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. 2009 Aug 15;25(16):1999-2005.
doi: 10.1093/bioinformatics/btp364. Epub 2009 Jun 19.

Copy number variation has little impact on bead-array-based measures of DNA methylation

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Copy number variation has little impact on bead-array-based measures of DNA methylation

E Andrés Houseman et al. Bioinformatics. .

Abstract

Motivation: Integration of various genome-scale measures of molecular alterations is of great interest to researchers aiming to better define disease processes or identify novel targets with clinical utility. Particularly important in cancer are measures of gene copy number DNA methylation. However, copy number variation may bias the measurement of DNA methylation. To investigate possible bias, we analyzed integrated data obtained from 19 head and neck squamous cell carcinoma (HNSCC) tumors and 23 mesothelioma tumors.

Results: Statistical analysis of observational data produced results consistent with those anticipated from theoretical mathematical properties. Average beta value reported by Illumina GoldenGate (a bead-array platform) was significantly smaller than a similar measure constructed from the ratio of average dye intensities. Among CpGs that had only small variations in measured methylation across tumors (filtering out clearly biological methylation signatures), there were no systematic copy number effects on methylation for three and more than four copies; however, one copy led to small systematic negative effects, and no copies led to substantial significant negative effects.

Conclusions: Since mathematical considerations suggest little bias in methylation assayed using bead-arrays, the consistency of observational data with anticipated properties suggests little bias. However, further analysis of systematic copy number effects across CpGs suggest that though there may be little bias when there are copy number gains, small biases may result when one allele is lost, and substantial biases when both alleles are lost. These results suggest that further integration of these measures can be useful for characterizing the biological relationships between these somatic events.

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Figures

Fig. 1.
Fig. 1.
Boxplots depicting signal (y-axis) by copy number (x-axis) associations; white = HNSCC and gray = mesothelioma.
Fig. 2.
Fig. 2.
Systematic effect of copy number on methylation at CpG sites for which overall variation in methylation is small. (A) The range of standard deviation thresholds is depicted on the x-axis and the value of the correlation coefficient for the regression of copy number on small methylation changes is depicted on the y-axis for the given copy number states. (B) The range of standard deviation thresholds is depicted on the x-axis and the value of the correlation coefficient and its point-wise 95% confidence band for the regression of copy number on small methylation changes is depicted on the y-axis for each copy number state.
Fig. 3.
Fig. 3.
Copy number and methylation on Chromosome 8 among mesothelioma tumors. For copy number, green=loss, white=no change, red=gain. For methylation, yellow=unmethylated, blue=methylated. In both panels, the 23 tumors are ordered by their copy number profiles via hierarchical clustering.

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