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Lessons from a decade of integrating cancer copy number alterations with gene expression profiles

机译:将癌症拷贝数改变与基因表达谱整合在一起的十年经验

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Over the last decade, multiple functional genomic datasets studying chromosomal aberrations and their downstream effects on gene expression have accumulated for several cancer types. A vast majority of them are in the form of paired gene expression profiles and somatic copy number alterations (CNA) information on the same patients identified using microarray platforms. In response, many algorithms and software packages are available for integrating these paired data. Surprisingly, there has been no serious attempt to review the currently available methodologies or the novel insights brought using them. In this work, we discuss the quantitative relationships observed between CNA and gene expression in multiple cancer types and biological milestones achieved using the available methodologies. We discuss the conceptual evolution of both, the step-wise and the joint data integration methodologies over the last decade. We conclude by providing suggestions for building efficient data integration methodologies and asking further biological questions.
机译:在过去的十年中,研究了几种染色体类型的染色体畸变及其对基因表达的下游影响的多功能基因组数据集。在使用微阵列平台鉴定的同一名患者中,绝大多数是成对的基因表达谱和体拷贝数改变(CNA)信息。作为响应,许多算法和软件包可用于集成这些配对的数据。令人惊讶的是,还没有认真的尝试来审查当前可用的方法或使用它们所带来的新颖见解。在这项工作中,我们讨论了在多种癌症类型中的CNA与基因表达之间观察到的定量关系以及使用现有方法实现的生物学里程碑。我们讨论了过去十年中逐步和联合数据集成方法的概念演变。最后,我们通过提供建议来建立有效的数据集成方法并提出进一步的生物学问题。

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