Abstract

Cancer development involves alterations in both cellular protooncogenes and in tumor suppressor genes. In vitro systems have provided molecular details of the pathways potentially disrupted in this multi-step process. However, understanding tumorigenesis of diverse cell types clearly requires the use of in vivo systems such as transgenic and """"""""knock-out"""""""" mouse models. The applicant has established transgenic tumor models based on the fact that tumor virus oncoproteins such as SV40 T antigen (T-Ag) inactivate key cellular growth regulatory proteins, including p53 and pRb. Using tissue-specific promoters to express wild-type and mutant T-Ags, we have explored the function of these tumor suppressors within the animal. Using transgenic and knock-out animals we recently showed that, in brain epithelial cells, p53-dependent apoptosis is induced in response to aberrant proliferation resulting in part from inactivation of the Rb family proteins. Loss of p53 function results in tumor progression coincident with a reduction in apoptosis. Moreover, inactivation of p53 is selected for as tumors develop in a p53 +/-background. These results suggest a mechanism by which p53 loss contributes to tumor progression in human cancer. Her continuation of these studies proposed herein includes the following aims: (1) To delineate key regulatory components of the p53-dependent apoptosis pathway. Directed studies involving crosses or chimera analyses with existing knockout strains will determine whether known or implicated factors are involved (e.g., p21, bax, mdm2, gadd45, E2F1). Further, genetic analyses of tumors arising in the p53 +/-mice will be used to determine whether those that have retained functional p53 have inactivated other components of the pathway, novel or known. (2) To determine the contribution of genetic instability to tumor progression, comparative genome analysis and simple sequence length polymorphism analysis of p53 _ and p53 - tumors will be performed to determine the extent and consistency of genetic aberration. (3) To determine whether p53 dependent apoptosis has a similar role in other cell types which display a high frequency of p53 mutation of human cancer. Here, studies are proposed for mammary epithelial cells. For further cell-specific studies, tissue specific inactivation of p53 by somatic delivery of a dominant negative mutant of p53 will be tested.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA046283-14
Application #
6137460
Study Section
Experimental Virology Study Section (EVR)
Program Officer
Mietz, Judy
Project Start
1988-03-01
Project End
2001-12-31
Budget Start
2000-02-02
Budget End
2000-12-31
Support Year
14
Fiscal Year
2000
Total Cost
$387,228
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Biochemistry
Type
Schools of Medicine
DUNS #
078861598
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Song, Yurong; Zhang, Qian; Kutlu, Burak et al. (2013) Evolutionary etiology of high-grade astrocytomas. Proc Natl Acad Sci U S A 110:17933-8
Song, Yurong; Gilbert, Debra; O'Sullivan, T Norene et al. (2013) Carcinoma initiation via RB tumor suppressor inactivation: a versatile approach to epithelial subtype-dependent cancer initiation in diverse tissues. PLoS One 8:e80459
Lu, Xiangdong; Yang, Chunyu; Yin, Chaoying et al. (2011) Apoptosis is the essential target of selective pressure against p53, whereas loss of additional p53 functions facilitates carcinoma progression. Mol Cancer Res 9:430-9
DelBove, Jessica; Kuwahara, Yasumichi; Mora-Blanco, E Lorena et al. (2009) Inactivation of SNF5 cooperates with p53 loss to accelerate tumor formation in Snf5(+/-);p53(+/-) mice. Mol Carcinog 48:1139-48
Lu, Xiangdong; Yang, Chunyu; Hill, Reginald et al. (2008) Inactivation of gadd45a sensitizes epithelial cancer cells to ionizing radiation in vivo resulting in prolonged survival. Cancer Res 68:3579-83
Herschkowitz, Jason I; Simin, Karl; Weigman, Victor J et al. (2007) Identification of conserved gene expression features between murine mammary carcinoma models and human breast tumors. Genome Biol 8:R76
Chai, Jingjing; Lu, Xiangdong; Godfrey, Virginia et al. (2007) Tumor-specific cooperation of retinoblastoma protein family and Snf5 inactivation. Cancer Res 67:3002-9
Nister, Monica; Tang, Mengjia; Zhang, Xiao-Qun et al. (2005) p53 must be competent for transcriptional regulation to suppress tumor formation. Oncogene 24:3563-73
Hill, Reginald; Song, Yurong; Cardiff, Robert D et al. (2005) Heterogeneous tumor evolution initiated by loss of pRb function in a preclinical prostate cancer model. Cancer Res 65:10243-54
Simin, K; Hill, R; Song, Y et al. (2005) Deciphering cancer complexities in genetically engineered mice. Cold Spring Harb Symp Quant Biol 70:283-90

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