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A highly accurate platform for clone-specific mutation discovery enables the study of active mutational processes

机译:高度精确的克隆特异性突变发现平台可用于研究活跃的突变过程

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摘要

Bulk whole genome sequencing (WGS) enables the analysis of tumor evolution but, because of depth limitations, can only identify old mutational events. The discovery of current mutational processes for predicting the tumor’s evolutionary trajectory requires dense sequencing of individual clones or single cells. Such studies, however, are inherently problematic because of the discovery of excessive false positive (FP) mutations when sequencing picogram quantities of DNA. Data pooling to increase the confidence in the discovered mutations, moves the discovery back in the past to a common ancestor. Here we report a robust WGS and analysis pipeline (DigiPico/MutLX) that virtually eliminates all F results while retaining an excellent proportion of true positives. Using our method, we identified, for the first time, a hyper-mutation (kataegis) event in a group of ∼30 cancer cells from a recurrent ovarian carcinoma. This was unidentifiable from the bulk WGS data. Overall, we propose DigiPico/MutLX method as a powerful framework for the identification of clone-specific variants at an unprecedented accuracy.
机译:大块全基因组测序(WGS)能够分析肿瘤的进展,但由于深度限制,只能识别出旧的突变事件。要发现目前预测肿瘤进化轨迹的突变过程,就需要对单个克隆或单个细胞进行密集测序。但是,由于对皮克数量的DNA进行测序时会发现过多的假阳性(FP)突变,因此此类研究固有地存在问题。数据池可提高对发现的突变的置信度,将发现移回过去的共同祖先。在这里,我们报告了一个可靠的WGS和分析管道(DigiPico / MutLX),它几乎消除了所有F结果,同时保留了极佳的真实正数比例。使用我们的方法,我们首次确定了一组来自复发性卵巢癌的约30个癌细胞中的超突变(kataegis)事件。从大量的WGS数据中无法确定。总体而言,我们建议使用DigiPico / MutLX方法作为功能强大的框架,以前所未有的准确性来识别克隆特定的变体。

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