Abstract

This is a competing renewal application for a project which was initiated in 1978. The objective of the project was to determine the molecular basis for biological differences among sub classes of colon carcinoma cells. It is ultimately intended to use these differences for new therapeutic approaches. The overall objectives of the last period of funding were to identify and characterize autocrine growth factors produced by previously identified sub-classes of colon carcinoma cell lines and to determine their responses to growth factors. Each of these objectives were accomplished. The colon carcinoma cell line bank was converted to growth in a chemically defined medium. This permitted the determination of the effects of exogenously added growth factors and combinations of growth factors on various growth assays of sub-classes of cells. TGF-alpha and gastin were identified as autocrine stimulatory factors. The expression of these autocrine factors at the mRNA and protein levels as a function of the sub- classes of carcinoma cells was determined. The response to the autocrine stimulatory and inhibitory factors (TGF-beta family) as function of sub- classes of colon carcinoma was determined. TGF-beta activity was associated with repression of c-myc oncogene and induction of extracellular matrix molecules. Having identified positive and negative autocrine factors for colon carcinoma cells, the next logical step is the characterization of how their expression is controlled by the cells and how it is affected by exogenous agents.
The specific aims of the renewal proposal are: 1. Characterize the control of TGF-alpha expression through the analysis of cis and trans elements of the TGF-alpha elements promoter, 2. Determine control of TGF-alpha expression in colon carcinoma by exogenous agents using promoter-reporter gene constructs, nuclear runoffs, Northern analysis of mRNA and protein determination, 3. Characterize the control of gastin expression in colon carcinoma using the approaches for TGF-alpha above, 4. Characterize the mechanism of TGF-beta inhibitory action in colon carcinoma.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA034432-08
Application #
3172110
Study Section
Metabolic Pathology Study Section (MEP)
Project Start
1982-02-01
Project End
1997-03-31
Budget Start
1993-04-01
Budget End
1994-03-31
Support Year
8
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
University of Toledo
Department
Type
Schools of Medicine
DUNS #
807418939
City
Toledo
State
OH
Country
United States
Zip Code
43614

  Publications

Leiphrakpam, Premila D; Agarwal, Ekta; Mathiesen, Michelle et al. (2014) In vivo analysis of insulin-like growth factor type 1 receptor humanized monoclonal antibody MK-0646 and small molecule kinase inhibitor OSI-906 in colorectal cancer. Oncol Rep 31:87-94
Leiphrakpam, Premila D; Rajput, Ashwani; Mathiesen, Michelle et al. (2014) Ezrin expression and cell survival regulation in colorectal cancer. Cell Signal 26:868-79
Agarwal, Ekta; Chaudhuri, Anathbandhu; Leiphrakpam, Premila D et al. (2014) Akt inhibitor MK-2206 promotes anti-tumor activity and cell death by modulation of AIF and Ezrin in colorectal cancer. BMC Cancer 14:145
Chowdhury, Sanjib; Ongchin, Melanie; Sharratt, Elizabeth et al. (2013) Intra-tumoral heterogeneity in metastatic potential and survival signaling between iso-clonal HCT116 and HCT116b human colon carcinoma cell lines. PLoS One 8:e60299
Agarwal, Ekta; Brattain, Michael G; Chowdhury, Sanjib (2013) Cell survival and metastasis regulation by Akt signaling in colorectal cancer. Cell Signal 25:1711-9
Zou, Yi; Howell, Gillian M; Humphrey, Lisa E et al. (2013) Ron knockdown and Ron monoclonal antibody IMC-RON8 sensitize pancreatic cancer to histone deacetylase inhibitors (HDACi). PLoS One 8:e69992
Wang, Jing; Rajput, Ashwani; Kan, Julie L C et al. (2009) Knockdown of Ron kinase inhibits mutant phosphatidylinositol 3-kinase and reduces metastasis in human colon carcinoma. J Biol Chem 284:10912-22
Sawhney, Rajinder S; Liu, Wensheng; Brattain, Michael G (2009) A novel role of ERK5 in integrin-mediated cell adhesion and motility in cancer cells via Fak signaling. J Cell Physiol 219:152-61
Li, Fengzhi; Brattain, Michael G (2006) Role of the Survivin gene in pathophysiology. Am J Pathol 169:1-11