Despite the recent advances in the clinical management, colorectal cancer (CRC) remains 2nd leading cause of the cancer-related deaths in Veteran armed forces personnel. Each year Veterans affairs manage and treat ~175,000 CRC-patients and cancer progression remains the principal cause of CRC-associated death. Thus, need for therapies that can prevent CRC progression remains urgent. This proposal exploits a key clinical observation by us and other groups that expression of claudin-2, a tight junction (TJ) protein, is highly upregulated in CRC, promotes colon tumorigenesis in vivo and protects from cell death induced by chemotherapeutic drugs. However, despite the proven ability of claudin-2 to promote CRC, underlying mechanisms as well as therapeutic potential of claudin-2 remain unexplored. Importantly, among claudins expressed in colon, claudin-2 is uniquely expressed only among the undifferentiated colonocytes at crypt bottom, the proliferative zone, and promotes colonic epithelial cell (CEC) proliferation, in vitro and in vivo. Notably, claudin-2 is a transcriptional target of Wnt-signaling. Further, tissue microenvironment regulates colonic claudin-2 expression in EGFR-dependent manner. The EGFR- and Wnt-signaling regulate colonic stem cell niche and accordingly we have found upregulated expression of Lgr-5, Olf4 and CD-133, stem cell markers in cells or mice overexpressing claudin-2 versus respective controls. In CRC, a proliferative phenotype associates with dedifferentiation. In accordance, claudin-2 expression decreases with the differentiation in CRC-cells and resists differentiation when overexpressed. In addition, our preliminary studies suggest that claudin-2 may help protect CECs from stress-induced death by regulating autophagy. Our additional data using Villin-claudin-2 transgenic mice suggest that constitutive claudin-2 expression renders immune-suppression. Notably, immune suppressive conditions help promote tumor progression. Taken together, we hypothesize that claudin-2 expression promotes colon tumorigenesis by facilitating stem cell expansion and plasticity, resistance to cell death and modulation of the host-tumor immune interaction. To test our hypothesis, we propose following specific aims:
Aim -1) to determine how claudin-2 regulates colon tumor growth and tumor cell plasticity. Here, we will determine: A) the role of claudin-2 in the regulation of colonocyte differentiation, stem cell niche and tumor cell plasticity; B) whether claudin-2 promotes autophagy to promote tumor cell survival and chemoresistance; and C) whether claudin-2 expression modulates host-tumor immune interaction to promote tumor progression;
and Aim -2) to determine the role of EGFR- and Wnt-signaling in the regulation of colonic claudin-2 expression and therapeutic potential. Here, we will determine: A) the role of EGFR-dependent signaling, transcriptional mechanism/s and potential cross-talk with Wnt/?-catenin signaling in the regulation of claudin-2 expression; and B role of claudin-2 as a CRC-biomarker in conjunction with EGFR and Wnt-signaling. Our short term goal is to better understand how dysregulation of claudin-2 expression modulates the ability of colon cancer cells to form tumor and further progression. Our long term goal is to develop strategies to inhibit claudin-2 expression applicable specifically to the colon cancer cell and thus to create an anti-CRC drug that can prevent disease progression. We believe such therapeutic interventions can significantly increase survival and quality of life US Veterans who are suffering from colorectal cancer.

Public Health Relevance

Colorectal cancer (CRC) is the second leading cause of the cancer-related mortality in the Veterans population. Majority of these patients die due to the disease progression and therefore therapies that can help prevent disease progression are urgently needed. Claudin-2, a tight junction protein, is highly upregulated in CRC and its expression correlates with cancer progression. Further, Cl-2TG mice overexpressing claudin-2 develop more and advanced tumors in the presence of APC mutation. Our aim is to understand how claudin-2 affects the tumorigenic ability of CRC cells, in order to define the best possible way to harness its use as a target molecule to inhibit CRC-progression. We predict our studies will help unravel novel role of claudin-2 in the regulation of tumor cell growth and plasticity and immune regulation to regulate CRC-growth & progression and will open new therapeutic opportunities.

Agency
National Institute of Health (NIH)
Institute
Veterans Affairs (VA)
Type
Non-HHS Research Projects (I01)
Project #
5I01BX002761-02
Application #
9252978
Study Section
Cellular and Molecular Medicine (CAMM)
Project Start
2016-04-01
Project End
2020-03-31
Budget Start
2017-04-01
Budget End
2018-03-31
Support Year
2
Fiscal Year
2017
Total Cost
Indirect Cost
Name
Omaha VA Medical Center
Department
Type
DUNS #
844360367
City
Omaha
State
NE
Country
United States
Zip Code
68105
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