Neurological and psychiatric phenotype of a multicenter cohort of patients with SETD5-related neurodevelopmental disorder

IF 2.3 3区 医学 Q3 CLINICAL NEUROLOGY
Alessandro De Falco , Angela De Dominicis , Marina Trivisano , Nicola Specchio , Maria Cristina Digilio , Carmelo Piscopo , Valeria Capra , Marcello Scala , Michele Iacomino , Andrea Accogli , Ferruccio Romano , Vincenzo Salpietro , Margherita Mancardi , Pasquale Striano , Francesca Felicia Operto , Janina Gburek-Augustat , Laurence Perrin , Yline Capri , Viviana Lupo , Maurizio Elia , Gaetano Terrone
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引用次数: 0

Abstract

Pathogenic variants in the SETD5 gene cause a neurodevelopmental disorder characterized by intellectual disability, autism, and facial dysmorphisms, with incomplete penetrance. To date, no distinctive neurological, psychiatric, electroencephalographic, and neuroimaging features have been identified in this condition. We expand the clinical phenotype of SETD5-related disorder by describing 28 previously unreported patients, 26 carrying single nucleotide variants, and 2 with copy number variations involving SETD5 gene, focusing on neurological, psychiatric, EEG, and brain MRI data. In our cohort neurological symptoms include hypotonia (39.2 %), hyperkinetic movement disorders including stereotypies and chorea (21.4 %) and gait abnormalities ranging from tip-toe or unsteady walking and alterations of fine motor skills (35.7 %). Epilepsy was present in about 14 % of patients, including different types of seizures as epileptic spasms, focal motor, and non-motor seizures. Concerning the cognitive phenotype, intellectual disability or global developmental delay depending on age, ranging from mild to severe, was present in 75 % of cohort, 21.4 % exhibit borderline intellectual functioning while an individual has a normal intelligence quotient.
Other psychiatric comorbidities include autism, ADHD, psychotic disorder and other internalizing and externalizing symptoms.
Finally, we conduct a comprehensive review of the available literature, suggesting a possible genotype-phenotype correlation.
SETD5 相关神经发育障碍多中心队列患者的神经和精神表型
SETD5 基因的致病变异会导致一种神经发育障碍,其特征是智力障碍、自闭症和面部畸形,且具有不完全渗透性。迄今为止,尚未发现这种疾病在神经学、精神病学、脑电图和神经影像学方面有明显特征。我们通过描述 28 例之前未报道过的患者(其中 26 例携带单核苷酸变异,2 例涉及 SETD5 基因拷贝数变异),扩展了 SETD5 相关障碍的临床表型,重点研究了神经、精神、脑电图和脑磁共振成像数据。在我们的队列中,神经系统症状包括肌张力低下(39.2%)、过度运动障碍(包括刻板行为和舞蹈症)(21.4%)、步态异常(包括踮脚或行走不稳以及精细动作技能改变)(35.7%)。约 14% 的患者患有癫痫,包括癫痫痉挛、局灶性运动性和非运动性发作等不同类型。在认知表型方面,75%的患者存在智力障碍或全面发育迟缓(视年龄而定,从轻度到重度不等),21.4%的患者表现出边缘智力功能,而个别患者智商正常。其他精神疾病合并症包括自闭症、多动症、精神障碍以及其他内化和外化症状。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
6.30
自引率
3.20%
发文量
115
审稿时长
81 days
期刊介绍: The European Journal of Paediatric Neurology is the Official Journal of the European Paediatric Neurology Society, successor to the long-established European Federation of Child Neurology Societies. Under the guidance of a prestigious International editorial board, this multi-disciplinary journal publishes exciting clinical and experimental research in this rapidly expanding field. High quality papers written by leading experts encompass all the major diseases including epilepsy, movement disorders, neuromuscular disorders, neurodegenerative disorders and intellectual disability. Other exciting highlights include articles on brain imaging and neonatal neurology, and the publication of regularly updated tables relating to the main groups of disorders.
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