Abstract

The investigators have applied a stable expression cDNA cloning technology to search for novel human oncogenes, which might be undetectable by conventional techniques. By use of this strategy, they have isolated a novel ras- related oncogene, which contains a single base substitution at a position analogous to codon 61, known to activate ras oncogenes. In many human malignancies, oncogenes remain to be identified. The potent transforming properties of the TC21 oncogene, their preliminary findings that additional TC21 oncogenes can be identified in human tumor cells, the ubiquitous expression of ras-related genes in many tissues, and the lack of predictability of the prevalence of previously identified ras oncogenes despite their high frequency in a number of tumor types, all serve to justify systematic efforts to implicate ras related oncogenes in human tumors and determine their prevalence with respect to prototype ras. Approaches will involve immunologic screening combined with SCCP analysis to search for activating lesions affecting these genes in human tumor cell lines and primary tumors. They will develop models in tissue culture and in vivo including transgene targeting to confirm that the genetic alterations observed contribute importantly to the neoplastic process. Finally, they seek to compare their biochemical signaling properties with those of prototype ras, and correlate any differences observed with transforming potency in model cell systems. These studies should aid in elucidating differences in signaling functions which may account for differences in the prevalence of these oncogenes in various tumor types.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA066654-03
Application #
2633898
Study Section
Pathology B Study Section (PTHB)
Program Officer
Spalholz, Barbara A
Project Start
1996-03-25
Project End
1999-12-31
Budget Start
1998-01-01
Budget End
1998-12-31
Support Year
3
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Mount Sinai School of Medicine
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
114400633
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Kimmelman, Alec C; Nunez Rodriguez, Nelson; Chan, Andrew M-L (2002) R-Ras3/M-Ras induces neuronal differentiation of PC12 cells through cell-type-specific activation of the mitogen-activated protein kinase cascade. Mol Cell Biol 22:5946-61
Tolkacheva, T; Chan, A M (2000) Inhibition of H-Ras transformation by the PTEN/MMAC1/TEP1 tumor suppressor gene. Oncogene 19:680-9
Kimmelman, A C; Osada, M; Chan, A M (2000) R-Ras3, a brain-specific Ras-related protein, activates Akt and promotes cell survival in PC12 cells. Oncogene 19:2014-22
Fang, L; Igarashi, M; Leung, J et al. (1999) p21Waf1/Cip1/Sdi1 induces permanent growth arrest with markers of replicative senescence in human tumor cells lacking functional p53. Oncogene 18:2789-97
Osada, M; Tolkacheva, T; Li, W et al. (1999) Differential roles of Akt, Rac, and Ral in R-Ras-mediated cellular transformation, adhesion, and survival. Mol Cell Biol 19:6333-44
Fang, L; Lee, S W; Aaronson, S A (1999) Comparative analysis of p73 and p53 regulation and effector functions. J Cell Biol 147:823-30
Bafico, A; Gazit, A; Wu-Morgan, S S et al. (1998) Characterization of Wnt-1 and Wnt-2 induced growth alterations and signaling pathways in NIH3T3 fibroblasts. Oncogene 16:2819-25
Sugrue, M M; Shin, D Y; Lee, S W et al. (1997) Wild-type p53 triggers a rapid senescence program in human tumor cells lacking functional p53. Proc Natl Acad Sci U S A 94:9648-53
Kimmelman, A; Tolkacheva, T; Lorenzi, M V et al. (1997) Identification and characterization of R-ras3: a novel member of the RAS gene family with a non-ubiquitous pattern of tissue distribution. Oncogene 15:2675-85