Abstract

The small GTPase Ras relays signals from activated cell surface receptors to intracellular signaling pathways. In adenocarcinomas, which originate from polarized epithelial cells, Ras signaling is often deregulated as a result of activating mutations or gene amplification. The mechanisms by which oncogenic Ras elicits transformation of polarized epithelial cells are poorly understood. A major effector pathway of Ras signaling is the Raf-MEK-ERK pathway, which mimics numerous effects of Ras on cells. Expression of activated Ras or Raf in polarized epithelial cells leads to profound alterations in the actin cytoskeleton and associated changes in cellular architecture. The actin eytoskeleton is subject to control by Rho family GTP-binding proteins. Ras or Raf activation in polarized epithelial cells leads to induced expression of the Rho-like protein Rnd3, which appears to function as an endogenous antagonist to Rho proteins. Accordingly, effects of Rnd proteins on cells are counteracted by expression of activated forms of Rho proteins. Virtually nothing is known about effector molecules of Rnd signaling. It is important to identify effectors of Rnd proteins as their expression in cells elicits a phenotype that suggests that they play key roles in cell transformation and developmental processes. In new studies we have identified the Rho GTPase activating protein p190 as a putative effector molecule of Rnd signaling.
Aim 1 is to dissect the interaction between Rnd and p190 proteins and to generate an inhibitory molecule of this interaction.
Aim 2 is to test the hypothesis that the interaction between Rnd and p190 molecules affects functional domains of the p190 molecule, and that p190 is an effector molecule of Rnd proteins in vivo using cells in which p190 has been knocked out.
Aim 3 addresses whether the Rnd-p190 interaction is critical to oncogenic transformation of polarized epithelial by the Ras activated Raf-MEK-ERK pathway using the inhibitory molecule generated in Aim 1. Together, the proposed studies will elucidate mechanisms whereby Ras transforms epithelial cells leading to invasion and metastasis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
7R01CA092354-04
Application #
7016342
Study Section
Physiological Chemistry Study Section (PC)
Program Officer
Perry, Mary Ellen
Project Start
2003-03-01
Project End
2008-02-29
Budget Start
2006-04-14
Budget End
2007-02-28
Support Year
4
Fiscal Year
2006
Total Cost
$371,315
Indirect Cost

  Institution

Name
Children's Hospital Boston
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

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Doehn, Ulrik; Hauge, Camilla; Frank, Scott R et al. (2009) RSK is a principal effector of the RAS-ERK pathway for eliciting a coordinate promotile/invasive gene program and phenotype in epithelial cells. Mol Cell 35:511-22
Frank, Scott R; Hansen, Steen H (2008) The PIX-GIT complex: a G protein signaling cassette in control of cell shape. Semin Cell Dev Biol 19:234-44
Bustos, Rodrigo I; Forget, Marie-Annick; Settleman, Jeffrey E et al. (2008) Coordination of Rho and Rac GTPase function via p190B RhoGAP. Curr Biol 18:1606-11
Frank, Scott R; Adelstein, Molly R; Hansen, Steen H (2006) GIT2 represses Crk- and Rac1-regulated cell spreading and Cdc42-mediated focal adhesion turnover. EMBO J 25:1848-59
Rubenstein, Nicola M; Chan, James F; Kim, Joseph Y et al. (2005) Rnd3/RhoE induces tight junction formation in mammary epithelial tumor cells. Exp Cell Res 305:74-82
Wennerberg, Krister; Forget, Marie-Annick; Ellerbroek, Shawn M et al. (2003) Rnd proteins function as RhoA antagonists by activating p190 RhoGAP. Curr Biol 13:1106-15