Abstract

Familial cancer syndromes provide a unique opportunity to examine the mechanism of inherited susceptibility to cancer, as well as the more general processes involved in the development of malignancy. Our laboratory is studying a family with Li-Fraumeni syndrome, which is characterized by the development of diverse neoplasms as multiple primary tumors within single individuals. Particular emphasis has been placed on the role of oncogenes in the development of these tumors. Oncogenes are genes involved in the development of malignancy. Oncogenes derive from normal cellular genes, termed proto-oncogenes, when the latter are altered by point mutation, deletion, rearrangement, or amplification. Evidence for the involvement of oncogenes in non-inherited human malignancy, as well as in inherited predisposition to cancer, continues to accumulate. The normal functions of several proto-oncogenes have been elucidated; they are involved in normal cell growth, division, metabolism, and/or differentiation. Proto-oncogene products functions as growth factors or growth factor receptors, tyrosine-specific or serine/threonine-specific protein kinases, G-proteins exhibiting GTPase activities, or nuclear proteins participating in DNA synthesis. In this application, we propose to study the involvement of proto-oncogene(s), oncogene(s), and suppressor genes in the predisposition of the members of a cancer-prone family. Our goal is to identify and characterize the primary genetic defect shared in this family; however, in this process, we may have uncovered certain oncogenes which may represent secondary and tertiary genetic defects. We will (1) continue to analyse two transforming genes derived from the normal skin fibroblasts of two affected family members, the proband, and his brother, (2) attempt to identify the transforming gene(s) in normal skin fibroblasts of other family members, and (3) assess the possible involvement of a suppressor gene, Rb, in the family genetic defect. The oncogene will be molecularly cloned and compared to their normal counterparts. The genetic defect will be defined by DNA sequence analysis and site-directed mutagenesis. Specific antibodies will be raised to synthetic peptides and the biosynthesis and subcellular localization of the oncogene product will be examined. Attempts will be made to characterize the oncogene product and to explore its function. RNA profile of the Rb gene in normal skin fibroblasts of the family members will be examined by Northern analysis. Rb DNA RFLPs will be detected by Southern hybridization.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
7R01CA045158-09
Application #
2091764
Study Section
Experimental Virology Study Section (EVR)
Project Start
1986-09-01
Project End
1995-01-09
Budget Start
1994-09-01
Budget End
1995-01-09
Support Year
9
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Surgery
Type
Schools of Medicine
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Xu, Liang; Huang, Cheng-Cheng; Huang, Weiqun et al. (2002) Systemic tumor-targeted gene delivery by anti-transferrin receptor scFv-immunoliposomes. Mol Cancer Ther 1:337-46
Sherif, Z A; Nakai, S; Pirollo, K F et al. (2001) Downmodulation of bFGF-binding protein expression following restoration of p53 function. Cancer Gene Ther 8:771-82
Xu, L; Pirollo, K F; Chang, E H (2001) Tumor-targeted p53-gene therapy enhances the efficacy of conventional chemo/radiotherapy. J Control Release 74:115-28
Xu, L; Tang, W H; Huang, C C et al. (2001) Systemic p53 gene therapy of cancer with immunolipoplexes targeted by anti-transferrin receptor scFv. Mol Med 7:723-34
Pirollo, K F; Bouker, K B; Chang, E H (2000) Does p53 status influence tumor response to anticancer therapies? Anticancer Drugs 11:419-32
Xu, L; Pirollo, K F; Tang, W H et al. (1999) Transferrin-liposome-mediated systemic p53 gene therapy in combination with radiation results in regression of human head and neck cancer xenografts. Hum Gene Ther 10:2941-52
Pirollo, K F; Hao, Z; Rait, A et al. (1997) Evidence supporting a signal transduction pathway leading to the radiation-resistant phenotype in human tumor cells. Biochem Biophys Res Commun 230:196-201
Xu, L; Pirollo, K F; Chang, E H (1997) Transferrin-liposome-mediated p53 sensitization of squamous cell carcinoma of the head and neck to radiation in vitro. Hum Gene Ther 8:467-75
Pirollo, K F; Hao, Z; Rait, A et al. (1997) p53 mediated sensitization of squamous cell carcinoma of the head and neck to radiotherapy. Oncogene 14:1735-46
Srivastava, S; Wang, S; Tong, Y A et al. (1993) Several mutant p53 proteins detected in cancer-prone families with Li-Fraumeni syndrome exhibit transdominant effects on the biochemical properties of the wild-type p53. Oncogene 8:2449-56

Showing the most recent 10 out of 16 publications