King's College London, Department of Medical & Molecular Genetics, School of Medicine, Guy's Hospital, London, United Kingdom.
Hum Mutat. 2011 Feb;32(2):231-9. doi: 10.1002/humu.21413.
Dyggve-Melchior-Clausen syndrome (DMC), a severe autosomal recessive skeletal disorder with mental retardation, is caused by mutation of the gene encoding Dymeclin (DYM). Employing patient fibroblasts with mutations characterized at the genomic and, for the first time, transcript level, we identified profound disruption of Golgi organization as a pathogenic feature, resolved by transfection of heterologous wild-type Dymeclin. Collagen targeting appeared defective in DMC cells leading to near complete absence of cell surface collagen fibers. DMC cells have an elevated apoptotic index (P< 0.01) likely due to a stress response contingent upon Golgi-related trafficking defects. We performed spatiotemporal mapping of Dymeclin expression in zebrafish embryos and identified high levels of transcript in brain and cartilage during early development. Finally, in a chondrocyte cDNA library, we identified two novel secretion pathway proteins as Dymeclin interacting partners: GOLM1 and PPIB. Together these data identify the role of Dymeclin in secretory pathways essential to endochondral bone formation during early development.
狄格夫-梅尔乔尔-克劳斯综合征(DMC)是一种严重的常染色体隐性骨骼疾病,伴有智力迟钝,是由编码 Dymeclin(DYM)的基因突变引起的。我们利用具有基因组和首次在转录本水平上特征化突变的患者成纤维细胞,鉴定出高尔基体组织严重破坏是一种致病特征,通过转染异源野生型 Dymeclin 可得到纠正。在 DMC 细胞中胶原靶向似乎存在缺陷,导致细胞表面胶原纤维几乎完全缺失。DMC 细胞的凋亡指数升高(P<0.01),可能是由于高尔基体相关运输缺陷引起的应激反应所致。我们在斑马鱼胚胎中进行了 Dymeclin 表达的时空图谱绘制,并在早期发育过程中在大脑和软骨中鉴定到高水平的转录物。最后,在软骨细胞 cDNA 文库中,我们鉴定出两种新型分泌途径蛋白作为 Dymeclin 的相互作用伙伴:GOLM1 和 PPIB。这些数据共同确定了 Dymeclin 在早期发育过程中对软骨内骨形成至关重要的分泌途径中的作用。
