Department of Immunology, Genetics and Pathology, Uppsala University, Science for Life Laboratory, Uppsala, Sweden.
Department of Pathology and Cytology, Uppsala University Hospital, Uppsala, Sweden.
Clin Genet. 2017 Nov;92(5):510-516. doi: 10.1111/cge.13012. Epub 2017 May 3.
Mutations in genes involved in the cilium-centrosome complex are called ciliopathies. Meckel-Gruber syndrome (MKS) is a ciliopathic lethal autosomal recessive syndrome characterized by genetically and clinically heterogeneous manifestations, including renal cystic dysplasia, occipital encephalocele and polydactyly. Several genes have previously been associated with MKS and MKS-like phenotypes, but there are still genes remaining to be discovered. We have used whole-exome sequencing (WES) to uncover the genetics of a suspected autosomal recessive Meckel syndrome phenotype in a family with 2 affected fetuses. RNA studies and histopathological analysis was performed for further delineation. WES lead to identification of a homozygous nonsense mutation c.256C>T (p.Arg86*) in CEP55 (centrosomal protein of 55 kDa) in the affected fetus. The variant has previously been identified in carriers in low frequencies, and segregated in the family. CEP55 is an important centrosomal protein required for the mid-body formation at cytokinesis. Our results expand the list of centrosomal proteins implicated in human ciliopathies and provide evidence for an essential role of CEP55 during embryogenesis and development of disease.
与纤毛-中心体复合物相关基因的突变称为纤毛病。Meckel-Gruber 综合征(MKS)是一种纤毛病致死性常染色体隐性综合征,其特征为遗传和临床表现多样,包括肾囊性发育不良、枕部脑膨出和多指(趾)畸形。先前已有多个基因与 MKS 和 MKS 样表型相关联,但仍有一些基因有待发现。我们使用全外显子组测序(WES)发现了一个具有疑似常染色体隐性 Meckel 综合征表型的家族中 2 个受影响胎儿的遗传学特征。进行了 RNA 研究和组织病理学分析以进一步阐明。WES 导致在受影响的胎儿中鉴定出 CEP55(55 kDa 中心体蛋白)中的纯合无义突变 c.256C>T(p.Arg86*)。该变体以前在携带者中以低频率被识别,并在家族中分离。CEP55 是一种重要的中心体蛋白,对于细胞分裂过程中的中体形成是必需的。我们的结果扩展了参与人类纤毛病的中心体蛋白列表,并为 CEP55 在胚胎发生和疾病发展过程中的重要作用提供了证据。
