Abstract

The broad, long-term objectives of this proposal are to understand how growth factors control the proliferation of animal cells. We wish to define at a molecular and biochemical level the mechanisms by which growth factor signals are transmitted to the nucleus to regulate the transcription of genes involved in the control of cell proliferation. And we would like to understand the basis for the specificity of action of growth factors-how different growth factors elicit distinct biological responses from cells. Our principal experimental focus is the proto-oncogene c-fos, which is rapidly and transiently induced at the transcriptional level as a primary response to activation of several growth factor signal transduction pathways. In this proposal we address a specific model for how such signals activate transcription of the c-fos gene. Our previous work has demonstrated that two different signal transduction pathways act through different protein complexes bound to a common cis-acting regulatory element, the serum response element (SRE), in the c-fos gene. We propose that each signal transduction pathway that activates c-fos transcription via the SRE acts through a distinct protein complex, with one shared component, the transcription factor SRF, and one or more unique accessory proteins. We have three specific aims. First, using mutagenesis of the c-fos promoter coupled with gene transfer assays, we wish to identify new sequence elements in the c-fos promoter that cooperate with the SRE by providing binding sites for putative accessory factors. Second, using biochemical and molecular approaches, we wish to characterize a series of proteins that we believe may function as accessory proteins for SRF. Third, we wish to begin a detailed biochemical analysis of the organization of the protein complexes that form among these proteins and of the function of these complexes in vivo. We believe that this data will contribute to our understanding of how proliferative signals are processed and how the cell distinguishes among signals with different biological activities. Understanding these control mechanisms will aid in the design of novel therapeutic strategies to deal with proliferative disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA045642-07
Application #
3188803
Study Section
Molecular Biology Study Section (MBY)
Project Start
1987-09-17
Project End
1997-08-31
Budget Start
1993-09-01
Budget End
1994-08-31
Support Year
7
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Cold Spring Harbor Laboratory
Department
Type
DUNS #
065968786
City
Cold Spring Harbor
State
NY
Country
United States
Zip Code
11724

  Publications

Vignais, M L; Gilman, M (1999) Distinct mechanisms of activation of Stat1 and Stat3 by platelet-derived growth factor receptor in a cell-free system. Mol Cell Biol 19:3727-35
Harrison, D A; McCoon, P E; Binari, R et al. (1998) Drosophila unpaired encodes a secreted protein that activates the JAK signaling pathway. Genes Dev 12:3252-63
Grueneberg, D A; Henry, R W; Brauer, A et al. (1997) A multifunctional DNA-binding protein that promotes the formation of serum response factor/homeodomain complexes: identity to TFII-I. Genes Dev 11:2482-93
Simon, K J; Grueneberg, D A; Gilman, M (1997) Protein and DNA contact surfaces that mediate the selective action of the Phox1 homeodomain at the c-fos serum response element. Mol Cell Biol 17:6653-62
Vignais, M L; Sadowski, H B; Watling, D et al. (1996) Platelet-derived growth factor induces phosphorylation of multiple JAK family kinases and STAT proteins. Mol Cell Biol 16:1759-69
Grueneberg, D A; Simon, K J; Brennan, K et al. (1995) Sequence-specific targeting of nuclear signal transduction pathways by homeodomain proteins. Mol Cell Biol 15:3318-26
Harrison, D A; Binari, R; Nahreini, T S et al. (1995) Activation of a Drosophila Janus kinase (JAK) causes hematopoietic neoplasia and developmental defects. EMBO J 14:2857-65
Natesan, S; Gilman, M (1995) YY1 facilitates the association of serum response factor with the c-fos serum response element. Mol Cell Biol 15:5975-82
Lee, G; Gilman, M (1994) Dual modes of control of c-fos mRNA induction by intracellular calcium in T cells. Mol Cell Biol 14:4579-87
Sadowski, H B; Shuai, K; Darnell Jr, J E et al. (1993) A common nuclear signal transduction pathway activated by growth factor and cytokine receptors. Science 261:1739-44

Showing the most recent 10 out of 21 publications