Abstract

The overall objective of this grant is to investigate the structure and function of viral and cellular mos proteins. Our previously published studies have provided convincing evidence that the viral mos protein is a serine/threonine protein kinase. Furthermore, our studies with various mutants of the viral mos gene have shown an absolute correlation between the cellular transformation function of the activated oncogene and its associated protein kinase function. This correlation indicates that the serine/threonine kinase function of v-mos proteins plays an essential role in malignant transformation induced by Moloney mouse sarcoma virus. We proposed to investigate how the p37env-mos protein kinase activity is regulated via phosphorylation and how it relates to cell cycle regulation. We have identified the c-mos gene product (p43c-mos) in germ cells from mouse testes. Western blotting experiments have detected a similar size c- mos protein in somatic cells. Further studies are underway on the struc- ture and function of this protein, and to determine whether it may be functionally associated with components of the maturation promotion complex (MPF).
The specific aims i nclude: 1) Characterize the components of two complexes (500-kDa and 98 kDa) that house p37 env-mos in chronically transformed cells; 2) Characterize the interaction of p37env-mos with p34cdc2 protein kinase (a component of MPF) detected in 500-kDa size complexes from chronically transformed (MoMuSV 3T3 cells; 3) Determine whether p37env-mos and p43c-mos phosphorylate cyclin (a component of MPF), and other mitotic proteins; 4) Study the cell cycle regulation of the p37env-mos kinase by phosphorylation; 5) Investigate the role of protein kinase C and other cellular kinases including p34cdc2 of MPF in the activation of p37env-mos kinase; 6) Search for important substrates for p37env-mos kinase; 7) Determine the biochemical basis of vimentin altera- tion by p37env-mos; 8) Characterize the testicular and somatic cell forms of p43c-mos; 9) Determine the cell cycle regulation of somatic p43c-mos and its possible association with components of MPF; 10) Clone the v-mos and c- mos genes in a baculovirus vector, which will allow the production of higher amounts of active mos proteins for further biochemical studies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA045125-04A1
Application #
3188104
Study Section
Experimental Virology Study Section (EVR)
Project Start
1986-09-30
Project End
1995-06-30
Budget Start
1990-07-01
Budget End
1991-06-30
Support Year
4
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
University of Texas MD Anderson Cancer Center
Department
Type
Other Domestic Higher Education
DUNS #
001910777
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Pham, C D; Vuyyuru, V B; Yang, Y et al. (1999) Evidence for an important role of serine 16 and its phosphorylation in the stabilization of c-Mos. Oncogene 18:4287-94
Liu, H; Vuyyuru, V B; Pham, C D et al. (1999) Evidence of an interaction between Mos and Hsp70: a role of the Mos residue serine 3 in mediating Hsp70 association. Oncogene 18:3461-70
Yang, Y; Pham, C D; Vuyyuru, V B et al. (1998) Evidence of a functional interaction between serine 3 and serine 25 Mos phosphorylation sites. A dominant inhibitory role of serine 25 phosphorylation on Mos protein kinase. J Biol Chem 273:15946-53
Yang, Y; Pham, C D; Arlinghaus, R B et al. (1998) Elevated level of cyclin D1 in mos-transformed cells. Int J Oncol 12:1199-202
Singh, B; Arlinghaus, R B (1997) Mos and the cell cycle. Prog Cell Cycle Res 3:251-9
Gao, C; Arlinghaus, R B; Singh, B (1996) Further characterization of the c-mos transcript and its cell cycle specific expression in NIH3T3 cells. Oncogene 12:1571-6
Yang, Y; Herrmann, C H; Arlinghaus, R B et al. (1996) Inhibition of v-Mos kinase activity by protein kinase A. Mol Cell Biol 16:800-9
Pham, C D; Arlinghaus, R B; Zheng, C F et al. (1995) Characterization of MEK1 phosphorylation by the v-Mos protein. Oncogene 10:1683-8
Bai, W; Arlinghaus, R B; Singh, B (1993) Association of v-Mos with soluble vimentin in vitro and in transformed cells. Oncogene 8:2207-12
Bai, W; Singh, B; Yang, Y et al. (1992) Evidence for interaction between v-Mos and a p34cdc2 isoform, p35cdk. Oncogene 7:1757-63

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