12885_2020_6777_MOESM4_ESM.pdf (4.11 MB)
Additional file 4 of The DNA hypermethylation phenotype of colorectal cancer liver metastases resembles that of the primary colorectal cancers
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posted on 2020-04-08, 09:09 authored by Stephany Orjuela, Mirco Menigatti, Peter Schraml, Patryk Kambakamba, Mark D. Robinson, Giancarlo MarraAdditional file 4: Supplementary Fig. 4. In-silico analysis of Gene Expression Omnibus DataSet GSE53051 (submitted by Timp et al., reference [39]). For each sample, the normalized average beta values per probe were downloaded. A. MDS (multidimensional scaling) plot of the beta values for 6 patients with paired normal mucosa (NM), primary cancer (CRC) and liver metastasis (Met). The limma package (reference [25]) was used to identify the 1000 probes displaying the highest variability and to plot the MDS. Consistent with the findings of our own study (Supplementary Fig. 1), normal mucosa samples from the DataSet clustered together and were appreciably separated from tumors, whereas there was no obvious separation between CRCs and liver metastases. B. Scatter plots of the mean beta values per tissue (Met vs NM, CRC vs NM, CRC vs Met) for all the probes (Genome, top 3 plots), and for probes located in CpG Islands (Islands, bottom 3 plots). CRCs and Mets had similar methylomes, both with Genome and Island probes (top and bottom panels on the right, respectively), while skewed profiles towards hypomethylation (Genome probes) or hypermethylation (Islands probes) in tumors (vs NM) were detected (the four panels on the left and in the middle). C. The similarity of the CRC and Met methylation patterns is also reflected by the mean beta values per sample across all probes (Genome, top) and the probes in CpG Islands (Islands, bottom).