Abstract

The mechanisms whereby integrins signal to the interior of the cell are largely unknown. Evidence indicates that tyrosine phosphorylation of intracellular proteins may be a key event p130Cas (Cas) is one of the prominent proteins that are tyrosine-phosphorylated upon integrin- mediated cell attachment. Cas is an SH3-domain containing protein that has a cluster of putative SH2-binding sites; Cas also has several proline-rich regions that are candidates for SH3-binding sites. Preliminary results suggest that Cas is important in integrin signaling; Cas bound to multiple SH2-domain containing signaling proteins upon integrin ligand binding, cell adhesion resulted in changes in the subcellular localization of Cas, and Cas antisense mRNA expression reduced integrin-dependent MAP kinase activation. The studies proposed here will explore the molecular mechanisms and significance of Cas in integrin signaling. Because Cas has no known enzymatic activity, Cas most likely exerts its signaling effects through protein-protein interactions. It is thus important to identify the proteins that interact with Cas. The first part of the study will characterize the protein-protein interactions between Cas and known SH2-domain containing proteins.
This aim also includes an analysis of the signaling molecules known to interact with the SH2- proteins present in the Cas signaling complex. Next, novel signaling proteins interacting with Cas in an adhesion- dependent manner will be identified and characterized. These experiments use two powerful genetic systems suitable for direct cloning of proteins that interact with tyrosine-phosphorylated Cas. In another approach, proteins interacting with Cas in an adhesion-dependent manner regardless of the phosphorylation status of Cas will be identified. The functional effects of Cas on integrin signaling will be studied. These experiments will be designed based on what is currently known about the Cas-associated molecules, and on the outcome of experiments described above. Cell lines expressing reduced levels of Cas have been generated by using antisense technology, and will be used in these studies. These studies will provide insights into the role of Cas in intracellular signaling of integrins. This work should also lead to a better understanding of mechanisms whereby extracellular matrix influences cell behavior, such as normal growth regulation and adhesion dependency.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA071560-03
Application #
2733254
Study Section
Pathobiochemistry Study Section (PBC)
Program Officer
Mohla, Suresh
Project Start
1996-07-10
Project End
1999-12-31
Budget Start
1998-07-01
Budget End
1999-12-31
Support Year
3
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Sanford-Burnham Medical Research Institute
Department
Type
DUNS #
009214214
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Nasertorabi, Fariborz; Tars, Kaspars; Becherer, Kathleen et al. (2006) Molecular basis for regulation of Src by the docking protein p130Cas. J Mol Recognit 19:30-8
Briknarova, Klara; Nasertorabi, Fariborz; Havert, Marnie L et al. (2005) The serine-rich domain from Crk-associated substrate (p130cas) is a four-helix bundle. J Biol Chem 280:21908-14
Nasertorabi, Fariborz; Alonso, Andres; Rogers, Scott W et al. (2005) Crystallization of the SH2-binding site of p130Cas in complex with Lck, a Src-family kinase. Acta Crystallogr Sect F Struct Biol Cryst Commun 61:174-7
Nasertorabi, Fariborz; Garcia-Guzman, Miguel; Briknarova, Klara et al. (2004) Organization of functional domains in the docking protein p130Cas. Biochem Biophys Res Commun 324:993-8
Abassi, Yama A; Vuori, Kristiina (2002) Tyrosine 221 in Crk regulates adhesion-dependent membrane localization of Crk and Rac and activation of Rac signaling. EMBO J 21:4571-82
Aoudjit, F; Vuori, K (2001) Matrix attachment regulates Fas-induced apoptosis in endothelial cells: a role for c-flip and implications for anoikis. J Cell Biol 152:633-43
Garcia-Guzman, M; Larsen, E; Vuori, K (2000) The proto-oncogene c-Cbl is a positive regulator of Met-induced MAP kinase activation: a role for the adaptor protein Crk. Oncogene 19:4058-65
Aoudjit, F; Vuori, K (2000) Engagement of the alpha2beta1 integrin inhibits Fas ligand expression and activation-induced cell death in T cells in a focal adhesion kinase-dependent manner. Blood 95:2044-51
Garcia-Guzman, M; Dolfi, F; Zeh, K et al. (1999) Met-induced JNK activation is mediated by the adapter protein Crk and correlates with the Gab1 - Crk signaling complex formation. Oncogene 18:7775-86
Blaukat, A; Ivankovic-Dikic, I; Gronroos, E et al. (1999) Adaptor proteins Grb2 and Crk couple Pyk2 with activation of specific mitogen-activated protein kinase cascades. J Biol Chem 274:14893-901

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