携带意义未明变异的家族性地中海热患者的表型特征。
Phenotypic characterization of Familial Mediterranean Fever patients harboring variants of uncertain significance.
机构信息
Department of Rheumatology, Faculty of Medicine, Hacettepe University, Ankara, Turkey
Department of Rheumatology, Faculty of Medicine, Osmangazi University, Eskisehir, Turkey
出版信息
Turk J Med Sci. 2021 Aug 30;51(4):1695-1701. doi: 10.3906/sag-2011-273.
BACKGROUND/AIM: Familial Mediterranean Fever (FMF) is the prototype of hereditary autoinflammatory disorders and caused by mutations on the MEFV gene located on the short arm of chromosome 16. Although some MEFV variants are clearly associated with disease phenotype, there are numerous variants with unknown clinical association which are termed as variants of uncertain significance (VUS). Here, we present clinical correlations of VUS in a large cohort of adult FMF patients from three tertiary centers located in Central Anatolia.
MATERIALS AND METHODS
All patients were recruited from FMF in Central Anatolia (FiCA) cohort. Demographic (sex, age at disease onset) and clinical features (disease characteristics, attack frequency, mean colchicine dose, colchicine nonresponsiveness, amyloidosis, and persistent inflammation) of patients with VUS were compared with those harboring pathogenic variants. Disease severity and damage were also evaluated using international severity score for FMF (ISSF) and autoinflammatory disease damage index (ADDI), respectively.
RESULTS
Among 971 participants included, MEFV gene analysis results were available for 814 patients. Twenty-six (3.2%) patients had single heterozygous VUS and 54 (6.6%) had pathogenic/VUS complex heterozygous variants. Patients with single heterozygous VUS had similar demographic/clinical features, ISSF and ADDI scores compared to those with single heterozygous pathogenic variant (p > 0.05 for all). No difference was observed in the demographic and clinical features of patients with single heterozygous pathogenic mutation and pathogenic/VUS complex heterozygous variant (p > 0.05 for all). ISSF and ADDI scores were lower in pathogenic/VUS complex heterozygous patients than those harboring single pathogenic mutation (p = 0.006 and 0.004, respectively).
CONCLUSION
Our findings suggest that patients with single heterozygous VUS has mild FMF phenotype similar to those with single pathogenic mutation. Pathogenic/VUS complex heterozygosity does not lead to a more severe clinical phenotype than having a single pathogenic variant.
背景/目的:家族性地中海热(FMF)是遗传性自炎症性疾病的原型,由位于 16 号染色体短臂上的 MEFV 基因突变引起。虽然一些 MEFV 变体显然与疾病表型相关,但也有许多变体与临床关联不明,被称为意义未明的变体(VUS)。在这里,我们展示了来自位于安纳托利亚中部的三个三级中心的大型成年 FMF 患者队列中 VUS 的临床相关性。
材料和方法
所有患者均来自安纳托利亚中部的 FMF(FiCA)队列。比较 VUS 患者与携带致病性变异的患者的人口统计学(性别、发病年龄)和临床特征(疾病特征、发作频率、平均秋水仙碱剂量、秋水仙碱无反应性、淀粉样变性和持续炎症)。使用国际 FMF 严重程度评分(ISSF)和自身炎症性疾病损伤指数(ADDI)分别评估疾病的严重程度和损伤。
结果
在纳入的 971 名参与者中,有 814 名患者可进行 MEFV 基因分析。26 名(3.2%)患者存在单一杂合 VUS,54 名(6.6%)患者存在致病性/VUS 复合杂合变异。与携带单一杂合致病性变异的患者相比,单一杂合 VUS 患者具有相似的人口统计学/临床特征、ISSF 和 ADDI 评分(p > 0.05)。携带单一杂合致病性突变和致病性/VUS 复合杂合变异的患者的人口统计学和临床特征无差异(p > 0.05)。与携带单一致病性突变的患者相比,致病性/VUS 复合杂合患者的 ISSF 和 ADDI 评分较低(p = 0.006 和 0.004)。
结论
我们的研究结果表明,携带单一杂合 VUS 的患者具有与携带单一致病性突变相似的轻度 FMF 表型。致病性/VUS 复合杂合性并不导致比携带单一致病性变异更严重的临床表型。
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