SYNGAP1 的行为和神经发育特征。

IF 4.1 2区医学 Q1 CLINICAL NEUROLOGY Journal of Neurodevelopmental Disorders Pub Date : 2024-08-15 DOI:10.1186/s11689-024-09563-8

Nadja Bednarczuk, Harriet Housby, Irene O Lee, Imagine Consortium, David Skuse, Jeanne Wolstencroft

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引用次数: 0

摘要

背景：SYNGAP1变异与不同程度的智力障碍（ID）、发育迟缓（DD）、癫痫、自闭症和行为障碍有关。在其他单基因疾病中也可观察到这些特征。有必要系统地比较 SYNGAP1 与其他导致 ID 和 DD 的单基因病因的特征，以确定 SYNAGP1 表型的独特特征。我们的目的是将SYNGAP1相关ID（SYNGAP1-ID）患儿的神经发育和行为表型与其他单基因病因和匹配程度的ID患儿进行对比：参与者是从 IMAGINE-ID 研究中确定的，IMAGINE-ID 研究是一项基于英国的全国性队列研究，研究对象是已知遗传源的 ID 儿童的神经精神风险。13名患有SYNGAP1变异体的儿童（4-16岁；85%为女性）与26名患有其他单基因ID的对照组儿童（2:1）在年龄和心理年龄、性别、社会经济贫困程度、适应行为和身体健康困难方面进行了配对。照顾者填写了发展与福利评估（DAWBA）和身体健康问卷：结果：我们的研究结果表明，SYNGAP1-ID患儿（84.6%）的癫痫发作频率高于ID对比组（7.6%；P = 结论：我们首次证明，SYNGAP1-ID患儿的癫痫发作频率高于ID对比组：我们首次证明，SYNGAP1-ID 与精细运动和语言障碍的关系超出了其他遗传原因导致的 DD 和 ID 儿童。在对 SYNGAP1-ID 进行管理时，应尽早纳入有针对性的职业和言语及语言疗法。

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Behavioural and neurodevelopmental characteristics of SYNGAP1.

Background: SYNGAP1 variants are associated with varying degrees of intellectual disability (ID), developmental delay (DD), epilepsy, autism, and behavioural difficulties. These features may also be observed in other monogenic conditions. There is a need to systematically compare the characteristics of SYNGAP1 with other monogenic causes of ID and DD to identify features unique to the SYNAGP1 phenotype. We aimed to contrast the neurodevelopmental and behavioural phenotype of children with SYNGAP1-related ID (SYNGAP1-ID) to children with other monogenic conditions and a matched degree of ID.

Methods: Participants were identified from the IMAGINE-ID study, a UK-based, national cohort study of neuropsychiatric risk in children with ID of known genetic origin. Thirteen children with SYNGAP1 variants (age 4-16 years; 85% female) were matched (2:1) with 26 controls with other monogenic causes of ID for chronological and mental age, sex, socio-economic deprivation, adaptive behaviour, and physical health difficulties. Caregivers completed the Development and Wellbeing Assessment (DAWBA) and physical health questionnaires.

Results: Our results demonstrate that seizures affected children with SYNGAP1-ID (84.6%) more frequently than the ID-comparison group (7.6%; p = < 0.001). Fine-motor development was disproportionally impaired in SYNGAP1-ID, with 92.3% of children experiencing difficulties compared to 50% of ID-comparisons(p = 0.03). Gross motor and social development did not differ between the two groups. Children with SYNGAP1-ID were more likely to be non-verbal (61.5%) than ID-comparisons (23.1%; p = 0.01). Those children able to speak, spoke their first words at the same age as the ID-comparison group (mean = 3.25 years), yet achieved lower language competency (p = 0.04). Children with SYNGAP1-ID compared to the ID-comparison group were not more likely to meet criteria for autism (SYNGAP1-ID = 46.2%; ID-comparison = 30.7%; p = .35), attention-deficit hyperactivity disorder (15.4%;15.4%; p = 1), generalised anxiety (7.7%;15.4%; p = .49) or oppositional defiant disorder (7.7%;0%; p = .15).

Conclusion: For the first time, we demonstrate that SYNGAP1-ID is associated with fine motor and language difficulties beyond those experienced by children with other genetic causes of DD and ID. Targeted occupational and speech and language therapies should be incorporated early into SYNGAP1-ID management.

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来源期刊

Journal of Neurodevelopmental Disorders 医学-临床神经学

CiteScore

7.60

自引率

4.10%

发文量

审稿时长

>12 weeks

期刊介绍： Journal of Neurodevelopmental Disorders is an open access journal that integrates current, cutting-edge research across a number of disciplines, including neurobiology, genetics, cognitive neuroscience, psychiatry and psychology. The journal’s primary focus is on the pathogenesis of neurodevelopmental disorders including autism, fragile X syndrome, tuberous sclerosis, Turner Syndrome, 22q Deletion Syndrome, Prader-Willi and Angelman Syndrome, Williams syndrome, lysosomal storage diseases, dyslexia, specific language impairment and fetal alcohol syndrome. With the discovery of specific genes underlying neurodevelopmental syndromes, the emergence of powerful tools for studying neural circuitry, and the development of new approaches for exploring molecular mechanisms, interdisciplinary research on the pathogenesis of neurodevelopmental disorders is now increasingly common. Journal of Neurodevelopmental Disorders provides a unique venue for researchers interested in comparing and contrasting mechanisms and characteristics related to the pathogenesis of the full range of neurodevelopmental disorders, sharpening our understanding of the etiology and relevant phenotypes of each condition.