It has become clear that there is no single type of breast cancer, but rather at least six sub-types of human cancer have been identified through gene expression profiling. Our recent work has focused on understanding which mouse models of human mammary cancer represent specific sub-types of human breast cancer in order 1) to better understand what determines the mechanisms that underlie the lineage determinants of breast cancer sub-types, and 2) which models best represent particular sub-types of human breast cancer for use in pre-clinical testing for those sub-types. Recently, we have identified in mouse models where functions of both p53 and Rb have been compromised a very comprehensive, integrated genetic network of genes related to replication, DNA synthesis and repair, chromosome maintenance, proliferation, and apoptosis. This network is highly represented in- and predictive of basal-type breast cancer and the most aggressive forms of prostate and lung cancers. We hypothesize that many of these previously unrecognized genes related to basal type tumors may be potentially important targets for anti-cancer therapies and we are pursuing this experimentally. We have also expanded our work related to understanding global genomic changes that occur in GEM mammary tumor models based upon the initiating oncogenic event. We have developed gene expression, array CGH and miRNA datasets from the same tumors from eight mammary tumor models. We hypothesize that cancer may evolve differently depending upon the initiating oncogenic event and that understanding these processes may provide insights into identifying secondary changes that are critical for tumor development and progression. We have determined that models with compromised function of p53, Rb or BRCA1 evolve into a basal-type of mammary cancer, whereas the MMTV-oncogene driven models reflect a luminal phenotype. Interestingly, significant differences in genomic copy number changes and ploidy also distinguish these various mammary tumor models. Analysis of miRNA expression patterns also differ significantly between the models and the functional significance of this is being explored and compared to miRNA expression patterns in human breast cancer. Many of these distinguishing molecular features may be related to the lineage specificity of the mammary tumors that develop. We have recently used a novel informatics approach to correlate inverse relationships between miRNA and mRNA expression of predicted miRNA targets to identify new miRNA targets that may be related to tumor lineage and biology. We have continued to characterize several new mouse models of mammary cancer that demonstrate the critical interactions of genetic mutations in altering the histologic tumor phenotype that develops. Preliminary analyses indicate that the loss of expression of a particular gene can switch the tumor lineage from an adenosquamous to adencarcinoma phenotype. The molecular mechanisms related to this lineage specificity are being further explored through microarray analyses and functional studies. We have also begun to demonstrate that targeted expression of key transcription factors to breast cancer cells can significantly alter their phenotype and biologic properties. We are pursuing this approach as a means of novel differentiation therapy with the goal of reducing aggressive and metastatic properties of breast cancer cells. Ultimately, this could have translational value for prevention or therapeutic approaches. Crucial to understanding how various sub-types of breast cancer evolve is to explore the potential relationships between mammary cancer cells with stem-cell like properties to tumor development with luminal or basal characteristics. We hypothesize that mammary stem cell like cells can be developed from certain mouse cells through molecular manipulations and we are pursuing these approaches. Establishing such cell lines will enable us to more precisely understand mechanism that transform such cancer precursor cells and expand our ability to find therapies to overcome resistance to cancer treatments. It has become clear that tumor cells do not exist as isolated entities, but interact in critical ways with the microenvironment and neighboring stromal cells. We are pursuing studies to explore cross talk between tumor epithelial cells and stromal cells under various conditions using genomic technologies. This will expand our understanding of systems biology where information exchange in a multicellular system will be determined. This will likely have important implications for identifying potential targets to interrupt this important cross-talk between tumor cells and their environment.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Investigator-Initiated Intramural Research Projects (ZIA)
Project #
1ZIABC005740-17
Application #
7965074
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
17
Fiscal Year
2009
Total Cost
$1,214,015
Indirect Cost
Name
National Cancer Institute Division of Basic Sciences
Department
Type
DUNS #
City
State
Country
Zip Code
Min, Dong-Joon; He, Siping; Green, Jeffrey E (2016) Birinapant (TL32711) Improves Responses to GEM/AZD7762 Combination Therapy in Triple-negative Breast Cancer Cell Lines. Anticancer Res 36:2649-57
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Rodriguez, Virginia; Vasudevan, Sona; Noma, Akiko et al. (2012) Structure-function analysis of human TYW2 enzyme required for the biosynthesis of a highly modified Wybutosine (yW) base in phenylalanine-tRNA. PLoS One 7:e39297
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Bennett, Christina N; Tomlinson, Christine C; Michalowski, Aleksandra M et al. (2012) Cross-species genomic and functional analyses identify a combination therapy using a CHK1 inhibitor and a ribonucleotide reductase inhibitor to treat triple-negative breast cancer. Breast Cancer Res 14:R109
Reindl, Wolfgang; Bowen, Benjamin P; Balamotis, Michael A et al. (2011) Multivariate analysis of a 3D mass spectral image for examining tissue heterogeneity. Integr Biol (Camb) 3:460-7

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