Genentech, Inc., 1 DNA Way, South San Francisco, CA, 94080, USA.
Maze Therapeutics, 131 Oyster Point Blvd STE 200, South San Francisco, CA, 94080, USA.
Sci Rep. 2022 Apr 2;12(1):5574. doi: 10.1038/s41598-022-09447-8.
Genome-wide association studies (GWAS) have identified many common variant loci associated with asthma susceptibility, but few studies investigate the genetics underlying moderate-to-severe asthma risk. Here, we present a whole-genome sequencing study comparing 3181 moderate-to-severe asthma patients to 3590 non-asthma controls. We demonstrate that asthma risk is genetically correlated with lung function measures and that this component of asthma risk is orthogonal to the eosinophil genetics that also contribute to disease susceptibility. We find that polygenic scores for reduced lung function are associated with younger asthma age of onset. Genome-wide, seven previously reported common asthma variant loci and one previously reported lung function locus, near THSD4, reach significance. We replicate association of the lung function locus in a recently published GWAS of moderate-to-severe asthma patients. We additionally replicate the association of a previously reported rare (minor allele frequency < 1%) coding variant in IL33 and show significant enrichment of rare variant burden in genes from common variant allergic disease loci. Our findings highlight the contribution of lung function genetics to moderate-to-severe asthma risk, and provide initial rare variant support for associations with moderate-to-severe asthma risk at several candidate genes from common variant loci.
全基因组关联研究(GWAS)已经确定了许多与哮喘易感性相关的常见变异位点,但很少有研究探讨中度至重度哮喘风险的遗传基础。在这里,我们进行了一项全基因组测序研究,将 3181 名中度至重度哮喘患者与 3590 名非哮喘对照进行比较。我们证明哮喘风险与肺功能测量值在遗传上相关,而这种哮喘风险成分与也有助于疾病易感性的嗜酸性粒细胞遗传学是正交的。我们发现,肺功能降低的多基因评分与哮喘发病年龄较小有关。全基因组范围内,七个先前报道的常见哮喘变异位点和一个先前报道的肺功能位点,位于 THSD4 附近,达到了显著性水平。我们在最近发表的一项中度至重度哮喘患者的 GWAS 中复制了肺功能位点的关联。我们还复制了先前报道的 IL33 中一个罕见(次要等位基因频率<1%)编码变异的关联,并显示常见变异过敏疾病位点基因中罕见变异负担的显著富集。我们的研究结果强调了肺功能遗传学对中度至重度哮喘风险的贡献,并为几个常见变异位点的候选基因与中度至重度哮喘风险的关联提供了初步的罕见变异支持。
