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Estimating the order of mutations during tumorigenesis from tumor genome sequencing data

机译:从肿瘤基因组测序数据估算肿瘤发生过程中的突变顺序

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Motivation: Tumors are thought to develop and evolve through a sequence of genetic and epigenetic somatic alterations to progenitor cells. Early stages of human tumorigenesis are hidden from view. Here, we develop a method for inferring some aspects of the order of mutational events during tumorigenesis based on genome sequencing data for a set of tumors. This method does not assume that the sequence of driver alterations is the same for each tumor, but enables the degree of similarity or difference in the sequence to be evaluated. Results: To evaluate the new method, we applied it to colon cancer tumor sequencing data and the results are consistent with the multi-step tumorigenesis model previously developed based on comparing stages of cancer. We then applied the new method to DNA sequencing data for a set of lung cancers. The model may be a useful tool for better understanding the process of tumorigenesis.
机译:动机:人们认为肿瘤是通过一系列对祖细胞的遗传和表观遗传的体细胞发育而发展和进化的。人类肿瘤发生的早期阶段是看不见的。在这里,我们基于一组肿瘤的基因组测序数据,开发了一种在肿瘤发生过程中推断突变事件顺序的某些方面的方法。该方法不假定每种肿瘤的驱动程序改变序列相同,但是可以评估序列的相似性或差异性。结果:为评估该新方法,我们将其应用于结肠癌肿瘤测序数据,结果与先前基于比较癌症分期而开发的多步骤肿瘤发生模型一致。然后,我们将新方法应用于一组肺癌的DNA测序数据。该模型可能是更好地了解肿瘤发生过程的有用工具。

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