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首页> 外文期刊>Frontiers in Pediatrics >Molecular Diagnosis of Panel-Based Next-Generation Sequencing Approach and Clinical Symptoms in Patients With Glycogen Storage Disease: A Single Center Retrospective Study
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Molecular Diagnosis of Panel-Based Next-Generation Sequencing Approach and Clinical Symptoms in Patients With Glycogen Storage Disease: A Single Center Retrospective Study

机译:基于面板的下一代测序方法的分子诊断和糖原储存疾病患者的临床症状:单一中心回顾性研究

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Aim: The aim of this study was to investigate the clinical utility of panel-based next-generation sequencing (NGS) in the diagnostic approach of glycogen storage disease (GSD). Methods: We performed a retrospective review of the 32 cases with suspected GSDs between April 2013 and November 2019 through panel-based NGS, clinical and biochemical data and long-term complications. Results: Of the 32 clinical cases, we identified 41 different variants, including 24 missense (58.5%), one synonymous (2.4%), three nonsense (8%), one splice (2.4%), four frameshift (9.8%), one deletion (2.4%), four insertions (9.8%), two deletion-insertion (4.9%) and one duplication(2.4%), of which 13(31.7%) were previously unreported in the literature. In addition, patients with different types of GSDs showed important differences in biochemical parameters (i.e., CK, rGGT, TG, and UA). Conclusions: The panel-based NGS played an important diagnostic role in the suspicious GSDs patients, especially in the mild phenotype and ruled out detectable pathologic conditions. Besides, differences between our GSDs patients reflect biochemical heterogeneity.
机译:目的:本研究的目的是研究基于面板的下一代测序(NGS)在糖原储存疾病(GSD)的诊断方法中的临床用途。方法:通过基于基于基于面板,临床和生物化学数据和长期并发症,对涉嫌GSDS的32例疑似GSD进行了回顾性审查。结果:在32例临床病例中,我们确定了41种不同的变体,包括24个错过(58.5%),一个同义词(2.4%),三个废话(8%),一种拼接(2.4%),四个架子(9.8%),一种缺失(2.4%),四个插入(9.8%),两种缺失插入(4.9%)和一个重复(2.4%),其中13(31.7%)在文献中未报告。此外,不同类型的GSD患者表现出生物化学参数的重要差异(即CK,RGGT,TG和UA)。结论:基于面板的NGS在可疑的GSDS患者中发挥了重要的诊断作用,特别是在轻度表型中,并排除了可检测的病理条件。此外,我们的GSDS患者之间的差异反映了生物化学的异质性。

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