Abstract

Colorectal carcinoma is the second greatest cause of death in the United States among all types of neoplasms. The mortality of this disease is the result of regional and systemic metastasis. Although a variety of biological and biochemical properties that determine the metastatic capability of mammary carcinoma, lung carcinoma, melanoma and lymphosarcoma have been elucidated in experimental animal model systems, little is known about the mechanisms and determinants of colorectal carcinoma metastasis in cancer patients because of the lack of a suitable experimental model. Since the most commonly use therapeutic procedure for colorectal carcinoma is surgery, a relatively large number of fresh tumor specimens, together with comprehensive patient records, are available at the M.D. Anderson Hospital. In the proposed project, we will develop a rapid, micro-scale analytical method for the examination of biochemically definable cell surface properties in colorectal cancer which have been proposed to be related to metastatic behavior of tumor cells in experimental systems. These include various types of cell surface glycoproteins, extracellular proteoglycans, and hydrolytic enzymes responsible for the destruction of tissue integrity, such as heparanase and type IV collagenase. When relatively large tumor tissues are available, the targeted molecules will be purified from them. Antibodies (monoclonal or polyclonal) against the e molecules together with specific histochemical agents for glycoconjugates will be histochemically utilized in order to examine localization and intercellular heterogeneity in the distribution of the molecules. The results of this proposed study will provide new information concerning the cell surface properties of the highly metastatic subpopulation of primary colorectal tumors. The development of this technology could serve as a useful tool for prognosticating matastasis of this disease. Also, the results may be a basis for the study of specific antimentastatic therapy which can be applied in concert with other therapeutic modalities of the primary tumor.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA039319-01
Application #
3178154
Study Section
Pathology B Study Section (PTHB)
Project Start
1985-04-01
Project End
1988-03-31
Budget Start
1985-04-01
Budget End
1986-03-31
Support Year
1
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Type
Hospitals
DUNS #
001910777
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Izumi, Y; Taniuchi, Y; Tsuji, T et al. (1995) Characterization of human colon carcinoma variant cells selected for sialyl Lex carbohydrate antigen: liver colonization and adhesion to vascular endothelial cells. Exp Cell Res 216:215-21
Lotan, R; Ito, H; Yasui, W et al. (1994) Expression of a 31-kDa lactoside-binding lectin in normal human gastric mucosa and in primary and metastatic gastric carcinomas. Int J Cancer 56:474-80
Lotan, R; Belloni, P N; Tressler, R J et al. (1994) Expression of galectins on microvessel endothelial cells and their involvement in tumour cell adhesion. Glycoconj J 11:462-8
Dohi, D F; Sutton, R C; Frazier, M L et al. (1993) Regulation of sialomucin production in colon carcinoma cells. J Biol Chem 268:10133-8
Matsushita, Y; Hoff, S D; Nudelman, E D et al. (1991) Metastatic behavior and cell surface properties of HT-29 human colon carcinoma variant cells selected for their differential expression of sialyl-dimeric Le(x)-antigen. Clin Exp Metastasis 9:283-99
Irimura, T; Wynn, D M; Hager, L G et al. (1991) Human colonic sulfomucin identified by a specific monoclonal antibody. Cancer Res 51:5728-35
Irimura, T; Matsushita, Y; Sutton, R C et al. (1991) Increased content of an endogenous lactose-binding lectin in human colorectal carcinoma progressed to metastatic stages. Cancer Res 51:387-93
Irimura, T; Matsushita, Y; Hoff, S D et al. (1991) Ectopic expression of mucins in colorectal cancer metastasis. Semin Cancer Biol 2:129-39
Matsushita, Y; Nakamori, S; Seftor, E A et al. (1991) Human colon carcinoma cells with increased invasive capacity obtained by selection for sialyl-dimeric LeX antigen. Exp Cell Res 196:20-5
Lotan, R; Matsushita, Y; Ohannesian, D et al. (1991) Lactose-binding lectin expression in human colorectal carcinomas. Relation to tumor progression. Carbohydr Res 213:47-57

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