Exome-wide evidence of compound heterozygous effects across common phenotypes in the UK Biobank.

IF 11.1 Q1 CELL BIOLOGY Cell genomics Pub Date : 2024-07-10 Epub Date: 2024-06-28 DOI:10.1016/j.xgen.2024.100602
Frederik H Lassen, Samvida S Venkatesh, Nikolas Baya, Barney Hill, Wei Zhou, Alex Bloemendal, Benjamin M Neale, Benedikt M Kessler, Nicola Whiffin, Cecilia M Lindgren, Duncan S Palmer
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Abstract

The phenotypic impact of compound heterozygous (CH) variation has not been investigated at the population scale. We phased rare variants (MAF ∼0.001%) in the UK Biobank (UKBB) exome-sequencing data to characterize recessive effects in 175,587 individuals across 311 common diseases. A total of 6.5% of individuals carry putatively damaging CH variants, 90% of which are only identifiable upon phasing rare variants (MAF < 0.38%). We identify six recessive gene-trait associations (p < 1.68 × 10-7) after accounting for relatedness, polygenicity, nearby common variants, and rare variant burden. Of these, just one is discovered when considering homozygosity alone. Using longitudinal health records, we additionally identify and replicate a novel association between bi-allelic variation in ATP2C2 and an earlier age at onset of chronic obstructive pulmonary disease (COPD) (p < 3.58 × 10-8). Genetic phase contributes to disease risk for gene-trait pairs: ATP2C2-COPD (p = 0.000238), FLG-asthma (p = 0.00205), and USH2A-visual impairment (p = 0.0084). We demonstrate the power of phasing large-scale genetic cohorts to discover phenome-wide consequences of compound heterozygosity.

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英国生物库中常见表型的复合杂合效应的全外显子证据。
复合杂合子(CH)变异的表型影响尚未在人群范围内进行调查。我们对英国生物库(UKBB)外显子组测序数据中的罕见变异(MAF ∼0.001%)进行了分阶段分析,以确定311种常见疾病中175,587人的隐性效应特征。共有6.5%的个体携带有可能造成损害的CH变异,其中90%的变异只有在考虑了亲缘关系、多基因性、附近的常见变异和罕见变异负担后,通过分期罕见变异(MAF -7)才能确定。如果只考虑同源性,其中只有一个变异被发现。利用纵向健康记录,我们还发现并复制了 ATP2C2 双等位基因变异与慢性阻塞性肺病(COPD)发病年龄提前之间的新型关联(p -8)。遗传阶段对基因-性状对的疾病风险有影响:ATP2C2-COPD (p = 0.000238)、FLG-哮喘 (p = 0.00205) 和 USH2A-视力障碍 (p = 0.0084)。我们展示了大规模遗传队列分期发现复合杂合子全表型后果的能力。
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