| Literature DB >> 32005960 |
Sophie Nambot1,2,3, Laurence Faivre1,2,3, Ghayda Mirzaa4,5, Julien Thevenon1,2,3,6, Ange-Line Bruel1,2,6, Anne-Laure Mosca-Boidron1,2,6, Alice Masurel-Paulet1,3, Alice Goldenberg7, Nathalie Le Meur7, Aude Charollais8, Cyril Mignot9, Florence Petit10, Massimiliano Rossi11, Julia Metreau12, Valérie Layet13, Daniel Amram14, Odile Boute-Bénéjean10, Elizabeth Bhoj15,16, Margot A Cousin17,18, Teresa M Kruisselbrink17,19, Brendan C Lanpher17,19, Eric W Klee17,18,19, Elise Fiala20, Dorothy K Grange21, Wendy S Meschino22, Susan M Hiatt23, Gregory M Cooper23, Hilde Olivié24, Wendy E Smith25, Meghan Dumas25, Anna Lehman26, Cara Inglese26, Mathilde Nizon27, Renzo Guerrini28, Annalisa Vetro28, Eitan S Kaplan5, Dolores Miramar29, Julien Van Gils30, Patricia Fergelot31, Olaf Bodamer32, Johanna C Herkert33, Sander Pajusalu34, Katrin Õunap34, James J Filiano35, Thomas Smol36, Amélie Piton37, Bénédicte Gérard37, Sandra Chantot-Bastaraud9,38, Thierry Bienvenu39, Dong Li17, Jane Juusola40, Koen Devriendt41, Frederic Bilan42, Charlotte Poé2, Martin Chevarin2, Thibaud Jouan2, Emilie Tisserant2, Jean-Baptiste Rivière2,3,6, Frédéric Tran Mau-Them2,6, Christophe Philippe2,6, Yannis Duffourd2,6, William B Dobyns4, Robert Hevner4, Christel Thauvin-Robinet43,44,45,46.
Abstract
TBR1, a T-box transcription factor expressed in the cerebral cortex, regulates the expression of several candidate genes for autism spectrum disorders (ASD). Although TBR1 has been reported as a high-confidence risk gene for ASD and intellectual disability (ID) in functional and clinical reports since 2011, TBR1 has only recently been recorded as a human disease gene in the OMIM database. Currently, the neurodevelopmental disorders and structural brain anomalies associated with TBR1 variants are not well characterized. Through international data sharing, we collected data from 25 unreported individuals and compared them with data from the literature. We evaluated structural brain anomalies in seven individuals by analysis of MRI images, and compared these with anomalies observed in TBR1 mutant mice. The phenotype included ID in all individuals, associated to autistic traits in 76% of them. No recognizable facial phenotype could be identified. MRI analysis revealed a reduction of the anterior commissure and suggested new features including dysplastic hippocampus and subtle neocortical dysgenesis. This report supports the role of TBR1 in ID associated with autistic traits and suggests new structural brain malformations in humans. We hope this work will help geneticists to interpret TBR1 variants and diagnose ASD probands.Entities:
Mesh:
Substances:
Year: 2020 PMID: 32005960 PMCID: PMC7253452 DOI: 10.1038/s41431-020-0571-6
Source DB: PubMed Journal: Eur J Hum Genet ISSN: 1018-4813 Impact factor: 4.246