Dipartimento di Medicina Molecolare e Biotecnologie Mediche, Università degli Studi di Napoli Federico II, 80131 Napoli, Italy.
CEINGE Biotecnologie Avanzate, 80145 Napoli, Italy.
Genes (Basel). 2021 Jun 8;12(6):881. doi: 10.3390/genes12060881.
To identify host genetic determinants involved in humoral immunity and associated with the risk of developing severe COVID-19, we analyzed 500 SARS-CoV-2 positive subjects from Southern Italy. We examined the coding sequences of 10 common variable immunodeficiency-associated genes obtained by the whole-exome sequencing of 121 hospitalized patients. These 10 genes showed significant enrichment in predicted pathogenic point mutations in severe patients compared with the non-severe ones. Moreover, in the gene, the minor allele of the p.His159Tyr variant, which is known to increase NF-kB activation and B-cell production, was significantly more frequent in the 38 severe cases compared to both the 83 non-severe patients and the 375 asymptomatic subjects further genotyped. This finding identified a potential genetic risk factor of severe COVID-19 that not only may serve to unravel the mechanisms underlying the disease severity but, also, may contribute to build the rationale for individualized management based on B-cell therapy.
为了确定与体液免疫相关并与发生严重 COVID-19 风险相关的宿主遗传决定因素,我们分析了来自意大利南部的 500 名 SARS-CoV-2 阳性受试者。我们通过对 121 名住院患者的全外显子组测序,检测了 10 个常见可变免疫缺陷相关基因的编码序列。与非重症患者相比,这些基因在重症患者中预测的致病性点突变中显著富集。此外,在 基因中,已知增加 NF-kB 激活和 B 细胞产生的 p.His159Tyr 变异的次要等位基因在 38 例重症病例中明显比 83 例非重症患者和进一步进行基因分型的 375 例无症状患者更为频繁。这一发现确定了一个严重 COVID-19 的潜在遗传风险因素,它不仅可以帮助我们揭示疾病严重程度的潜在机制,而且还可能有助于基于 B 细胞治疗制定个体化管理的理论基础。
