| Literature DB >> 30268909 |
Nancy Vegas1, Mara Cavallin1, Tjitske Kleefstra2, Lonneke de Boer3, Marion Philbert1, Camille Maillard4, Nathalie Boddaert5, Arnold Munnich6, Laurence Hubert7, Amandine Bery4, Claude Besmond7, Nadia Bahi-Buisson8.
Abstract
The advent of next generation sequencing has improved gene discovery in neurodevelopmental disorders. A greater understanding of the genetic basis of these disorders has expanded the spectrum of pathogenic genes, thus enhancing diagnosis and therapeutic management. Genetic overlap between distinct neurodevelopmental disorders has also been revealed, which can make determining a strict genotype-phenotype correlation more difficult. Intellectual disability and cortical malformations are two neurodevelopmental disorders particularly confronted by this difficulty. Indeed, for a given pathogenic gene, intellectual disability can be associated, or not, with cortical malformations. Here, we report for the first time, two individuals with the same de novo mutation in TBR1, leading to a frameshift starting at codon Thr532, and resulting in a premature stop codon 143 amino acids downstream (c.1588_1594dup, p.(Thr532Argfs*144)). These individuals presented with a developmental encephalopathy characterized by frontal pachygyria and severe intellectual disability. Remarkably, 11 TBR1 gene mutations were previously reported in intellectual disability and autism spectrum disorders. Our study supports the observation that TBR1-related disorders range from intellectual disability to frontal pachygyria. We also highlight the need for first-line, good quality neuroimaging for patients with intellectual disability.Entities:
Keywords: Autistic spectrum disorder; Cortical malformation; Developmental delay; Intellectual disability; Neurodevelopmental disorder; TBR1
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Year: 2018 PMID: 30268909 DOI: 10.1016/j.ejmg.2018.09.012
Source DB: PubMed Journal: Eur J Med Genet ISSN: 1769-7212 Impact factor: 2.708