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LoFreq: a sequence-quality aware, ultra-sensitive variant caller for uncovering cell-population heterogeneity from high-throughput sequencing datasets

机译:LoFreq:具有序列质量意识的超灵敏变异调用者,可用于从高通量测序数据集中发现细胞种群的异质性

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摘要

The study of cell-population heterogeneity in a range of biological systems, from viruses to bacterial isolates to tumor samples, has been transformed by recent advances in sequencing throughput. While the high-coverage afforded can be used, in principle, to identify very rare variants in a population, existing ad hoc approaches frequently fail to distinguish true variants from sequencing errors. We report a method (LoFreq) that models sequencing run-specific error rates to accurately call variants occurring in <0.05% of a population. Using simulated and real datasets (viral, bacterial and human), we show that LoFreq has near-perfect specificity, with significantly improved sensitivity compared with existing methods and can efficiently analyze deep Illumina sequencing datasets without resorting to approximations or heuristics. We also present experimental validation for LoFreq on two different platforms (Fluidigm and Sequenom) and its application to call rare somatic variants from exome sequencing datasets for gastric cancer. Source code and executables for LoFreq are freely available at http://sourceforge.net/projects/lofreq/.
机译:测序通量的最新进展已改变了从病毒到细菌分离物再到肿瘤样品等一系列生物系统中细胞种群异质性的研究。虽然原则上可以使用提供的高覆盖率来识别种群中非常罕见的变异,但是现有的临时方法经常无法将真正的变异与测序错误区分开。我们报告了一种方法(LoFreq),该方法可以对测序运行特定的错误率进行建模,以准确调用发生在<0.05%人口中的变异。使用模拟的和真实的数据集(病毒,细菌和人类),我们显示LoFreq具有近乎完美的特异性,与现有方法相比灵敏度显着提高,并且可以有效地分析Illumina的深度测序数据集而无需求助于近似法或启发式法。我们还介绍了LoFreq在两个不同平台(Fluidigm和Sequenom)上的实验验证,及其在从胃癌外显子组测序数据集中调用稀有体细胞变异体的应用。 LoFreq的源代码和可执行文件可从http://sourceforge.net/projects/lofreq/免费获得。

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