Abstract

Gastric cancer accounts for approximately 13,000 deaths in the United States. The pathology of gastric cancer is characterized by diverse histology between and within tumors, and the variable presence of necrosis , lymphocytic infiltration, and stroma. In many tumors, the carcinoma cells comprise only a minority of the total population, and it is likely that many genetic alterations are obscured by the overwhelming contamination from normal cells. Similarly, the genetic analysis of potential pre-neoplastic gastric lesions is complicated by the overwhelming numbers of normal mucosal and stromal cells. A new method which can analyze specific and small numbers of cells has been developed in my laboratory to overcome the above difficulties. The method involves the selective destruction and protection of DNA present on a microscope slide by ultraviolet radiation followed by PCR mediated analysis. Preliminary data suggests a resolution of approximately 50 cells with a theoretic ability to analyze one cell. This novel technique will be further developed and employed to detect mutations and loss of heterozygosity of the K-ras, retinoblastoma, p53 genes, and other alterations in gastric cancers. The method should allow the detection of these mutations in any gastric cancer regardless of its stromal contamination. Tumor progression of individual tumors will be directly studied by determining the topography of the primary mutations in adjacent dysplastic, metaplastic, and normal mucosa. The location of each mutation should provide an estimate of their relative contribution to the malignancy. The ultimate goal is a greater understanding of the timing and extent of the molecular events in gastric cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA058704-02
Application #
2099391
Study Section
Pathology B Study Section (PTHB)
Project Start
1993-02-01
Project End
1998-01-31
Budget Start
1994-02-01
Budget End
1995-01-31
Support Year
2
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
University of Southern California
Department
Pathology
Type
Schools of Medicine
DUNS #
041544081
City
Los Angeles
State
CA
Country
United States
Zip Code
90089

  Publications

Blake, C; Tsao, J L; Wu, A et al. (2001) Stepwise deletions of polyA sequences in mismatch repair-deficient colorectal cancers. Am J Pathol 158:1867-70
Ireland, A P; Shibata, D K; Chandrasoma, P et al. (2000) Clinical significance of p53 mutations in adenocarcinoma of the esophagus and cardia. Ann Surg 231:179-87
Tsao, J L; Yatabe, Y; Salovaara, R et al. (2000) Genetic reconstruction of individual colorectal tumor histories. Proc Natl Acad Sci U S A 97:1236-41
Tsao, J L; Yatabe, Y; Markl, I D et al. (2000) Bladder cancer genotype stability during clinical progression. Genes Chromosomes Cancer 29:26-32
Tsao, J L; Tavare, S; Salovaara, R et al. (1999) Colorectal adenoma and cancer divergence. Evidence of multilineage progression. Am J Pathol 154:1815-24
Baker, S M; Harris, A C; Tsao, J L et al. (1998) Enhanced intestinal adenomatous polyp formation in Pms2-/-;Min mice. Cancer Res 58:1087-9
Tsao, J L; Zhang, J; Salovaara, R et al. (1998) Tracing cell fates in human colorectal tumors from somatic microsatellite mutations: evidence of adenomas with stem cell architecture. Am J Pathol 153:1189-200
Shibata, D (1998) The dynamics of early intestinal tumour proliferation: to be or not to be. Cancer Surv 32:181-200
Shibata, D (1997) Molecular tumor clocks and dynamic phenotype. Am J Pathol 151:643-6
Tsao, J L; Davis, S D; Baker, S M et al. (1997) Intestinal stem cell division and genetic diversity. A computer and experimental analysis. Am J Pathol 151:573-9

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