Abstract

Colorectal carcinoma is the second most common cause of cancer deaths in the U.S.A. At present, prognostication is based mainly on pathologic staging (Dukes' classification). Molecular probes have not been applied in large groups of patients to determine if molecular markers can be used to predict clinical outcome and assist in selecting appropriate therapy. The utility of probes in defining the pathogenesis of primary human colorectal carcinoma has not been studied extensively. We propose to evaluate a select group of markers in unique subsets of patients with colorectal carcinoma whose tumors have metastatic phenotype as defined by pathologic and clinical criteria. Our long-term goal is to find molecular probes which will assist in providing appropriate therapy by identifying patients with high risk of metastases. Our hypothesis to be tested is that primary colorectal carcinomas with propensity to metastasize (i.e. which show metastatic phenotype) demonstrate interrelated pathogenetic cellular markers, including mutation of the c-Ki-ras gene with expression of the mutant ras p21 gene product, DNA aneuploidy, and high activity of ornithine decarboxylase with high concentrations of polyamines and rapid tumor cell proliferation.
Our specific aims are: (1) To begin collaborative exchange of colorectal carcinoma specimens from the tissue banks of the Bowel Tumor Working Group at The Johns Hopkins Hospital and St. Mark's Hospital, London, England. This will provide adequate pathologically well-defined populations of prospectively identified patients with definable clinical outcomes for studies of the potential markers described in Specific Aims 2 through 4. (2) To assess colorectal carcinomas for mutation of c-Ki-ras, c-Ha-ras, and N-ras genes by hybridization assay and determine ras gene product p21 expression by immunoblotting, enzyme-linked immunosorbent assay, and immunohistochemistry using a panel of monoclonal and polyclonal antibodies against native and mutated p21. (3) To assess colorectal carcinomas for DNA aneuploidy by flow cytometry. (4) To assess colorectal carcinomas for activity of ornithine decarboxylase by radiometric assay, concentrations of polyamines by high-pressure liquid chromotography, and cell proliferation by immunohistochemistry with monoclonal antibody Ki-67 against proliferating cells. (5) To analyze using appropriate statistical methods the data for the various markers in relation to each other as well as to the pathologic features of the colorectal carcinomas, the presence of metastases, and patient survival.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA047527-03
Application #
3191214
Study Section
Special Emphasis Panel (SRC (50))
Project Start
1988-04-01
Project End
1992-01-09
Budget Start
1990-04-01
Budget End
1992-01-09
Support Year
3
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

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Rashid, A; Pizer, E S; Moga, M et al. (1997) Elevated expression of fatty acid synthase and fatty acid synthetic activity in colorectal neoplasia. Am J Pathol 150:201-8
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Wu, T T; Rezai, B; Rashid, A et al. (1997) Genetic alterations and epithelial dysplasia in juvenile polyposis syndrome and sporadic juvenile polyps. Am J Pathol 150:939-47
Rashid, A; Hamilton, S R (1997) Genetic alterations in sporadic and Crohn's-associated adenocarcinomas of the small intestine. Gastroenterology 113:127-35
Nicolaides, N C; Palombo, F; Kinzler, K W et al. (1996) Molecular cloning of the N-terminus of GTBP. Genomics 31:395-7
Liu, B; Parsons, R; Papadopoulos, N et al. (1996) Analysis of mismatch repair genes in hereditary non-polyposis colorectal cancer patients. Nat Med 2:169-74
Liu, B; Farrington, S M; Petersen, G M et al. (1995) Genetic instability occurs in the majority of young patients with colorectal cancer. Nat Med 1:348-52

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