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首页> 外文期刊>Human Genetics >Rapid detection of gene mutations responsible for non-syndromic aortic aneurysm and dissection using two different methods: resequencing microarray technology and next-generation sequencing.
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Rapid detection of gene mutations responsible for non-syndromic aortic aneurysm and dissection using two different methods: resequencing microarray technology and next-generation sequencing.

机译:使用两种不同的方法快速检测导致非综合征性主动脉瘤和解剖的基因突变:重新测序微阵列技术和下一代测序。

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摘要

Aortic aneurysm and/or dissection (AAD) is a life-threatening condition, and several syndromes are known to be related to AAD. In this study, two new technologies, resequencing array technology (ResAT) and next-generation sequencing (NGS), were used to analyze eight genes associated with syndromic AAD in 70 patients with non-syndromic AAD. Eighteen sequence variants were detected using both ResAT and NGS. In addition one of these sequence variants was detected by ResAT only and two additional variants by NGS only. Three of the 18 variants are likely to be pathogenic (in 4.3% of AAD patients and in 8.6% of a subset of patients with thoracic AAD), highlighting the importance of genetic analysis in non-syndromic AAD. ResAT and NGS similarly detected most, but not all, of the variants. Resequencing array technology was a rapid and efficient method for detecting most nucleotide substitutions, but was unable to detect short insertions/deletions, and it is impractical to update custom arrays frequently. Next-generation sequencing was able to detect almost all types of mutation, but requires improved informatics methods.
机译:主动脉瘤和/或夹层(AAD)是一种危及生命的疾病,已知多种综合征与AAD相关。在这项研究中,两项新技术,即重测序阵列技术(ResAT)和下一代测序(NGS),被用于分析70例非综合征AAD患者中与综合征AAD相关的八个基因。使用ResAT和NGS检测到18个序列变体。另外,仅通过ResAT检测到这些序列变体之一,而仅通过NGS检测到另外两个变体。 18个变体中的三个很可能具有致病性(在4.3%的AAD患者中和8.6%的一部分胸AAD患者中),突出了基因分析在非综合征AAD中的重要性。 ResAT和NGS类似地检测到大多数(但不是全部)变体。重测序阵列技术是检测大多数核苷酸取代的一种快速有效的方法,但无法检测短插入/缺失,因此频繁更新定制阵列是不切实际的。下一代测序能够检测几乎所有类型的突变,但需要改进的信息学方法。

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