Department of Dermatology, Tel Aviv Sourasky Medical Center, Tel Aviv, Israel.
Am J Med Genet A. 2013 Sep;161A(9):2204-15. doi: 10.1002/ajmg.a.36059. Epub 2013 Aug 5.
3-Methylglutaconic aciduria (3-MGCA) type IV is defined as a heterogeneous group of inborn errors featuring in common 3-MGCA and associated with primary mitochondrial dysfunction leading to a spectrum of multisystem conditions. We studied four patients who presented at birth with a clinical picture simulating a primary mitochondrial hepatic disorder consistent with the MEGDEL syndrome including 3-MGCA, sensorineural deafness, encephalopathy and a brain magnetic resonance imaging with signs of Leigh disease. All affected children displayed biochemical features consistent with mitochondrial OXPHOS dysfunction including hepatic mitochondrial DNA depletion in one patient. Homozygosity mapping identified a candidate locus on 6q25.2-6q26. Using whole exome sequencing, we identified two novel homozygous mutations in SERAC1 recently reported to harbor mutations in MEGDEL syndrome. Both mutations were found to lead to decreased or absent expression of SERAC1. The present findings indicate that infantile hepatopathy is a cardinal feature of MEGDEL syndrome. We thus propose to rename the disease MEGDHEL syndrome.
3-甲基戊烯二酸尿症(3-MGCA)IV 型被定义为一组异质性的先天性遗传疾病,其共同特征是 3-MGCA 和与原发性线粒体功能障碍相关,导致一系列多系统疾病。我们研究了 4 名患者,他们在出生时表现出类似于原发性线粒体肝脏疾病的临床特征,符合 MEGDEL 综合征,包括 3-MGCA、感觉神经性耳聋、脑病和磁共振成像显示 Leigh 病的脑征象。所有受影响的儿童均表现出与线粒体 OXPHOS 功能障碍一致的生化特征,包括 1 名患者的肝线粒体 DNA 耗竭。纯合子作图确定了 6q25.2-6q26 上的一个候选位点。使用全外显子组测序,我们在 SERAC1 中发现了两个最近报道在 MEGDEL 综合征中存在突变的新的纯合突变。这两种突变都导致 SERAC1 的表达减少或缺失。目前的发现表明婴儿期肝病变是 MEGDEL 综合征的主要特征。因此,我们建议将该疾病重新命名为 MEGDHEL 综合征。
