Department of Prosthodontics, Peking University School and Hospital of Stomatology, National Clinical Research Center for Oral Diseases, National Engineering Laboratory for Digital and Material Technology of Stomatology, Beijing Key Laboratory of Digital Stomatology, Beijing, China.
Division of Comprehensive Oral Health, Periodontology Program, Adams School of Dentistry, University of North Carolina, Chapel Hill, North Carolina, USA.
Hum Mutat. 2020 Nov;41(11):1957-1966. doi: 10.1002/humu.24104. Epub 2020 Sep 16.
Nonsyndromic oligodontia is a rare congenital anomaly. Mutations in the ectodysplasin A receptor (EDAR) gene are the primary cause of hypohidrotic ectodermal dysplasia but are rarely reported in nonsyndromic oligodontia. This study investigated EDAR mutations in multiplex nonsyndromic oligodontia and comparatively analyzed the EDAR- and EDA-related tooth agenesis patterns. Mutation screening was carried out using whole-exome sequencing and familial segregation. Evolutionary conservation and conformational analyses were used to evaluate the potential pathogenic influence of EDAR mutants. EDAR mutations were found to occur in 10.7% of nonsyndromic oligodontia cases. We reported seven heterozygous mutations of EDAR, including five novel mutations (c.404G>A, c.871G>A, c.43G>A, c.1072C>T, and c.1109T>C) and two known mutations (c.319A>G and c.1138A>C). Genotype-phenotype correlation analysis demonstrated that the EDAR-related tooth agenesis pattern was markedly different from EDA. The mandibular second premolars were most frequently missing (57.69%) in EDAR-mutated patients. Our results provide new evidence for the genotypic study of nonsyndromic oligodontia and suggest that EDAR haploinsufficiency results in nonsyndromic tooth agenesis. Furthermore, the distinct pattern between EDAR- and EDA-related tooth agenesis can be used as a guide for mutation screening during the clinical genetic diagnosis of this genetic disorder.
非综合征性少牙症是一种罕见的先天性异常。外胚层发育不全 A 受体(EDAR)基因突变是少汗型外胚层发育不全的主要原因,但在非综合征性少牙症中很少报道。本研究调查了多例非综合征性少牙症中 EDAR 基因突变,并比较分析了 EDAR 和 EDA 相关牙齿缺失模式。采用全外显子组测序和家族分离进行突变筛查。利用进化保守性和构象分析来评估 EDAR 突变体的潜在致病影响。发现 EDAR 突变发生在 10.7%的非综合征性少牙症病例中。我们报道了 EDAR 的七个杂合突变,包括五个新突变(c.404G>A、c.871G>A、c.43G>A、c.1072C>T 和 c.1109T>C)和两个已知突变(c.319A>G 和 c.1138A>C)。基因型-表型相关性分析表明,EDAR 相关的牙齿缺失模式与 EDA 明显不同。EDAR 突变患者下颌第二前磨牙缺失最常见(57.69%)。我们的研究结果为非综合征性少牙症的基因研究提供了新的证据,并表明 EDAR 单倍不足导致非综合征性牙齿缺失。此外,EDAR 和 EDA 相关牙齿缺失之间的明显模式可作为该遗传疾病临床基因诊断中突变筛查的指导。
