The First Affiliated Hospital of Chongqing Medical University, Chongqing Key Laboratory of Ophthalmology, Chongqing Eye Institute, and Chongqing Branch of National Clinical Research Center for Ocular Diseases, Chongqing, China.
The First Affiliated Hospital of Zhengzhou University, Henan Province Eye Hospital, Henan International Joint Research Laboratory for Ocular Immunology and Retinal Injury Repair, Zhengzhou, China.
Ophthalmology. 2022 Jul;129(7):821-828. doi: 10.1016/j.ophtha.2022.03.014. Epub 2022 Mar 18.
The American College of Medical Genetics and Genomics (ACMG) and the Association for Molecular Pathology call for cautious interpretation of variants as causative of a monogenic disorder by stringent standards. We aimed to reclassify the pathogenicity of nucleotide binding oligomerization domain containing 2 (NOD2) variants according to the ACMG guidelines and to characterize clinical features in patients whose ocular disease might actually be explained by Blau syndrome.
Genetic analysis and descriptive study.
A total of 1003 unrelated healthy individuals and 3921 sporadic patients who presented with uveitis.
Whole-exome sequencing was performed on all healthy participants and 551 patients with uveitis, and targeted NOD2 resequencing was performed on the remaining 3370 patients with uveitis. Pathogenicity for Blau syndrome was classified for NOD2 variants identified by sequencing in study participants according to the ACMG guidelines. Clinical manifestations were compared among NOD2 variants of different levels of classification.
Pathogenicity of variants.
Eight NOD2 gain-of-function mutations, p.R334W, p.R334Q, p.E383K, p.G481D, p.W490S, p.M513T, p.R587C, and p.N670K, were classified as pathogenic, and 66 patients (1.7%) with uveitis were diagnosed with Blau syndrome due to these mutations. Of 66 with Blau syndrome, anterior uveitis accounted for 39.4%, posterior uveitis for 9.1%, and panuveitis for 51.5%. A proportion of 21.2% of Blau syndrome presented as multifocal choroiditis, 48.5% had papillitis, and 74.2% showed retinal microvasculitis detected by fundus fluorescein angiography. Six NOD2 variants, p.P268S, p.R311W, p.R471C, p.A612T, p.R702W, and p.V955I, were considered nonpathogenic for Blau syndrome and were identified in 96 patients with uveitis. The incidence of bilateral uveitis (86.4%), secondary glaucoma (47.0%), epiretinal membrane (7.6%), choroidal neovascularization (4.6%), retinal atrophy (10.6%), arthritis (69.7%), joint deformity (51.5%), and skin rash (40.9%) was higher in Blau syndrome than in patients with uveitis carrying non-Blau-causing NOD2 variants. Patients with Blau syndrome permanently experienced overall poorer best-corrected visual acuity. Several rare NOD2 mutations, p.I722L (2 cases), p.T476P (1 case), p.T476del (1 case), and p.R439H (1 case), were newly identified.
Pathogenic NOD2 variants for Blau syndrome were limited to those gain-of-function mutations and were associated with a high risk for arthritis, skin rash, permanent visual loss, and ocular complications in patients with uveitis.
美国医学遗传学与基因组学学会(ACMG)和分子病理学协会呼吁根据严格标准谨慎解释变异为单基因疾病的致病因素。我们旨在根据 ACMG 指南重新分类核苷酸结合寡聚结构域 2 (NOD2) 变异的致病性,并描述可能实际上由 Blau 综合征引起的眼部疾病的患者的临床特征。
遗传分析和描述性研究。
共纳入 1003 名无相关疾病的健康个体和 3921 名患有葡萄膜炎的散发性患者。
对所有健康参与者和 551 名患有葡萄膜炎的患者进行全外显子组测序,并对其余 3370 名患有葡萄膜炎的患者进行靶向 NOD2 重测序。根据 ACMG 指南,对研究参与者测序中发现的 NOD2 变异进行 Blau 综合征致病性分类。比较不同分类水平的 NOD2 变异的临床表现。
变异的致病性。
发现 8 种 NOD2 功能获得性突变,p.R334W、p.R334Q、p.E383K、p.G481D、p.W490S、p.M513T、p.R587C 和 p.N670K,被归类为致病性,66 名(1.7%)患有葡萄膜炎的患者被诊断为 Blau 综合征,原因是这些突变。在 66 名患有 Blau 综合征的患者中,前葡萄膜炎占 39.4%,后葡萄膜炎占 9.1%,全葡萄膜炎占 51.5%。21.2%的 Blau 综合征表现为多灶性脉络膜炎,48.5%有视乳头炎,74.2%在眼底荧光血管造影下显示视网膜微血管炎。发现 6 种 NOD2 变异,p.P268S、p.R311W、p.R471C、p.A612T、p.R702W 和 p.V955I,被认为对 Blau 综合征无致病性,在 96 名患有葡萄膜炎的患者中发现。双侧葡萄膜炎(86.4%)、继发性青光眼(47.0%)、视网膜前膜(7.6%)、脉络膜新生血管(4.6%)、视网膜萎缩(10.6%)、关节炎(69.7%)、关节畸形(51.5%)和皮疹(40.9%)在 Blau 综合征患者中发生率高于携带非 Blau 综合征致病变异的葡萄膜炎患者。Blau 综合征患者的最佳矫正视力总体永久性较差。还发现了几种新的 NOD2 突变,p.I722L(2 例)、p.T476P(1 例)、p.T476del(1 例)和 p.R439H(1 例)。
Blau 综合征致病性 NOD2 变异仅限于那些功能获得性突变,并与葡萄膜炎患者的关节炎、皮疹、永久性视力丧失和眼部并发症风险增加相关。
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