| Literature DB >> 29878067 |
Jean Chemin1,2, Karine Siquier-Pernet3,4, Michaël Nicouleau3,4, Giulia Barcia3,4, Ali Ahmad1,2, Daniel Medina-Cano3,4, Sylvain Hanein5, Nami Altin3,4, Laurence Hubert5, Christine Bole-Feysot6, Cécile Fourage7,8, Patrick Nitschké7, Julien Thevenon9, Marlène Rio4,8, Pierre Blanc4,8, Céline Vidal5, Nadia Bahi-Buisson3,10,11, Isabelle Desguerre3,11, Arnold Munnich3,8, Stanislas Lyonnet3,8,10, Nathalie Boddaert3,12,13, Emily Fassi14, Marwan Shinawi14, Holly Zimmerman15, Jeanne Amiel3,8,10, Laurence Faivre9, Laurence Colleaux3,4, Philippe Lory1,2, Vincent Cantagrel3,4.
Abstract
Cerebellar atrophy is a key neuroradiological finding usually associated with cerebellar ataxia and cognitive development defect in children. Unlike the adult forms, early onset cerebellar atrophies are classically described as mostly autosomal recessive conditions and the exact contribution of de novo mutations to this phenotype has not been assessed. In contrast, recent studies pinpoint the high prevalence of pathogenic de novo mutations in other developmental disorders such as intellectual disability, autism spectrum disorders and epilepsy. Here, we investigated a cohort of 47 patients with early onset cerebellar atrophy and/or hypoplasia using a custom gene panel as well as whole exome sequencing. De novo mutations were identified in 35% of patients while 27% had mutations inherited in an autosomal recessive manner. Understanding if these de novo events act through a loss or a gain of function effect is critical for treatment considerations. To gain a better insight into the disease mechanisms causing these cerebellar defects, we focused on CACNA1G, a gene not yet associated with the early-onset form. This gene encodes the Cav3.1 subunit of T-type calcium channels highly expressed in Purkinje neurons and deep cerebellar nuclei. We identified four patients with de novo CACNA1G mutations. They all display severe motor and cognitive impairment, cerebellar atrophy as well as variable features such as facial dysmorphisms, digital anomalies, microcephaly and epilepsy. Three subjects share a recurrent c.2881G>A/p.Ala961Thr variant while the fourth patient has the c.4591A>G/p.Met1531Val variant. Both mutations drastically impaired channel inactivation properties with significantly slower kinetics (∼5 times) and negatively shifted potential for half-inactivation (>10 mV). In addition, these two mutations increase neuronal firing in a cerebellar nuclear neuron model and promote a larger window current fully inhibited by TTA-P2, a selective T-type channel blocker. This study highlights the prevalence of de novo mutations in early-onset cerebellar atrophy and demonstrates that A961T and M1531V are gain of function mutations. Moreover, it reveals that aberrant activity of Cav3.1 channels can markedly alter brain development and suggests that this condition could be amenable to treatment.Entities:
Mesh:
Substances:
Year: 2018 PMID: 29878067 DOI: 10.1093/brain/awy145
Source DB: PubMed Journal: Brain ISSN: 0006-8950 Impact factor: 13.501