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Individualized Iterative Phenotyping for Genome-wide Analysis of Loss-of-Function Mutations

机译:全基因组功能丧失突变分析的个性化迭代表型。

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摘要

Next-generation sequencing provides the opportunity to practice predictive medicine based on identified variants. Putative loss-of-function (pLOF) variants are common in genomes and understanding their contribution to disease is critical for predictive medicine. To this end, we characterized the consequences of pLOF variants in an exome cohort by iterative phenotyping. Exome data were generated on 951 participants from the ClinSeq cohort and filtered for pLOF variants in genes likely to cause a phenotype in heterozygotes. 103 of 951 exomes had such a pLOF variant and 79 participants were evaluated. Of those 79, 34 had findings or family histories that could be attributed to the variant (28 variants in 18 genes), 2 had indeterminate findings (2 variants in 2 genes), and 43 had no findings or a negative family history for the trait (34 variants in 28 genes). The presence of a phenotype was correlated with two mutation attributes: prior report of pathogenicity for the variant (p = 0.0001) and prior report of other mutations in the same exon (p = 0.0001). We conclude that 1/30 unselected individuals harbor a pLOF mutation associated with a phenotype either in themselves or their family. This is more common than has been assumed and has implications for the setting of prior probabilities of affection status for predictive medicine.
机译:下一代测序为基于已鉴定变体的预测医学实践提供了机会。假定的功能丧失(pLOF)变体在基因组中很常见,了解其对疾病的影响对于预测医学至关重要。为此,我们通过迭代表型表征了外显子组队列中pLOF变异的后果。从ClinSeq队列的951名参与者中产生了外显子组数据,并针对可能导致杂合子表型的基因中的pLOF变异进行了过滤。 951个外显子组中有103个具有这种pLOF变异,并对79位参与者进行了评估。在这79个中,有34个具有可归因于该变异的发现或家族史(18个基因中的28个变异),2个具有不确定的发现(2个基因中的2个变异)以及43个没有发现或该特征的家族史为阴性(28个基因中的34个变体)。表型的存在与两个突变属性相关:该变体的致病性的先前报告(p = 0.0001)和同一外显子中其他突变的先前报告(p = 0.0001)。我们得出的结论是,1/30未选择的个体在其自身或家人中都携带与表型相关的pLOF突变。这比预期的要普遍得多,并且对预测医学的情感状态先前概率的设置有影响。

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