| Literature DB >> 31184778 |
Eszter Vojcek1, Tália Magdolna Keszthelyi1,2, Eszter Jávorszky1,2, Lídia Balogh1, Kálmán Tory1,2.
Abstract
We report on a sibling pair with the EPG5 c.1007A > G mutation who developed a severe form of Vici syndrome and died in infancy. The c.1007A > G (p.Gln336Arg) mutation, affecting the penultimate nucleotide and the splicing of exon 2 is the most common mutation of EPG5 and is typically associated with a less devastating prognosis: cardiomyopathy and cataract are less frequent consequences and the median survival time is 78 months compared to an overall median survival of 42 months. The less severe course related to c.1007A > G was formerly explained by the preserved canonical splicing in 25% of the transcripts. In contrast, we found the messenger RNA encoded by the c.1007A > G allele to be absent, explaining the severe course of the disease. This family provides another example of phenotypic variability related to a differential splicing.Entities:
Keywords: Gln336Arg; Vici syndrome; differential splicing; phenotype variability
Year: 2019 PMID: 31184778 DOI: 10.1111/ahg.12337
Source DB: PubMed Journal: Ann Hum Genet ISSN: 0003-4800 Impact factor: 1.670