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首页> 外文期刊>Nucleic Acids Research >Sequence-matched probes produce increased cross-platform consistency and more reproducible biological results in microarray-based gene expression measurements
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Sequence-matched probes produce increased cross-platform consistency and more reproducible biological results in microarray-based gene expression measurements

机译:序列匹配的探针在基于微阵列的基因表达测量中可产生更高的跨平台一致性和更可重复的生物学结果

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摘要

Cancer derived microarray data sets are routinely produced by various platforms that are either commercially available or manufactured by academic groups. The fundamental difference in their probe selection strategies holds the promise that identical observations produced by more than one platform prove to be more robust when validated by biology. However, cross-platform comparison requires matching corresponding probe sets. We are introducing here sequence-based matching of probes instead of gene identifier-based matching. We analyzed breast cancer cell line derived RNA aliquots using Agilent cDNA and Affymetrix oligonucleotide microarray platforms to assess the advantage of this method. We show, that at different levels of the analysis, including gene expression ratios and difference calls, cross-platform consistency is significantly improved by sequence- based matching. We also present evidence that sequence-based probe matching produces more consistent results when comparing similar biological data sets obtained by different microarray platforms. This strategy allowed a more efficient transfer of classification of breast cancer samples between data sets produced by cDNA microarray and Affymetrix gene-chip platforms.
机译:癌症衍生的微阵列数据集通常由各种平台产生,这些平台可以商购获得,也可以由学术团体制造。他们的探针选择策略的根本区别在于,可以保证由多个平台产生的相同观察结果在通过生物学验证时被证明更加可靠。但是,跨平台比较需要匹配相应的探针集。我们在这里介绍探针的基于序列的匹配,而不是基于基因标识符的匹配。我们使用安捷伦cDNA和Affymetrix寡核苷酸微阵列平台分析了乳腺癌细胞系衍生的RNA等分试样,以评估该方法的优势。我们显示,在不同的分析级别(包括基因表达率和差异调用),基于序列的匹配显着提高了跨平台一致性。我们还提供了证据,当比较由不同微阵列平台获得的相似生物学数据集时,基于序列的探针匹配会产生更一致的结果。这种策略允许在cDNA微阵列和Affymetrix基因芯片平台产生的数据集之间更有效地转移乳腺癌样本的分类。

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