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Human genetic variation database a reference database of genetic variations in the Japanese population

机译:人类遗传变异数据库日本人口遗传变异的参考数据库

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摘要

Whole-genome and -exome resequencing using next-generation sequencers is a powerful approach for identifying genomic variations that are associated with diseases. However, systematic strategies for prioritizing causative variants from many candidates to explain the disease phenotype are still far from being established, because the population-specific frequency spectrum of genetic variation has not been characterized. Here, we have collected exomic genetic variation from 1208 Japanese individuals through a collaborative effort, and aggregated the data into a prevailing catalog. In total, we identified 156 622 previously unreported variants. The allele frequencies for the majority (88.8%) were lower than 0.5% in allele frequency and predicted to be functionally deleterious. In addition, we have constructed a Japanese-specific major allele reference genome by which the number of unique mapping of the short reads in our data has increased 0.045% on average. Our results illustrate the importance of constructing an ethnicity-specific reference genome for identifying rare variants. All the collected data were centralized to a newly developed database to serve as useful resources for exploring pathogenic variations. Public access to the database is available at .
机译:使用下一代测序仪进行全基因组和外显子组重测序是一种鉴定与疾病相关的基因组变异的有效方法。但是,由于尚未对遗传变异的特定人群频谱进行表征,因此尚未建立用于确定来自许多候选者的致病性变异以解释疾病表型的系统策略。在这里,我们通过合作收集了1208名日本人的外显子遗传变异,并将这些数据汇总到一个流行的目录中。总的来说,我们确定了156-622个以前未报告的变体。大多数(88.8%)的等位基因频率低于等位基因频率的0.5%,并且预测为功能有害的。此外,我们已经构建了一个日本特有的主要等位基因参考基因组,通过该基因组,我们的数据中短读的独特映射数量平均增加了0.045%。我们的结果说明了构建种族特异性参考基因组以鉴定罕见变体的重要性。所有收集的数据都集中到一个新开发的数据库中,作为探索病原变异的有用资源。可通过访问公共访问数据库。

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