Abstract

Breast cancer (BC) is the leading cause of cancer mortality in women worldwide. Triple negative breast cancer (TNBC) represents an aggressive subtype with limited therapeutic options that exhibits high rates of recurrence and metastasis. These tumors are called triple negative because they do not express the estrogen and progesterone receptors or overexpress the HER2 oncogene, which makes them refractory to current targeted therapeutic regimens. Although cancer stem cells (CSCs) remain controversial, studies support a role for a self- renewing cell population in tumor maintenance and therapeutic resistance. NANOG is a master regulator of pluripotency and self-renewal that has been implicated in breast cancer progression. Through collaborative efforts of the Lathia and Reizes laboratories, we have developed TNBC cell lines containing a green fluorescent protein (GFP) reporter driven by the NANOG promoter to analyze the stem cell state in real time. Our preliminary data show that cells expressing GFP from the NANOG promoter exhibit cellular characteristics of CSCs, whereas GFP-negative cells do not, suggesting these cells are non-CSCs. We plan to use these reporter cells to interrogate how CSCs communicate within tumors to orchestrate growth and metastasis, and here we focus on the role of CSC cell-cell communication in metastatic progression. Through the analysis of Oncomine datasets, we found that connexins, the protein subunits of gap junctions, one method of cell-cell communication, are differentially expressed in TNBCs and inform patient outcomes. Biochemical analysis of CSCs and non-CSCs using our reporter lines shows selective expression of connexin 26 (Cx26) in CSCs. The translational goal of this project is to yield proof-of-concept evidence for a therapeutic benefit of blocking cell-cell communication in CSC pluripotency and invasiveness/metastasis. Based on our observations, we hypothesize that the inhibition of gap junctions will yield therapeutic benefit against TNBC recurrence and metastasis by blocking CSC self-renewal and viability. We will test this hypothesis through the following two aims.
Aim 1 will test the hypothesis that Cx26 is necessary for CSC maintenance and metastasis.
Aim 2 will test the therapeutic benefit of gap junction inhibition on CSC maintenance and metastatic progression. The long-term goal of this research is to address the unmet medical need for effective TNBC therapies with a therapeutic focus on nonhormonal and nongenetic approaches to inhibit tumor progression by attenuating cell-cell communication in CSCs.

Public Health Relevance

Breast cancer is the leading cause of cancer mortality in women worldwide. The goal of this research is to address the unmet medical need for effective breast cancer therapies with a focus of inhibiting cell-cell communication and specifically target tumor initiating cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Exploratory/Developmental Grants (R21)
Project #
5R21CA191263-02
Application #
8977495
Study Section
Special Emphasis Panel (ZCA1)
Program Officer
Ault, Grace S
Project Start
2014-12-03
Project End
2017-11-30
Budget Start
2015-12-01
Budget End
2017-11-30
Support Year
2
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
Cleveland Clinic Lerner
Department
Other Basic Sciences
Type
Schools of Medicine
DUNS #
135781701
City
Cleveland
State
OH
Country
United States
Zip Code
44195

  Publications

Silver, Daniel J; Lathia, Justin D (2018) Therapeutic Injury and Tumor Regrowth: Tumor Resection and Radiation Establish the Recurrent Glioblastoma Microenvironment. EBioMedicine 31:13-14
Thiagarajan, Praveena S; Sinyuk, Maksim; Turaga, Soumya M et al. (2018) Cx26 drives self-renewal in triple-negative breast cancer via interaction with NANOG and focal adhesion kinase. Nat Commun 9:578
Mesnil, Marc; Aasen, Trond; Boucher, Jonathan et al. (2018) An update on minding the gap in cancer. Biochim Biophys Acta Biomembr 1860:237-243
Silver, Daniel J; Lathia, Justin D (2018) Revealing the glioma cancer stem cell interactome, one niche at a time. J Pathol 244:260-264
Saygin, Caner; Wiechert, Andrew; Rao, Vinay S et al. (2017) CD55 regulates self-renewal and cisplatin resistance in endometrioid tumors. J Exp Med 214:2715-2732
Thiagarajan, Praveena S; Zheng, Qiao; Bhagrath, Manvir et al. (2017) STAT3 activation by leptin receptor is essential for TNBC stem cell maintenance. Endocr Relat Cancer 24:415-426
Alvarado, Alvaro G; Thiagarajan, Praveena S; Mulkearns-Hubert, Erin E et al. (2017) Glioblastoma Cancer Stem Cells Evade Innate Immune Suppression of Self-Renewal through Reduced TLR4 Expression. Cell Stem Cell 20:450-461.e4
Thomas, Dustin; Thiagarajan, Praveena S; Rai, Vandana et al. (2016) Increased cancer stem cell invasion is mediated by myosin IIB and nuclear translocation. Oncotarget 7:47586-47592
Otvos, Balint; Silver, Daniel J; Mulkearns-Hubert, Erin E et al. (2016) Cancer Stem Cell-Secreted Macrophage Migration Inhibitory Factor Stimulates Myeloid Derived Suppressor Cell Function and Facilitates Glioblastoma Immune Evasion. Stem Cells 34:2026-39
Silver, Daniel J; Sinyuk, Maksim; Vogelbaum, Michael A et al. (2016) The intersection of cancer, cancer stem cells, and the immune system: therapeutic opportunities. Neuro Oncol 18:153-9

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