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首页> 外文期刊>Nucleic Acids Research >A phylogenetic model for understanding the effect of gene duplication on cancer progression
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A phylogenetic model for understanding the effect of gene duplication on cancer progression

机译:系统发育模型,用于了解基因复制对癌症进展的影响

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摘要

As biotechnology advances rapidly, a tremendous amount of cancer genetic data has become available, providing an unprecedented opportunity for understanding the genetic mechanisms of cancer. To understand the effects of duplications and deletions on cancer progression, two genomes (normal and tumor) were sequenced from each of five stomach cancer patients in different stages (I, II, III and IV). We developed a phylogenetic model for analyzing stomach cancer data. The model assumes that duplication and deletion occur in accordance with a continuous time Markov Chain along the branches of a phylogenetic tree attached with five extended branches leading to the tumor genomes. Moreover, coalescence times of the phylogenetic tree follow a coalescence process. The simulation study suggests that the maximum likelihood approach can accurately estimate parameters in the phylogenetic model. The phylogenetic model was applied to the stomach cancer data. We found that the expected number of changes (duplication and deletion) per gene for the tumor genomes is significantly higher than that for the normal genomes. The goodness-of-fit test suggests that the phylogenetic model with constant duplication and deletion rates can adequately fit the duplication data for the normal genomes. The analysis found nine duplicated genes that are significantly associated with stomach cancer.RI Ma, Qin/O-1525-2013OI Ma, Qin/0000-0002-3264-8392
机译:随着生物技术的飞速发展,已经获得了大量的癌症遗传数据,为了解癌症的遗传机制提供了前所未有的机会。为了了解重复和缺失对癌症进展的影响,从五位不同阶段(I,II,III和IV)的胃癌患者中分别测序了两个基因组(正常和肿瘤)。我们开发了用于分析胃癌数据的系统发育模型。该模型假定重复和缺失是沿着系统发育树的分支连续的时间马尔可夫链发生的,该系统树的分支连接有五个延伸到肿瘤基因组的延伸分支。此外,系统发育树的合并时间遵循合并过程。仿真研究表明,最大似然方法可以准确估计系统发育模型中的参数。系统发育模型被应用于胃癌数据。我们发现,肿瘤基因组每个基因的预期变化(重复和缺失)数量明显高于正常基因组。拟合优度测试表明,具有恒定重复和缺失率的系统发育模型可以充分拟合正常基因组的重复数据。分析发现九个与胃癌显着相关的重复基因.RI Ma,Qin / O-1525-2013OI Ma,Qin / 0000-0002-3264-8392

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