Baala Lekbir, Audollent Sophie, Martinovic Jéléna, Ozilou Catherine, Babron Marie-Claude, Sivanandamoorthy Sivanthiny, Saunier Sophie, Salomon Rémi, Gonzales Marie, Rattenberry Eleanor, Esculpavit Chantal, Toutain Annick, Moraine Claude, Parent Philippe, Marcorelles Pascale, Dauge Marie-Christine, Roume Joëlle, Le Merrer Martine, Meiner Vardiella, Meir Karen, Menez Françoise, Beaufrère Anne-Marie, Francannet Christine, Tantau Julia, Sinico Martine, Dumez Yves, MacDonald Fiona, Munnich Arnold, Lyonnet Stanislas, Gubler Marie-Claire, Génin Emmanuelle, Johnson Colin A, Vekemans Michel, Encha-Razavi Férechté, Attié-Bitach Tania
Université René Descartes et INSERM U-781, Hôpital Necker-Enfants Malades, 149 rue de Sèvres, 75743 Paris Cedex 15, France.
Am J Hum Genet. 2007 Jul;81(1):170-9. doi: 10.1086/519494. Epub 2007 Jun 4.
Meckel syndrome (MKS) is a rare autosomal recessive lethal condition characterized by central nervous system malformations, polydactyly, multicystic kidney dysplasia, and ductal changes of the liver. Three loci have been mapped (MKS1-MKS3), and two genes have been identified (MKS1/FLJ20345 and MKS3/TMEM67), whereas the gene at the MKS2 locus remains unknown. To identify new MKS loci, a genomewide linkage scan was performed using 10-cM-resolution microsatellite markers in eight families. The highest heterogeneity LOD score was obtained for chromosome 12, in an interval containing CEP290, a gene recently identified as causative of Joubert syndrome (JS) and isolated Leber congenital amaurosis. In view of our recent findings of allelism, at the MKS3 locus, between these two disorders, CEP290 was considered a candidate, and homozygous or compound heterozygous truncating mutations were identified in four families. Sequencing of additional cases identified CEP290 mutations in two fetuses with MKS and in four families presenting a cerebro-reno-digital syndrome, with a phenotype overlapping MKS and JS, further demonstrating that MKS and JS can be variable expressions of the same ciliopathy. These data identify a fourth locus for MKS (MKS4) and the CEP290 gene as responsible for MKS.
梅克尔综合征(MKS)是一种罕见的常染色体隐性致死性疾病,其特征为中枢神经系统畸形、多指(趾)畸形、多囊性肾发育不良以及肝脏导管改变。已定位了三个基因座(MKS1 - MKS3),并鉴定出两个基因(MKS1/FLJ20345和MKS3/TMEM67),而MKS2基因座上的基因仍未知。为了鉴定新的MKS基因座,我们使用10厘摩分辨率的微卫星标记对8个家系进行了全基因组连锁扫描。在12号染色体上获得了最高的异质性对数优势(LOD)分数,该区间包含CEP290基因,这是一个最近被确定为导致乔伯特综合征(JS)和孤立性莱伯先天性黑蒙病因的基因。鉴于我们最近在MKS3基因座发现这两种疾病之间存在等位性,CEP290被视为一个候选基因,并且在4个家系中鉴定出纯合或复合杂合截短突变。对其他病例的测序在两个患有MKS的胎儿以及4个表现出脑 - 肾 - 指综合征的家系中鉴定出CEP290突变,其表型与MKS和JS重叠,进一步证明MKS和JS可能是同一纤毛病的不同表现形式。这些数据确定了MKS的第四个基因座(MKS4)以及CEP290基因是MKS的致病基因。
