| Literature DB >> 26688339 |
Xènia Ferrer-Cortès1, Juan Narbona2, Núria Bujan1, Leslie Matalonga1, Mireia Del Toro3, José Antonio Arranz3, Encarnació Riudor3, Angels Garcia-Cazorla4, Cristina Jou4, Mar O'Callaghan4, Mercé Pineda4, Raquel Montero4, Angela Arias1, Judit García-Villoria1, Charlotte L Alston5, Robert W Taylor5, Paz Briones6, Antonia Ribes7, Frederic Tort8.
Abstract
Mutations in NFU1 were recently identified in patients with fatal encephalopathy. NFU1 is an iron-sulfur cluster protein necessary for the activity of the mitochondrial respiratory chain complexes I-II and the synthesis of lipoic acid. We report two NFU1 compound heterozygous individuals with normal complex I and lipoic acid-dependent enzymatic activities and low, but detectable, levels of lipoylated proteins. We demonstrated a leaky splicing regulation due to a splice site mutation (c.545+5G>A) that produces small amounts of wild type NFU1 mRNA that might result in enough protein to partially lipoylate and restore the activity of lipoic acid-dependent enzymes and the assembly and activity of complex I. These results allowed us to gain insights into the molecular basis underlying this disease and should be considered for the diagnosis of NFU1 patients.Entities:
Keywords: Iron–sulfur cluster; Lipoic acid; Metabolic disorder; Mitochondrial cofactor; Mitochondrial disease; NFU1
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Year: 2015 PMID: 26688339 DOI: 10.1016/j.mito.2015.12.004
Source DB: PubMed Journal: Mitochondrion ISSN: 1567-7249 Impact factor: 4.160