Abstract

To better understand how oncogenes initiate and maintain tumorigenesis, we have developed novel conditional transgenic models of tumorigenesis utilizing the Tet system. During the first grant cycle we have used these models to illustrate that the inactivation of a single oncogene can induce sustained tumor regression. Now, we will focus on further studies to investigate the mechanism by which MYC inactivation induces tumor regression. Our general hypothesis is that upon MYC inactivation, tumor cells recover physiologic programs of proliferative arrest, differentiation, apoptosis and angiogenesis. We know that this process is likely complex and will likely involve both cell autonomous and cell dependent processes, varies depending upon the type of tumor and can be influenced by the genetic context and the particular oncogene examined. In the midst of this complexity, we have chosen to focus on the examination mechanism by which the inactivation of the MYC oncogene induces the regression of MYC-induced T-ALL (lymphoblastic lymphoma). Specifically, we have found circumstances when tumors can escape dependence upon the MYC oncogene. Two observations that we have made may provide mechanistic insight into how MYC inactivation induces tumor regression and how tumors can escape dependence upon MYC. First, we found that lymphomas that have escaped dependence upon MYC appear to frequently possess already or have already acquired specific chromosomal abnormalities detected by Spectral Karyotypic Analysis (SKY). We have localized by array Comparative Genomic Hybridization (CGH) and Fluorescent In Situ Hybridization (FISH) a chromosomal translocation and deletion in chromosome 3 associated with tumor escape and now identified a candidate gene product. We hypothesize that this gene product facilitates the ability of tumors to escape from MYC dependence, which we now propose to evaluate. Second, we have found that loss of p53 function greatly impairs sustained tumor regression upon MYC inactivation. We hypothesize that restoration of p53 will permit MYC inactivation to induce sustained tumor regression. We present preliminary results that the loss of p53 impairs apoptosis and inhibition of angiogenesis associated with MYC inactivation, which we will now confirm. We will validate the relevance of our results to human tumors by taking advantage of our access a lymphoma repository as well as human T-ALL cell lines. The results of these studies will provide novel insights into the mechanism of """"""""oncogene addiction"""""""" and will be useful towards the development of new treatments for T-ALL/lymphoblastic lymphoma.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA089305-09
Application #
7769908
Study Section
Cancer Genetics Study Section (CG)
Program Officer
Mietz, Judy
Project Start
2000-12-01
Project End
2012-02-29
Budget Start
2010-03-01
Budget End
2011-02-28
Support Year
9
Fiscal Year
2010
Total Cost
$399,339
Indirect Cost

  Institution

Name
Stanford University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Casey, Stephanie C; Tong, Ling; Li, Yulin et al. (2016) MYC regulates the antitumor immune response through CD47 and PD-L1. Science 352:227-31
Shroff, Emelyn H; Eberlin, Livia S; Dang, Vanessa M et al. (2015) MYC oncogene overexpression drives renal cell carcinoma in a mouse model through glutamine metabolism. Proc Natl Acad Sci U S A 112:6539-44
Casey, Stephanie C; Vaccari, Monica; Al-Mulla, Fahd et al. (2015) The effect of environmental chemicals on the tumor microenvironment. Carcinogenesis 36 Suppl 1:S160-83
Yetil, Alper; Anchang, Benedict; Gouw, Arvin M et al. (2015) p19ARF is a critical mediator of both cellular senescence and an innate immune response associated with MYC inactivation in mouse model of acute leukemia. Oncotarget 6:3563-77
Casey, Stephanie C; Amedei, Amedeo; Aquilano, Katia et al. (2015) Cancer prevention and therapy through the modulation of the tumor microenvironment. Semin Cancer Biol 35 Suppl:S199-S223
Gabay, Meital; Li, Yulin; Felsher, Dean W (2014) MYC activation is a hallmark of cancer initiation and maintenance. Cold Spring Harb Perspect Med 4:
Li, Y; Casey, S C; Felsher, D W (2014) Inactivation of MYC reverses tumorigenesis. J Intern Med 276:52-60
Casey, Stephanie C; Li, Yulin; Felsher, Dean W (2014) An essential role for the immune system in the mechanism of tumor regression following targeted oncogene inactivation. Immunol Res 58:282-91
Casey, Stephanie C; Bellovin, David I; Felsher, Dean W (2013) Noncanonical roles of the immune system in eliciting oncogene addiction. Curr Opin Immunol 25:246-58
Bisikirska, B C; Adam, S J; Alvarez, M J et al. (2013) STK38 is a critical upstream regulator of MYC's oncogenic activity in human B-cell lymphoma. Oncogene 32:5283-91

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