asymmetric microarray data produces gene lists highly predictive of research literature on multiple cancer types不对称的微阵列数据产生基因列表高度预测多种癌症类型的研究文献.pdfVIP
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asymmetric microarray data produces gene lists highly predictive of research literature on multiple cancer types不对称的微阵列数据产生基因列表高度预测多种癌症类型的研究文献
Dawany and Tozeren BMC Bioinformatics 2010, 11:483
/1471-2105/11/483
METHODOLOGY ARTICLE Open Access
Asymmetric microarray data produces gene lists
highly predictive of research literature on
multiple cancer types
*
Noor B Dawany, Aydin Tozeren
Abstract
Background: Much of the public access cancer microarray data is asymmetric, belonging to datasets containing
no samples from normal tissue. Asymmetric data cannot be used in standard meta-analysis approaches (such as
the inverse variance method) to obtain large sample sizes for statistical power enrichment. Noting that plenty of
normal tissue microarray samples exist in studies not involving cancer, we investigated the viability and accuracy of
an integrated microarray analysis approach based on significance analysis of microarrays (merged SAM) using a
collection of data from separate diseased and normal samples.
Results: We focused on five solid cancer types (colon, kidney, liver, lung, and pancreas), where available microarray
data allowed us to compare meta-analysis and integrated approaches. Our results from the merged SAM
significantly overlapped gene lists from the validated inverse-variance method. Both meta-analysis and merged
SAM approaches successfully captured the aberrances in the cell cycle that commonly occur in the different cancer
types. However, the integrated SAM analysis replicated the known cancer literature (excluding microarray studies)
with much more accuracy than the meta-analysis.
Conclusion: The merged SAM test is a powerful, robust approach for combining data from similar platforms and
for analyzing asymmetric datasets, including those with only normal or only cancer samples that cannot be utilized
by meta-analysis methods. The integrated SAM approach can also be used in comparing global gene expressio
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