Schizophrenia is a highly heritable disorder. Genome-wide association studies based largely on commonalleles have identified over 100 schizophrenia risk loci, but it is also evident from studies of copy number variants (CNVs) and from exome-sequencing studies that rare alleles are also involved. Full characterization of the contribution of rare alleles to the disorder awaits the deployment of sequencing technology in very large sample sizes, meanwhile, as an interim measure, exome arrays allow rare non-synonymous variants to be sampled at a fraction of the cost. In an analysis of exome array data from 13 688 individuals (5585 cases and 8103 controls) from the UK, we found that rare (minor allele frequency <0.1%) variant association signal was enriched among genes that map to autosomal loci that are genome-wide significant (GWS) in common variant studies of schizophrenia genome-wide association study (P-GWAS = 0.01) as well as gene sets known to be enriched for rare variants in sequencing studies (P-RARE = 0.026). We also identified the gene-wise equivalent of GWS support for WDR88 (WD repeat-containing protein 88), a gene of unknown function (P = 6.5 x 10(-7)). Rare alleles represented on exome chip arrays contribute to the genetic architecture of schizophrenia, but as is the case for GWAS, very large studies are required to reveal additional susceptibility alleles for the disorder.
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机译:精神分裂症是一种高度遗传的疾病。全基因组关联研究主要基于共同等位基因,已鉴定出100多个精神分裂症危险基因座,但从拷贝数变异(CNV)研究和外显子组测序研究中也可以看出,罕见的等位基因也参与其中。罕见等位基因对疾病的贡献的完整表征有待在非常大的样本量中应用测序技术,同时,作为一项临时措施,外显子组阵列允许以很少的成本对罕见的非同义变体进行采样。在对来自英国的13688名个体(5585例病例和8103例对照)的外显子组阵列数据进行的分析中,我们发现罕见的(次等位基因频率<0.1%)变体关联信号在映射到常染色体位点的基因中富集了在精神分裂症全基因组关联研究的常见变异研究中(P-GWAS = 0.01)以及在测序研究中已知富含稀有变异的基因集(P-RARE = 0.026)中具有广泛显着性(GWS)。我们还确定了GWS对WDR88(含WD重复序列的蛋白88)的基因支持,这是一个功能未知的基因(P = 6.5 x 10(-7))。外显子组芯片阵列上代表的罕见等位基因有助于精神分裂症的遗传结构,但对于GWAS而言,需要进行大量研究才能揭示该疾病的其他易感性等位基因。
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