A Novel Case of IFNAR1 Deficiency Identified a Common Canonical Splice Site Variant in DOCK8 in Western Polynesia: The Importance of Validating Variants of Unknown Significance in Under-Represented Ancestries.

IF 7.2 2区 医学 Q1 IMMUNOLOGY
Aimee Huynh, Paul E Gray, Anna Sullivan, Joseph Mackie, Antoine Guerin, Geetha Rao, Karrnan Pathmanandavel, Erika Della Mina, Georgina Hollway, Matthew Hobbs, Karen Enthoven, Patrick O'Young, Sam McManus, Luke H Wainwright, Megan Higgins, Fallon Noon, Melanie Wong, Paul Bastard, Qian Zhang, Jean-Laurent Casanova, Kuang-Chih Hsiao, Alberto Pinzon-Charry, Cindy S Ma, Stuart G Tangye
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Abstract

Advanced genomic technologies such as whole exome or whole genome sequencing have improved diagnoses and disease outcomes for individuals with genetic diseases. Yet, variants of unknown significance (VUS) require rigorous validation to establish disease causality or modification, or to exclude them from further analysis. Here, we describe a young individual of Polynesian ancestry who in the first 13 mo of life presented with SARS-CoV-2 pneumonia, severe enterovirus meningitis and adenovirus gastroenteritis, and severe adverse reaction to MMR vaccination. Genomic analysis identified a previously reported pathogenic homozygous variant in IFNAR1 (c.1156G > T, p.Glu386* LOF), which is common in Western Polynesia. Moreover, a new and putatively deleterious canonical splice site variant in DOCK8 was also found in homozygosity (c.3234 + 2T > C). This DOCK8 variant is common in Polynesians and other under-represented ancestries in large genomic databases. Despite in silico bioinformatic predictions, extensive in vitro and ex vivo analysis revealed the DOCK8 variant likely be neutral. Thus, our study reports a novel case of IFNAR1 deficiency, but also highlights the importance of functional validation of VUS, including those predicted to be deleterious, and the pressing need to expand our knowledge of the genomic architecture and landscape of under-represented populations and ancestries.

Abstract Image

西波利尼西亚的一例新型 IFNAR1 缺乏症患者发现了 DOCK8 中一个常见的规范剪接位点变异:在代表性不足的祖先中验证意义不明的变异的重要性。
全外显子组或全基因组测序等先进的基因组技术改善了遗传病患者的诊断和疾病治疗效果。然而,意义不明的变异(VUS)需要严格的验证才能确定疾病的因果关系或改变,或将其排除在进一步分析之外。在这里,我们描述了一位波利尼西亚血统的年轻人,他在出生后的头 13 个月里患上了 SARS-CoV-2 肺炎、严重的肠道病毒脑膜炎和腺病毒肠胃炎,以及接种麻风腮疫苗后出现的严重不良反应。基因组分析发现了之前报道过的 IFNAR1 致病性同源变体(c.1156G > T, p.Glu386* LOF),该变体在西波利尼西亚很常见。此外,在 DOCK8 中也发现了一个新的、可能是有害的典型剪接位点变异(c.3234 + 2T > C)。这种 DOCK8 变异在波利尼西亚人和其他在大型基因组数据库中代表性不足的祖先中很常见。尽管进行了硅学生物信息学预测,但大量的体外和体内分析表明 DOCK8 变体可能是中性的。因此,我们的研究报告了一个 IFNAR1 缺乏症的新病例,同时也强调了对 VUS(包括那些预测为有害的 VUS)进行功能验证的重要性,以及扩大我们对代表性不足的人群和祖先的基因组结构和景观的了解的迫切需要。
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来源期刊
CiteScore
12.20
自引率
9.90%
发文量
218
审稿时长
2 months
期刊介绍: The Journal of Clinical Immunology publishes impactful papers in the realm of human immunology, delving into the diagnosis, pathogenesis, prognosis, or treatment of human diseases. The journal places particular emphasis on primary immunodeficiencies and related diseases, encompassing inborn errors of immunity in a broad sense, their underlying genotypes, and diverse phenotypes. These phenotypes include infection, malignancy, allergy, auto-inflammation, and autoimmunity. We welcome a broad spectrum of studies in this domain, spanning genetic discovery, clinical description, immunologic assessment, diagnostic approaches, prognosis evaluation, and treatment interventions. Case reports are considered if they are genuinely original and accompanied by a concise review of the relevant medical literature, illustrating how the novel case study advances the field. The instructions to authors provide detailed guidance on the four categories of papers accepted by the journal.
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