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Analysis of optimal alignments unfolds aligners’ bias in existing variant profiles

机译:最佳比对的分析揭示了现有变体图谱中的比对偏差

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摘要

Efforts such as International HapMap Project and 1000 Genomes Project resulted in a catalog of millions of single nucleotides and insertion/deletion (INDEL) variants of the human population. Viewed as a reference of existing variants, this resource commonly serves as a gold standard for studying and developing methods to detect genetic variants. Our analysis revealed that this reference contained thousands of INDELs that were constructed in a biased manner. This bias occurred at the level of aligning short reads to reference genomes to detect variants. The bias is caused by the existence of many theoretically optimal alignments between the reference genome and reads containing alternative alleles at those INDEL locations. We examined several popular aligners and showed that these aligners could be divided into groups whose alignments yielded INDELs that agreed strongly or disagreed strongly with reported INDELs. This finding suggests that the agreement or disagreement between the aligners’ called INDEL and the reported INDEL is merely a result of the arbitrary selection of one of the optimal alignments. The existence of bias in INDEL calling might have a serious influence in downstream analyses. As such, our finding suggests that this phenomenon should be further addressed.
机译:诸如国际HapMap项目和1000个基因组项目之类的努力导致了人类数百万个单核苷酸和插入/缺失(INDEL)变异的目录。作为现有变异的参考,该资源通常用作研究和开发检测遗传变异的方法的黄金标准。我们的分析表明,该参考文献包含成千上万种以偏倚方式构建的INDEL。这种偏差发生在使短读与参考基因组比对以检测变体的水平上。该偏差是由于参考基因组和在这些INDEL位置上包含替代等位基因的读段之间存在许多理论上最佳的比对所致。我们检查了几种流行的比对仪,结果表明,这些比对仪可分为几组,其比对结果产生的INDEL与所报道的INDEL完全一致或完全不同。这一发现表明,对准子的INDEL与所报告的INDEL之间的同意或分歧仅仅是对最佳比对之一进行任意选择的结果。 INDEL调用中存在偏差可能会对下游分析产生严重影响。因此,我们的发现表明应进一步解决这一现象。

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