Abstract

Using gene expression data to enhance our knowledge of control networks relevant to cancer biology and therapy is a challenging but urgent task. Based on the premise that genes that are expressed together in a variety of cell types are likely to functions together, we derived mutually correlated genes that function together in various processes in epithelial-like tumor cells. Expression-correlated genes were derived from data for the NCI-60 human tumor cell lines, as well as data from the Broad Institute's CCLE cell lines. NCI-60 cell lines that selectively expressed a mutually correlated subset of tight junction genes served as a signature for epithelial-like cancer cells. Those signature cell lines served as a seed to derive other correlated genes, many of which had various other epithelial-related functions. Literature survey yielded molecular interaction and function information about those genes, from which molecular interaction maps were assembled. Many of the genes had epithelial functions unrelated to tight junctions, demonstrating that new function categories were elicited. The most highly correlated genes were implicated in the following epithelial functions: interactions at tight junctions (CLDN7, CLDN4, CLDN3, MARVELD3, MARVELD2, TJP3, CGN, CRB3, LLGL2, EPCAM, LNX1);interactions at adherens junctions (CDH1, ADAP1, CAMSAP3);interactions at desmosomes (PPL, PKP3, JUP);transcription regulation of cell-cell junction complexes (GRHL1 and 2);epithelial RNA splicing regulators (ESRP1 and 2);epithelial vesicle traffic (RAB25, EPN3, GRHL2, EHF, ADAP1, MYO5B);epithelial Ca(+2) signaling (ATP2C2, S100A14, BSPRY);terminal differentiation of epithelial cells (OVOL1 and 2, ST14, PRSS8, SPINT1 and 2);maintenance of apico-basal polarity (RAB25, LLGL2, EPN3). The findings provide a foundation for future studies to elucidate the functions of regulatory networks specific to epithelial-like cancer cells and to probe for anti-cancer drug targets. We are now using these methods and findings to investigate the molecular interaction network that controls the switch between epithelial and mesenchymal phenotypes in human cancer cell lines. We are searching databases of large numbers of compounds and human tumor cell lines to find compounds whose cytotoxicity patterns against various cell lines correlate with the expression pattern of genes central to the epithelial-mesenchymal transitions.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Investigator-Initiated Intramural Research Projects (ZIA)
Project #
1ZIABC006192-26
Application #
8937652
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
26
Fiscal Year
2014
Total Cost
Indirect Cost

  Institution

Name
Basic Sciences
Department
Type
DUNS #
City
State
Country
Zip Code

  Publications

Kohn, Kurt W; Zeeberg, Barry M; Reinhold, William C et al. (2014) Gene expression correlations in human cancer cell lines define molecular interaction networks for epithelial phenotype. PLoS One 9:e99269
Fried, Jake Y; van Iersel, Martijn P; Aladjem, Mirit I et al. (2013) PathVisio-Faceted Search: an exploration tool for multi-dimensional navigation of large pathways. Bioinformatics 29:1465-6
Reinhold, William C; Sunshine, Margot; Liu, Hongfang et al. (2012) CellMiner: a web-based suite of genomic and pharmacologic tools to explore transcript and drug patterns in the NCI-60 cell line set. Cancer Res 72:3499-511
Zeeberg, Barry R; Reinhold, William; Snajder, Rene et al. (2012) Functional categories associated with clusters of genes that are co-expressed across the NCI-60 cancer cell lines. PLoS One 7:e30317
Kohn, Kurt W; Zeeberg, Barry R; Reinhold, William C et al. (2012) Gene expression profiles of the NCI-60 human tumor cell lines define molecular interaction networks governing cell migration processes. PLoS One 7:e35716
Zeeberg, Barry R; Kohn, Kurt W; Kahn, Ari et al. (2012) Concordance of gene expression and functional correlation patterns across the NCI-60 cell lines and the Cancer Genome Atlas glioblastoma samples. PLoS One 7:e40062
Chandan, Kumar; van Iersel, Martijn P; Aladjem, Mirit I et al. (2012) PathVisio-Validator: a rule-based validation plugin for graphical pathway notations. Bioinformatics 28:889-90
Luna, Augustin; Karac, Evrim I; Sunshine, Margot et al. (2011) A formal MIM specification and tools for the common exchange of MIM diagrams: an XML-Based format, an API, and a validation method. BMC Bioinformatics 12:167
Luna, Augustin; Sunshine, Margot L; van Iersel, Martijn P et al. (2011) PathVisio-MIM: PathVisio plugin for creating and editing Molecular Interaction Maps (MIMs). Bioinformatics 27:2165-6
Liu, Hongfang; D'Andrade, Petula; Fulmer-Smentek, Stephanie et al. (2010) mRNA and microRNA expression profiles of the NCI-60 integrated with drug activities. Mol Cancer Ther 9:1080-91

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