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A DNA resequencing array for pathogenic mutation detection in hypertrophic cardiomyopathy.

机译:用于肥厚型心肌病中致病突变检测的DNA重测序阵列。

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Hypertrophic cardiomyopathy (HCM) is a heterogeneous autosomal dominant cardiac disorder with a prevalence of 1 in 500. Over 450 different pathogenic mutations in at least 16 genes have been identified so far. The large allelic and genetic heterogeneity of HCM requires high-throughput, rapid, and affordable mutation detection technologies to efficiently integrate molecular screening into clinical practice. We developed a custom DNA resequencing array that contains both strands of all coding exons (160), splice-site junctions, and 5'UTR regions of 12 genes that have been clearly implicated in HCM (MYH7, MYBPC3, TNNT2, TPM1, TNNI3, MYL3, MYL2, CSRP3, PLN, ACTC, TNNC1, and PRKAG2). We analyzed a first series of 38 unrelated patients with HCM (17 familial, 21 sporadic). A total of 953,306 bp across the 38 patients were sequenced with a mean nucleotide call rate of 96.92% (range: 93-99.9%). Pathogenic mutations (single nucleotide substitutions) in MYH7, MYBPC3, TNNI3, and MYL3 (six known and six novel) wereidentified in 60% (10/17) of familial HCM and 10% of sporadic cases (2/21). The high-throughput HCM resequencing array is the most rapid and cost-effective tool for molecular testing of HCM to date; it thus has considerable potential in diagnostic and predictive testing, and prognostic stratification.
机译:肥厚型心肌病(HCM)是一种异质性常染色体显性心脏病,患病率为500分之一。迄今为止,已鉴定出至少16个基因的450多种致病突变。 HCM的大等位基因和遗传异质性需要高通量,快速且负担得起的突变检测技术,才能将分子筛查有效地整合到临床实践中。我们开发了一种定制的DNA重测序阵列,其中包含所有编码外显子的两条链(160),剪接位点连接和12个已明确与HCM相关的基因(MYH7,MYBPC3,TNNT2,TPM1,TNNI3, MYL3,MYL2,CSRP3,PLN,ACTC,TNNC1和PRKAG2)。我们分析了第一批38例HCM无关患者(17例家族性,21例散发性)。在38位患者中总共953,306 bp进行了测序,平均核苷酸检出率为96.92%(范围:93-99.9%)。在60%(10/17)的家族性HCM和10%的散发性病例(2/21)中鉴定出MYH7,MYBPC3,TNNI3和MYL3(六个已知和六个新颖)中的致病突变(单核苷酸取代)。高通量HCM重测序阵列是迄今为止用于HCM分子测试的最快速,最具成本效益的工具。因此,它在诊断和预测测试以及预后分层方面具有相当大的潜力。

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