| Literature DB >> 26920903 |
Juliette Bouchereau1, Sandrine Vuillaumier Barrot2,3, Thierry Dupré2,3, Stuart E H Moore3, Ruxandra Cardas4, Yline Capri5, Pauline Gaignard6, Abdelhamid Slama6, Catherine Delanoë7, Hélène Ogier de Baulny1, Nathalie Seta2, Manuel Schiff1,8, Laurent Servais9.
Abstract
The C10orf2 gene encodes Twinkle, a protein involved in mitochondrial DNA (mtDNA) replication. Twinkle mutations cause mtDNA deletion or depletion and are associated with a large spectrum of clinical symptoms including dominant progressive external ophthalmoplegia (adPEO), infantile-onset spinocerebellar ataxia (IOSCA), and early-onset encephalopathy. The diagnosis remains difficult because of the wide range of symptoms and lack of association with specific metabolic changes. We report herein a child with early-onset encephalopathy, unusual abnormal movements, deafness, and axonal neuropathy. All laboratory investigations were normal with the exceptions of high alpha-fetoprotein levels and an abnormal glycosylation profile. These abnormal parameters resulted in misdiagnosis as a previously unidentified congenital disorder of glycosylation (CDG) type I syndrome. Whole exome sequencing revealed two point mutations in C10orf2 that were confirmed by Sanger sequencing; neither had been previously reported. This report enlarges the clinical phenotype of Twinkle mutations and suggests that an abnormal glycosylation profile suggestive of CDG type I associated with high blood alpha-fetoprotein levels without obvious cause should prompt Twinkle sequencing.Entities:
Year: 2016 PMID: 26920903 PMCID: PMC5059178 DOI: 10.1007/8904_2016_526
Source DB: PubMed Journal: JIMD Rep ISSN: 2192-8304