Abstract

GTP-binding proteins are key switches in signaling pathways that regulate critical cellular functions such as growth and differentiation. Ras, which serves as a prototype for GTP-binding is constitutively activated in a large number of cancers including those of the pancreas, bladder, colon, and lung. The long-term goal of this research is to interfere with the oncogenic forms of Ras in human disease by understanding its cycling. Because oncogenic Ras relies on its intrinsic ability to hydrolyze and exchange GTP, the primary goal of this research proposal is to better our understanding of Ras cycling between the active and inactive states by revealing structures of intermediates of the reactions of GTP hydrolysis and guanine nucleotide exchange. Screening of drugs that will stabilize a non-signaling conformation of oncogenic Ras will be also performed. This proposal is based on findings that altering the flexibility of a hinge region stabilizes structures of Ras that are normally transient. Using this approach, two structures of intermediates along the path for GTP hydrolysis were stabilized as well as an open non-signaling conformation, which is also adopted by the native protein.
The first aim of this proposal tests the hypothesis that the open conformation of Ras mimics the structure of an intermediate for nucleotide exchange and the structu-e of an unappreciated native conformation. Additional structures of intermediates for Ras cycling will be generated by altering the flexibility of another hinge region. The generated mutants will be studied using a combination of structural, molecular dynamics, biochemical, and in vivo techniques.
The second aim tests the hypothesis that Rho- family members and trimeric G-proteins do not follow the Ras path of GTP hydrolysis and nucleotide exchange despite strong sequence homology.
The third aim uses biophysical, structural, and cellular approaches to study how small molecules identified by screening the NCI database interact with the open non-signaling conformation and inhibit oncogenic Ras in a pancreatic cancer model system. The outcome of the proposed research should improve our understanding of the regulation of key signaling proteins and our ability to interfere with their action in human diseases. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA115611-01A2
Application #
7197417
Study Section
Macromolecular Structure and Function B Study Section (MSFB)
Program Officer
Blair, Donald G
Project Start
2007-05-04
Project End
2011-02-28
Budget Start
2007-05-04
Budget End
2008-02-29
Support Year
1
Fiscal Year
2007
Total Cost
$232,711
Indirect Cost

  Institution

Name
State University New York Stony Brook
Department
Physiology
Type
Schools of Medicine
DUNS #
804878247
City
Stony Brook
State
NY
Country
United States
Zip Code
11794

  Publications

Privette Vinnedge, Lisa M; Kappes, Ferdinand; Nassar, Nicolas et al. (2013) Stacking the DEK: from chromatin topology to cancer stem cells. Cell Cycle 12:51-66
San Luis, Boris; Nassar, Nicolas; Carpino, Nick (2013) New insights into the catalytic mechanism of histidine phosphatases revealed by a functionally essential arginine residue within the active site of the Sts phosphatases. Biochem J 453:27-35
San Luis, Boris; Sondgeroth, Ben; Nassar, Nicolas et al. (2011) Sts-2 is a phosphatase that negatively regulates zeta-associated protein (ZAP)-70 and T cell receptor signaling pathways. J Biol Chem 286:15943-54
Nassar, Nicolas; Singh, Kavita; Garcia-Diaz, Miguel (2010) Structure of the dominant negative S17N mutant of Ras. Biochemistry 49:1970-4
Jakoncic, Jean; Sondgeroth, Benjamin; Carpino, Nick et al. (2010) The 1.35 A resolution structure of the phosphatase domain of the suppressor of T-cell receptor signaling protein in complex with sulfate. Acta Crystallogr Sect F Struct Biol Cryst Commun 66:643-7
Carpino, Nick; Chen, Yunting; Nassar, Nicolas et al. (2009) The Sts proteins target tyrosine phosphorylated, ubiquitinated proteins within TCR signaling pathways. Mol Immunol 46:3224-31
Chen, Yunting; Jakoncic, Jean; Parker, Kathlyn A et al. (2009) Structures of the phosphorylated and VO(3)-bound 2H-phosphatase domain of Sts-2. Biochemistry 48:8129-35
Ford, Bradley; Boykevisch, Sean; Zhao, Chen et al. (2009) Characterization of a Ras mutant with identical GDP- and GTP-bound structures . Biochemistry 48:11449-57
Chen, Yunting; Jakoncic, Jean; Carpino, Nick et al. (2009) Structural and functional characterization of the 2H-phosphatase domain of Sts-2 reveals an acid-dependent phosphatase activity. Biochemistry 48:1681-90
Chen, Yunting; Jakoncic, Jean; Wang, Jin et al. (2008) Structural and functional characterization of the c-terminal domain of the ecdysteroid phosphate phosphatase from bombyx mori reveals a new enzymatic activity. Biochemistry 47:12135-45