工具,通常用于确定疾病易感性,临床表型和治疗反应的遗传因素。这篇综述考虑了使用GWAS鉴定MS中涉及的基因的主要成就和挑战。它还描述了假设驱动的研究,对选定区域进行了广泛的基因组覆盖,与GWAS互补。迄今为止,通过两种方法的组合已经确定了100多个MS风险位点。在至少两个GWAS中发现了40个,并且在至少一个GWAS中达到了全基因组显着性阈值(每千个货币符号的pa分数5 x 10(-8)),而其余GWAS的阈值在我们的在p <1 x 10(-5)下查看。然而,迄今为止确定的MS风险基因座仅解释了总遗传力的一部分,并讨论了“遗传力缺失”的原因。简要介绍了MS相关基因的功能。它们中的大多数编码参与MS发病机理主要阶段的免疫应答蛋白。

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