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首页> 外文期刊>Molecular Genetics & Genomic Medicine >The phenotype‐driven computational analysis yields clinical diagnosis for patients with atypical manifestations of known intellectual disability syndromes
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The phenotype‐driven computational analysis yields clinical diagnosis for patients with atypical manifestations of known intellectual disability syndromes

机译:表型驱动的计算分析产生了已知智力残疾综合征的非典型表现患者的临床诊断

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摘要

Background Due to extensive clinical and genetic heterogeneity of intellectual disability (ID) syndromes, the process of diagnosis is very challenging even for expert clinicians. Despite recent advancements in molecular diagnostics methodologies, a significant fraction of ID patients remains without a clinical diagnosis. Methods, results, and conclusions Here, in a prospective study on a cohort of 21 families (trios) with a child presenting with ID of unknown etiology, we executed phenotype‐driven bioinformatic analysis method, PhenIX, utilizing targeted next‐generation sequencing (NGS) data and Human Phenotype Ontology (HPO)‐encoded phenotype data. This approach resulted in clinical diagnosis for eight individuals presenting with atypical manifestations of Rubinstein–Taybi syndrome 2 (MIM 613684), Spastic Paraplegia 50 (MIM 612936), Wiedemann–Steiner syndrome (MIM 605130), Cornelia de Lange syndrome 2 (MIM 300590), Cerebral creatine deficiency syndrome 1 (MIM 300352), Glass Syndrome (MIM 612313), Mental retardation, autosomal dominant 31 (MIM 616158), and Bosch–Boonstra–Schaaf optic atrophy syndrome (MIM 615722).
机译:背景技术由于智力残疾(ID)综合征的广泛临床和遗传异质性,即使对于专家临床医生,诊断过程也非常具有挑战性。尽管最近进行了分子诊断方法的进步,但尚未临床诊断,仍有大部分ID患者。在此处的方法,结果和结论,在对21个家族队列(TRIOS)的前瞻性研究中,用孩子呈现未知病因的ID,我们执行了表型驱动的生物信息分析方法,利用靶向下一代测序(NGS )数据和人类表型本体(HPO) - 均表型数据。这种方法导致患有七种单独表现的临床诊断鉴于鲁宾斯坦-Taybi综合征2(MIM 613684),痉挛截瘫50(MIM 612936),Wiedemann-Steiner综合征(MIM 605130),Cornelia de Lange综合征2(MIM 300590) ,脑肌酸缺乏综合征1(MIM 300352),玻璃综合征(MIM 612313),精神发育迟滞,常染色体优势31(MIM 616158)和Bosch-Boonstra-SchaAF光学萎缩综合征(MIM 615722)。

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