Abstract

The Ras and Rho GTPases mediate signaling pathways associated with normal cellular growth control as well as oncogenesis. Although these two groups of GTPases interact with different effector targets, it is now clear that their coordinated activity is responsible for their biological functions in cell proliferation and morphology. The mechanism by which Ras and Rho pathways are coupled is presently unknown, however, a mitogen-promoted cellular complex that forms between a Ras-specific and a Rho-specific GTPase activating protein (GAP) establishes a direct physical connection between Ras and Rho signals. The role of this complex, the RasGAPpl9O complex, in Ras- and Rho-mediated cellular signaling is being investigated. In previous studies from this laboratory, several biochemical properties of p190 have been established, including its association with RasGAP, its activity as a RhoGAP, and its GTPase activity. In addition, using a knockout strategy in mice, a specific biological role for pl9O has been identified in the developing nervous system, where the protein is required for axonal pathfinding at the midline. Moreover, these studies have identified p190 as the single major tyrosine-phosphorylated protein in the brain, suggesting that it performs a general signaling function in the nervous system. In the newly proposed studies, three specific questions will be addressed: l. Where does p190 fit into signaling pathways initiated by extracellular mitogens? 2. How do the identified biochemical properties of p190 and its protein interactions account for its putative function as a coordinator of Ras- and Rho-mediated signaling pathways? 3. What is the role of the RasGAP-pl90 complex in a defined biological system, namely, axon guidance? To address the signaling role of pl9O, the kinase pathways that lead to pl9O phosphorylation will be identified, and the cellular consequences of disrupting the RasGAP-p190 complex will be examined. Protein interactions with pl90 will be investigated by the characterization of several candidate pl9O-interactors identified in a yeast two-hybrid screen. The apparent role of p190 in axonal pathfinding suggests that pl9O might mediate the downstream signals of extracellular axon guidance cues. This will be tested directly in two documented signaling systems associated with axon guidance. The pl90 knockout mice will be used to confirm the biological relevance of such observations. These studies should help to establish a connection between the role of pl9O in Ras- and Rho-mediated signal transduction and a specific biological function that is likely to require the coordinated activities of both Ras and Rho GTPases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA062142-04
Application #
2008388
Study Section
Cellular Biology and Physiology Subcommittee 1 (CBY)
Project Start
1994-01-01
Project End
2001-12-31
Budget Start
1997-01-01
Budget End
1997-12-31
Support Year
4
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Lévay, Magdolna; Settleman, Jeffrey; Ligeti, Erzsébet (2009) Regulation of the substrate preference of p190RhoGAP by protein kinase C-mediated phosphorylation of a phospholipid binding site. Biochemistry 48:8615-23
Jiang, Wei; Betson, Martha; Mulloy, Roseann et al. (2008) p190A RhoGAP is a glycogen synthase kinase-3-beta substrate required for polarized cell migration. J Biol Chem 283:20978-88
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
Chen, Guang-Chao; Lee, Janice Y; Tang, Hong-Wen et al. (2008) Genetic interactions between Drosophila melanogaster Atg1 and paxillin reveal a role for paxillin in autophagosome formation. Autophagy 4:37-45
Betson, Martha; Settleman, Jeffrey (2007) A rho-binding protein kinase C-like activity is required for the function of protein kinase N in Drosophila development. Genetics 176:2201-12
Verdier, Valerie; Johndrow, James E; Betson, Martha et al. (2006) Drosophila Rho-kinase (DRok) is required for tissue morphogenesis in diverse compartments of the egg chamber during oogenesis. Dev Biol 297:417-32
Bradley, William D; Hernandez, Samuel E; Settleman, Jeffrey et al. (2006) Integrin signaling through Arg activates p190RhoGAP by promoting its binding to p120RasGAP and recruitment to the membrane. Mol Biol Cell 17:4827-36
Ligeti, Erzsebet; Settleman, Jeffrey (2006) Regulation of RhoGAP specificity by phospholipids and prenylation. Methods Enzymol 406:104-17
Hakre, Shweta; Tussie-Luna, Maria Isabel; Ashworth, Todd et al. (2006) Opposing functions of TFII-I spliced isoforms in growth factor-induced gene expression. Mol Cell 24:301-8
Matheson, Stephen F; Hu, Kang-Quan; Brouns, Madeleine R et al. (2006) Distinct but overlapping functions for the closely related p190 RhoGAPs in neural development. Dev Neurosci 28:538-50

Showing the most recent 10 out of 15 publications