| Literature DB >> 30642806 |
Tommaso Schirinzi1, Giacomo Garone2, Lorena Travaglini3, Gessica Vasco3, Serena Galosi4, Loreto Rios5, Claudia Castiglioni5, Claudia Barassi5, Domenica Battaglia6, Maria Luigia Gambardella6, Laura Cantonetti3, Federica Graziola7, Carlo Efisio Marras3, Enrico Castelli3, Enrico Bertini3, Alessandro Capuano3, Vincenzo Leuzzi4.
Abstract
GNAO1 variants were recently discovered as causes of epileptic encephalopathies and heterogeneous syndromes presenting with movement disorders (MDs), whose phenomenology and clinical course are yet undefined. We herein focused on GNAO1-related MD, providing an analytical review of existing data to outline the main MD phenomenology and management, clinical evolution and genotype-phenotype correlations. Reviewing 41 previously published patients and assessing 5 novel cases, a comprehensive cohort of 46 patients was analyzed, reassuming knowledge about genotypes, phenotypes, disease course and treatment of this condition. GNAO1-related MD consisted of a severe early-onset hyperkinetic syndrome, with prominent chorea, dystonia and orofacial dyskinesia. Symptoms are poorly responsive to medical therapy and fluctuate, with critical and life-threatening exacerbations, such as status dystonicus. The presence of a choreiform MD appears to be predictive of a higher risk of movement disorder emergency. Surgical treatments are sometimes effective, although severe disabilities persist. Differently from the early infantile epileptic encephalopathy phenotype (associated with loss of function variants), no clear correlation between genotype and MD phenotype emerged, although some variants recurred more frequently, mainly affecting exons 6 and 7.Entities:
Keywords: Children movement disorders; Chorea; Dystonia; GNAO1; Movement disorder emergencies; Status dystonicus
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Year: 2018 PMID: 30642806 DOI: 10.1016/j.parkreldis.2018.11.019
Source DB: PubMed Journal: Parkinsonism Relat Disord ISSN: 1353-8020 Impact factor: 4.891