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Heterozygous deletion of SCN2A and SCN3A in a patient with autism spectrum disorder and Tourette syndrome: a case report

机译:自闭症谱图综合征和图雷特综合症患者SCN2A和SCN3A的杂合缺失:1例

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Mutations in voltage-gated sodium channel (SCN) genes are supposed to be of importance in the etiology of psychiatric and neurological diseases, in particular in the etiology of seizures. Previous studies report a potential susceptibility region at the chromosomal locus 2q including SCN1A, SCN2A and SCN3A genes for autism spectrum disorder (ASD). To date, there is no previous description of a patient with comorbid ASD and Tourette syndrome showing a deletion containing SCN2A and SCN3A. We present the unique complex case of a 28-year-old male patient suffering from developmental retardation and exhibiting a range of behavioral traits since birth. He received the diagnoses of ASD (in early childhood) and of Tourette syndrome (in adulthood) according to ICD-10 and DSM-5 criteria. Investigations of underlying genetic factors yielded a heterozygous microdeletion of approximately 719?kb at 2q24.3 leading to a deletion encompassing the five genes SCN2A (exon 1 to intron 14–15), SCN3A, GRB14 (exon 1 to intron 2–3), COBLL1 and SCL38A11. We discuss the association of SCN2A, SCN3A, GRB14, COBLL1 and SCL38A11 deletions with ASD and Tourette syndrome and possible implications for treatment.
机译:电压门控钠通道(SCN)基因的突变被认为在精神病和神经病的病因学中,特别是在癫痫发作的病因学中具有重要意义。先前的研究报告了在染色体基因座2q的潜在易感性区域,其中包括自闭症谱系障碍(ASD)的SCN1A,SCN2A和SCN3A基因。迄今为止,尚无关于患有合并症ASD和Tourette综合征的患者的先前描述,该患者显示含有SCN2A和SCN3A的缺失。我们介绍了一名28岁男性患者的独特复杂病例,该患者患有发育迟缓并自出生以来就表现出一系列行为特征。根据ICD-10和DSM-5标准,他接受了ASD(儿童早期)和Tourette综合征(成人)的诊断。对潜在遗传因素的研究在2q24.3处产生了大约719?kb的杂合微缺失,导致包含五个基因SCN2A(外显子1至内含子14-15),SCN3A,GRB14(外显子1至内含子2-3)的缺失, COBLL1和SCL38A11。我们讨论了SCN2A,SCN3A,GRB14,COBLL1和SCL38A11缺失与ASD和Tourette综合征的关联以及对治疗的潜在影响。

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