| Literature DB >> 26486472 |
Ali Abdullah Alfaiz1,2,3, Verena Müller4, Nadia Boutry-Kryza5,6,7, Dorothée Ville8, Nicolas Guex1,2, Julitta de Bellescize9, Clotilde Rivier10, Audrey Labalme5, Vincent des Portes6,8, Patrick Edery5,6,7, Marianne Till5, Ioannis Xenarios1,2, Damien Sanlaville5,6,7, Johannes M Herrmann4, Gaétan Lesca5,6,7, Alexandre Reymond1.
Abstract
West syndrome (WS), defined by the triad of infantile spasms, pathognomonic hypsarrhythmia and developmental regression, is a rare epileptic disease affecting about 1:3500 live births. To get better insights on the genetic of this pathology, we exome-sequenced the members of a consanguineous family affected with isolated WS. We identified a homozygous variant (c.1825G>T/p.(Ala609Ser)) in the GUF1 gene in the three affected siblings. GUF1 encodes a protein essential in conditions that counteract faithful protein synthesis: it is able to remobilize stuck ribosomes and transiently inhibit the elongation process to optimize protein synthesis. The variant identified in the WS family changes an alanine residue conserved in all eukaryotic organisms and positioned within the tRNA-binding moiety of this nuclear genome-encoded mitochondrial translational elongation factor. Yeast complementation assays show that the activity of GUF1(A609S) is modified in suboptimal environments. We suggest a new link between improper assembly of respiratory chain complexes and WS.Entities:
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Year: 2015 PMID: 26486472 PMCID: PMC5070883 DOI: 10.1038/ejhg.2015.227
Source DB: PubMed Journal: Eur J Hum Genet ISSN: 1018-4813 Impact factor: 4.246