Doğancı Tümay, Yüksel Konuk Berrin E, Alpan Nursel, Konuk Onur, Hämäläinen Riikka H, Lehesjoki Anna-Elina, Tekin Mustafa
Pediatric Gastroenterology Unit Pediatric Cardiology Unit, Dışkapı Children's Hospital Division of Pediatric Genetics, Ankara University School of Medicine Department of Ophthalmology, Gazi University School of Medicine, Ankara, Turkey Folkhälsan Institute of Genetics and Neuroscience Center, University of Helsinki, Helsinki, Finland.
Clin Dysmorphol. 2007 Jul;16(3):173-176. doi: 10.1097/MCD.0b013e3280f6d00b.
Mulibrey nanism is a rare autosomal-recessive disorder characterized by prenatal onset severe growth retardation and pericardial constriction associated with abnormalities of muscle, liver, brain and eye. More than 80% of previously reported patients are of Finnish origin in whom a founder mutation in the TRIM37 gene have been described. We report on a 7-year-old Turkish boy who presented with classical phenotypic features of mulibrey nanism. Mutation screening of the TRIM37 gene revealed that the proband had a homozygous two base pair deletion, c.1894_1895delGA, resulting in a frame-shift and a premature termination codon. Our proband is one of the rare examples of mulibrey nanism outside Finland and extends the mutation spectrum in this disorder.
穆利布瑞侏儒症是一种罕见的常染色体隐性疾病,其特征为产前起病的严重生长发育迟缓以及与肌肉、肝脏、脑和眼异常相关的心包缩窄。既往报道的患者中超过80%来自芬兰,在这些患者中已发现TRIM37基因的奠基者突变。我们报告了一名7岁的土耳其男孩,他具有穆利布瑞侏儒症的典型表型特征。对TRIM37基因进行突变筛查发现,先证者存在纯合的两个碱基对缺失,即c.1894_1895delGA,导致移码和提前终止密码子。我们的先证者是芬兰以外穆利布瑞侏儒症的罕见病例之一,扩展了该疾病的突变谱。