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Wiedemann-Steiner syndrome with a novel pathogenic variant in KMT2A: a case report

机译:Wietemann-Steiner综合征在KMT2A中具有新型致病性变异:病例报告

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Case Description: We report the case of a one-year-old girl who was diagnosed with Wiedemann-Steiner Syndrome based on the identification of a novel de novo frameshift mutation in the KMT2A gene by whole exome sequencing and supported by her clinical features. Clinical Findings: KMT2A mutations cause Wiedemann-Steiner Syndrome, a very rare genetic disorder characterized by congenital hypertrichosis, short stature, intellectual disability, and distinct facial features. Treatment and Outcome: Whole exome sequencing identified a novel frameshift variant: c. 4177dupA (p.Ile1393Asnfs * 14) in KMT2A ; this change generates an alteration of the specific binding to non-methylated CpG motifs of the DNA to the protein. The genotype and phenotype of the patient were compared with those of earlier reported patients in the literature. Clinical Relevance: In diseases with low frequency, it is necessary to establish a genotype-phenotype correlation that allows the establishment of therapeutic and follow-up goals. The phenotype comparation with other reported cases did not show differences attributable to sex or age among patients with Wiedemann-Steiner Syndrome. Whole exome sequencing allows identifying causality in conditions with high clinical and genetic heterogeneity like hypertrichosis.
机译:病例描述:我们报道了一个一岁女孩的病例,该女孩基于整个外显子组测序在KMT2A基因中发现的新型从头突变的基础上被诊断为Wiedemann-Steiner综合征,并得到她的临床特征的支持。临床发现:KMT2A突变引起Wiedemann-Steiner综合征,这是一种非常罕见的遗传性疾病,其特征是先天性高发症,身材矮小,智力残疾和独特的面部特征。治疗和结果:整个外显子组测序确定了一个新的移码变体:c。 KMT2A中的4177dupA(p.Ile1393Asnfs * 14);这种改变产生了与DNA与蛋白质的非甲基化CpG基序的特异性结合的改变。将患者的基因型和表型与文献中较早报道的患者进行了比较。临床相关性:在低频率的疾病中,有必要建立基因型与表型的相关性,以建立治疗和随访目标。与其他报告病例的表型比较未显示出Wiedemann-Steiner综合征患者的性别或年龄差异。完整的外显子组测序可在具有高度临床和遗传异质性的情况下(如肥大症)确定因果关系。

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