Le Caignec C, Lefevre M, Schott J J, Chaventre A, Gayet M, Calais C, Moisan J P
Laboratoire d'Etude du Polymorphisme de l'ADN, Faculté de Médecine, Nantes, France.
Am J Hum Genet. 2002 Jul;71(1):180-6. doi: 10.1086/341327. Epub 2002 May 17.
In the present study, we report a kindred with hearing loss, congenital heart defects, and posterior embryotoxon, segregating as autosomal dominant traits. Six of seven available affected patients manifested mild-to-severe combined hearing loss, predominantly affecting middle frequencies. Two patients were diagnosed with vestibular pathology. All patients had congenital heart defects, including tetralogy of Fallot, ventricular septal defect, or isolated peripheral pulmonic stenosis. No individual in this family met diagnostic criteria for any previously described clinical syndrome. A candidate-gene approach was undertaken and culminated in the identification of a novel Jagged 1 (JAG1) missense mutation (C234Y) in the first cysteine of the first epidermal-growth-factor-like repeat domain of the protein. JAG1 is a cell-surface ligand in the Notch signaling pathway. Mutations in JAG1 have been identified in patients with Alagille syndrome. Our findings revealed a unique phenotype with highly penetrant deafness, posterior embryotoxon, and congenital heart defects but with variable expressivity in a large kindred, which demonstrates that mutation in JAG1 can cause hearing loss.
在本研究中,我们报告了一个患有听力损失、先天性心脏缺陷和后胚胎毒素的家族,这些症状以常染色体显性性状分离。7名现有的受影响患者中有6名表现出轻度至重度的混合性听力损失,主要影响中频。2名患者被诊断出患有前庭病变。所有患者都有先天性心脏缺陷,包括法洛四联症、室间隔缺损或孤立性外周肺动脉狭窄。该家族中没有个体符合任何先前描述的临床综合征的诊断标准。我们采用了候选基因方法,最终在该蛋白第一个表皮生长因子样重复结构域的第一个半胱氨酸中鉴定出一种新的锯齿状蛋白1(JAG1)错义突变(C234Y)。JAG1是Notch信号通路中的一种细胞表面配体。在阿拉吉列综合征患者中已鉴定出JAG1的突变。我们的研究结果揭示了一种独特的表型,具有高度外显的耳聋、后胚胎毒素和先天性心脏缺陷,但在一个大家族中具有可变的表现度,这表明JAG1突变可导致听力损失。
