Genotype–phenotype correlation and treatment effects in young patients withGNAO1-associated disorders

脑深部刺激 张力减退 肌张力障碍 医学 运动障碍 儿科 癫痫 表型 内科学 精神科 遗传学 疾病 生物 帕金森病 基因
作者
M. Thiel,Daniel Bamborschke,Wibke G. Janzarik,Birgit Assmann,Simone Zittel,Steffi Patzer,Andrea Auhuber,Joachim Opp,Eva Matzker,Andrea Bevot,Juergen Seeger,Andreas van Baalen,Burkhard Stüve,Knut Brockmann,Sebahattin Çırak,Anne Koy
出处
期刊:Journal of Neurology, Neurosurgery, and Psychiatry [BMJ]
卷期号:94 (10): 806-815 被引量:4
标识
DOI:10.1136/jnnp-2022-330261
摘要

Patients carrying pathogenic variants in GNAO1 often present with early-onset central hypotonia and global developmental delay, with or without epilepsy. As the disorder progresses, a complex hypertonic and hyperkinetic movement disorder is a common phenotype. A genotype-phenotype correlation has not yet been described and there are no evidence-based therapeutic recommendations.To improve understanding of the clinical course and pathophysiology of this ultra-rare disorder, we built up a registry for GNAO1 patients in Germany. In this retrospective, multicentre cohort study, we collected detailed clinical data, treatment effects and genetic data for 25 affected patients.The main clinical features were symptom onset within the first months of life, with central hypotonia or seizures. Within the first year of life, nearly all patients developed a movement disorder comprising dystonia (84%) and choreoathetosis (52%). Twelve (48%) patients suffered life-threatening hyperkinetic crises. Fifteen (60%) patients had epilepsy with poor treatment response. Two patients showed an atypical phenotype and seven novel pathogenic variants in GNAO1 were identified. Nine (38%) patients were treated with bilateral deep brain stimulation of the globus pallidus internus. Deep brain stimulation reduced hyperkinetic symptoms and prevented further hyperkinetic crises. The in silico prediction programmes did not predict the phenotype by the genotype.The broad clinical spectrum and genetic findings expand the phenotypical spectrum of GNAO1-associated disorder and therefore disprove the assumption that there are only two main phenotypes. No specific overall genotype-phenotype correlation was identified. We highlight deep brain stimulation as a useful treatment option in this disorder.
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