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A new method for gene discovery in large-scale microarray data

机译:大规模芯片数据中基因发现的新方法

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摘要

Microarrays are an effective tool for monitoring genome-wide gene expression levels. In current microarray analyses, the majority of genes on arrays are frequently eliminated for further analysis because the changes in their expression levels (ratios) are considered to be not significant. This strategy risks failure to discover whole sets of genes related to a quantitative trait of interest, which is generally controlled by several loci that make various contributions. Here, we describe a high-throughput gene discovery method based on correspondence analysis with a new index for expression ratios [arctan (1/ratio)] and three artificial marker genes. This method allows us to quickly analyze the whole microarray dataset and discover up-/down-regulated genes related to a trait of interest. We employed an example dataset to show the theoretical advantage of this method. We then used the method to identify 88 cancer-related genes from a published microarray data from patients with breast cancer. This method also allows us to predict the phenotype of a given sample from the gene expression profile. This method can be easily performed and the result is also visible in 3D viewing software that we have developed.
机译:微阵列是监测全基因组基因表达水平的有效工具。在当前的微阵列分析中,阵列上的大多数基因经常被淘汰以进行进一步分析,因为它们的表达水平(比率)的变化被认为是不重要的。该策略冒着无法发现与感兴趣的定量特征相关的整套基因的风险,该基因通常由几个做出各种贡献的基因座控制。在这里,我们描述了一种基于对应分析的高通量基因发现方法,该方法具有一个新的表达比指标[arctan(1 / ratio)]和三个人工标记基因。这种方法使我们能够快速分析整个微阵列数据集,并发现与目的性状相关的上调/下调基因。我们使用一个示例数据集来显示此方法的理论优势。然后,我们使用该方法从已发表的乳腺癌患者微阵列数据中鉴定了88个与癌症相关的基因。这种方法还使我们能够根据基因表达谱预测给定样品的表型。这种方法可以轻松执行,并且在我们开发的3D观看软件中也可以看到结果。

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