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首页> 外文期刊>NPJ genomic medicine. >Genome sequencing as a platform for pharmacogenetic genotyping: a pediatric cohort study
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Genome sequencing as a platform for pharmacogenetic genotyping: a pediatric cohort study

机译:基因组测序作为药物遗传学基因分型的平台:一项儿科队列研究

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Whole-genome sequencing and whole-exome sequencing have proven valuable for diagnosing inherited diseases, particularly in children. However, usage of sequencing data as a pharmacogenetic screening tool to ensure medication safety and effectiveness remains to be explored. Sixty-seven variants in 19 genes with known effects on drug response were compared between genome sequencing and targeted genotyping data for coverage and concordance in 98 pediatric patients. We used targeted genotyping data as a benchmark to assess accuracy of variant calling, and to identify copy number variations of the CYP2D6 gene. We then predicted clinical impact of these variants on drug therapy. We find genotype concordance across those panels to be >?97%. Concordance of CYP2D6 predicted phenotype between estimates of whole-genome sequencing and targeted genotyping panel were 90%; a result from a lower coverage depth or variant calling difficulties in our whole-genome sequencing data when copy number variation and/or the CYP2D6*4 haplotype were present. Importantly, 95 children had at least one clinically actionable pharmacogenetic variant. Diagnostic genomic sequencing data can be used for pre-emptive pharmacogenetic screening. However, concordance between genome-wide sequencing and target genotyping needs to be characterized for each of the pharmacologically important genes.
机译:事实证明,全基因组测序和全外显子测序对于诊断遗传性疾病(尤其是儿童)具有重要的价值。然而,将测序数据用作药物遗传学筛选工具以确保药物安全性和有效性仍有待探索。比较了98例儿科患者中19种对药物反应有已知作用的基因的67个变体在基因组测序和靶向基因分型数据之间的覆盖率和一致性。我们使用靶向基因分型数据作为基准来评估变异调用的准确性,并鉴定CYP2D6基因的拷贝数变异。然后,我们预测了这些变体对药物治疗的临床影响。我们发现这些面板上的基因型一致性≥97%。 CYP2D6预测表型与全基因组测序估计值和靶向基因分型面板的一致性为90%;当存在拷贝数变异和/或CYP2D6 * 4单倍型时,我们的全基因组测序数据中较低的覆盖深度或变异调用困难导致的结果。重要的是,有95名儿童具有至少一种临床上可行的药物遗传学变异体。诊断基因组测序数据可用于先发性药物遗传学筛选。但是,对于每个重要的药理基因,都需要表征全基因组测序与目标基因分型之间的一致性。

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