Migliavacca Michele P, Sobreira Nara L M, Antonialli Graziela P M, Oliveira Mariana M, Melaragno Maria Isabel S A, Casteels Ingele, de Ravel Thomy, Brunoni Decio, Valle David, Perez Ana Beatriz A
Clinical Genetics, Department of Morphology and Genetics, UNIFESP, São Paulo, Brazil.
Am J Med Genet A. 2014 May;164A(5):1170-4. doi: 10.1002/ajmg.a.36425. Epub 2014 Jan 29.
Van den Ende-Gupta Syndrome (VDEGS) is an autosomal recessive disorder characterized by blepharophimosis, distinctive nose, hypoplastic maxilla, and skeletal abnormalities. Using homozygosity mapping in four VDEGS patients from three consanguineous families, Anastacio et al. [Anastacio et al. (2010); Am J Hum Genet 87:553-559] identified homozygous mutations in SCARF2, located at 22q11.2. Bedeschi et al. [2010] described a VDEGS patient with sclerocornea and cataracts with compound heterozygosity for the common 22q11.2 microdeletion and a hemizygous SCARF2 mutation. Because sclerocornea had been described in DiGeorge-velo-cardio-facial syndrome but not in VDEGS, they suggested that the ocular abnormalities were caused by the 22q11.2 microdeletion. We report on a 23-year-old male who presented with bilateral sclerocornea and the VDGEGS phenotype who was subsequently found to be homozygous for a 17 bp deletion in exon 4 of SCARF2. The occurrence of bilateral sclerocornea in our patient together with that of Bedeschi et al., suggests that the full VDEGS phenotype may include sclerocornea resulting from homozygosity or compound heterozygosity for loss of function variants in SCARF2.
范登恩德 - 古普塔综合征(VDEGS)是一种常染色体隐性疾病,其特征为睑裂狭小、独特的鼻子、上颌骨发育不全和骨骼异常。阿纳斯塔西奥等人[阿纳斯塔西奥等人(2010年);《美国人类遗传学杂志》87:553 - 559]通过对来自三个近亲家庭的四名VDEGS患者进行纯合性定位,在位于22q11.2的SCARF2中鉴定出纯合突变。贝德斯基等人[2010年]描述了一名患有角膜硬化和白内障的VDEGS患者,该患者对于常见的22q11.2微缺失为复合杂合子,且存在半合子SCARF2突变。由于角膜硬化已在迪乔治 - 心 - 面综合征中被描述,但在VDEGS中未被描述,他们认为眼部异常是由22q11.2微缺失引起的。我们报告了一名23岁男性,他患有双侧角膜硬化和VDGEGS表型,随后被发现SCARF2外显子4中存在一个17 bp缺失的纯合子。我们的患者以及贝德斯基等人的患者中双侧角膜硬化的出现表明,完整的VDEGS表型可能包括由于SCARF2功能丧失变体的纯合性或复合杂合性导致的角膜硬化。
