| Literature DB >> 26675814 |
Elham Jaberi1, Mohammad Rohani2, Gholam Ali Shahidi2, Shahriar Nafissi3, Ehsan Arefian1, Masoud Soleimani4, Paniz Rasooli1, Hamid Ahmadieh5, Narsis Daftarian6, Mohammad KaramiNejadRanjbar7, Brandy Klotzle8, Jian-Bing Fan8, Casey Turk8, Frank Steemers8, Elahe Elahi9.
Abstract
We aimed to identify the genetic cause of a neurologic disorder accompanied with mental deficiency in a consanguineous family with 3 affected siblings by linkage analysis and exome sequencing. Iron accumulation in the brain of the patients was a notable phenotypic feature. A full-field electroretinography revealed generalized dysfunction of photoreceptors, bipolar cells, and amacrine cells. A splice site mutation in GTPBP2 that encodes GTP-binding protein 2 was identified in the patients and considered possible cause of their disease. The mutation was empirically shown to cause deletion of exon 9 of the gene and result in production of a truncated protein-lacking conserved C-terminus domains. GTPBP2 is a member of the GTPase superfamily of proteins. A recent report of identification of another splice site mutation in GTPBP2 in mice that causes neurodegeneration, and retinal damage provides supportive evidence for our finding. The conditions in the affected individuals of the family studied may define a novel form of neurodegeneration with brain iron accumulation, and GTPBP2 may be a novel neurodegeneration with brain iron accumulation gene.Entities:
Keywords: Ataxia; Cognitive dysfunction; Exome sequencing; GTPBP2; NBIA; Neurodegenerative disease
Mesh:
Substances:
Year: 2015 PMID: 26675814 DOI: 10.1016/j.neurobiolaging.2015.10.034
Source DB: PubMed Journal: Neurobiol Aging ISSN: 0197-4580 Impact factor: 4.673