Afficher la couverture 'Copy number variants in patients with intellectual disability affect the regulation of ARX transcription factor gene. | Ishibashi, Minaka' en grand format
/5

0 avis

Copy number variants in patients with intellectual disability affect the regulation of ARX transcription factor gene.

Archive ouverte

Ishibashi, Minaka | Manning, Elizabeth | Shoubridge, Cheryl | Krecsmarik, Monika | Hawkins, Thomas A | Giacomotto, Jean | Zhao, Ting | Mueller, Thomas | Bader, Patricia I | Cheung, Sau W | Stankiewicz, Pawel | Bain, Nicole L | Hackett, Anna | Reddy, Chilamakuri C S | Mechaly, Alejandro S | Peers, Bernard | Wilson, Stephen W | Lenhard, Boris | Bally-Cuif, Laure | Gecz, Jozef | Becker, Thomas S | Rinkwitz, Silke

Edité par CCSD ; Springer Verlag -

International audience. Protein-coding mutations in the transcription factor-encoding gene ARX cause various forms of intellectual disability (ID) and epilepsy. In contrast, variations in surrounding non-coding sequences are correlated with milder forms of non-syndromic ID and autism and had suggested the importance of ARX gene regulation in the etiology of these disorders. We compile data on several novel and some already identified patients with or without ID that carry duplications of ARX genomic region and consider likely genetic mechanisms underlying the neurodevelopmental defects. We establish the long-range regulatory domain of ARX and identify its brain region-specific autoregulation. We conclude that neurodevelopmental disturbances in the patients may not simply arise from increased dosage due to ARX duplication. This is further exemplified by a small duplication involving a non-functional ARX copy, but with duplicated enhancers. ARX enhancers are located within a 504-kb region and regulate expression specifically in the forebrain in developing and adult zebrafish. Transgenic enhancer-reporter lines were used as in vivo tools to delineate a brain region-specific negative and positive autoregulation of ARX. We find autorepression of ARX in the telencephalon and autoactivation in the ventral thalamus. Fluorescently labeled brain regions in the transgenic lines facilitated the identification of neuronal outgrowth and pathfinding disturbances in the ventral thalamus and telencephalon that occur when arxa dosage is diminished. In summary, we have established a model for how breakpoints in long-range gene regulation alter the expression levels of a target gene brain region-specifically, and how this can cause subtle neuronal phenotypes relating to the etiology of associated neuropsychiatric disease.

Consulter en ligne

Suggestions

Du même auteur

Long-range evolutionary constraints reveal cis-regulatory interactions on the human X chromosome.

Archive ouverte | Naville, Magali | CCSD

International audience. Enhancers can regulate the transcription of genes over long genomic distances. This is thought to lead to selection against genomic rearrangements within such regions that may disrupt this fu...

A systematic, large-scale resequencing screen of X-chromosome coding exons in mental retardation

Archive ouverte | Tarpey, Patrick S. | CCSD

International audience. Large-scale systematic resequencing has been proposed as the key future strategy for the discovery of rare, disease-causing sequence variants across the spectrum of human complex disease. We ...

Chemical genetics unveils a key role of mitochondrial dynamics, cytochrome c release and IP3R activity in muscular dystrophy.

Archive ouverte | Giacomotto, Jean | CCSD

International audience. Duchenne muscular dystrophy (DMD) is a neuromuscular disease caused by mutations in the dystrophin gene. The subcellular mechanisms of DMD remain poorly understood and there is currently no c...

Chargement des enrichissements...