Mutations in NONO lead to syndromic intellectual disability and inhibitory synaptic defects

Dennis Mircsof,Maéva Langouët,Marlène Rio,Sébastien Moutton,Karine Siquier-Pernet,Christine Bole-Feysot,Nicolas Cagnard,Patrick Nitschke,Ludmila Gaspar,Matej Znidaric,Olivier Alibeu,Ann-Kristina Fritz,David P. Wolfer,Aileen Schröter,Giovanna Bosshard,Markus Rudin,Christina Koester,Florence Crestani,Petra Seebeck,Nathalie Boddaert,Katrina Prescott,Rochelle M. Hines,Steven J. Moss,Jean-Marc Fritschy,Arnold Munnich,Jeanne Amiel,Steven A. Brown,Shiva K. Tyagarajan,Laurence Colleaux

Mutations in NONO lead to syndromic intellectual disability and inhibitory synaptic defects

2015

The NONO protein has been characterized as an important transcriptional regulator in diverse cellular contexts. Here we show that loss of NONO function is a likely cause of human intellectual disability and that NONO-deficient mice have cognitive and affective deficits. Correspondingly, we find specific defects at inhibitory synapses, where NONO regulates synaptic transcription and gephyrin scaffold structure. Our data identify NONO as a possible neurodevelopmental disease gene and highlight the key role of the DBHS protein family in functional organization of GABAergic synapses.

Keywords:

Neuroscience
Cellular neuroscience
Gephyrin
Synapse
Protein family
Genetics
Intellectual disability
Mutation
Transcriptional regulation
Biology
Inhibitory postsynaptic potential

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