Abstract

Metastasis (i.e., tumor spread) is the major obstacle to cancer cure. The metastatic process consists of many steps. If the cascade of events is interrupted at any step, metastasis will not occur. Eristostatin, a member of the disintegrin family of viper venom proteins, has been found to inhibit melanoma metastasis in vivo using immunodeficient mice. To date, the basis for eristostatin's anti-metastatic effect remains unknown. The long term objective of this research is to identify molecular mechanisms by which melanoma metastasis may be inhibited. The specific goal proposed here is to investigate how eristostatin inhibits experimental metastasis by pursuing two specific aims: (i) Characterize the interactions of eristostatin and its mutants with four melanoma cell lines possessing distinct combinations of well-defined surface receptors. (ii) Identify the structural sequence within eristostatin which is most critical for its anti-metastatic ability. Recombinant eristostatin mutations will be created by alanine scanning mutagenesis, and made as bacterial fusion proteins with glutathione-S-transferase. These purified mutants will be used in a series of functional assays with four human metastatic melanoma cells lines. We will identify the specific molecule with which eristostatin interacts on each cell through crosslinking and immunological techniques. To determine which residue(s) of eristostatin are responsible for its cellular interactions, each mutant will be compared with wildtype eristostatin's activity in cellular assays. Those mutants which show the greatest difference in cellular interaction will be used in experimental metastasis assays. After i.v. injection of immunodeficient mice with melanoma cells and mutated eristostatin, mice will be observed for four weeks, and then necropsied. Metastatic potential will be assessed by counting lung metastases. Cryosections of lungs will be evaluated using immunohistochemical stains. Taken together, these studies will provide insights into how one naturally occurring protein possesses the """"""""right fit"""""""" to bind melanoma cells and block their metastatic ability. This information will, in turn, lead to a rational design of therapeutic agents which would target these cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA098056-02
Application #
6730656
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Program Officer
Ault, Grace S
Project Start
2003-04-01
Project End
2006-03-31
Budget Start
2004-04-01
Budget End
2005-03-31
Support Year
2
Fiscal Year
2004
Total Cost
$251,038
Indirect Cost

  Institution

Name
University of Delaware
Department
Other Health Professions
Type
Schools of Allied Health Profes
DUNS #
059007500
City
Newark
State
DE
Country
United States
Zip Code
19716

  Publications

Galan, Jacob A; Sanchez, Elda E; Rodriguez-Acosta, Alexis et al. (2008) Inhibition of lung tumor colonization and cell migration with the disintegrin crotatroxin 2 isolated from the venom of Crotalus atrox. Toxicon 51:1186-96
McLane, Mary Ann; Joerger, Torsten; Mahmoud, Alaa (2008) Disintegrins in health and disease. Front Biosci 13:6617-37
McLane, Mary Ann (2008) A classification and nomenclature of disintegrins isolated from snake venoms. Toxicon 51:941
Tian, Jing; Paquette-Straub, Carrie; Sage, E Helene et al. (2007) Inhibition of melanoma cell motility by the snake venom disintegrin eristostatin. Toxicon 49:899-908
McLane, Mary Ann; Zhang, Xiaoming; Tian, Jing et al. (2005) Scratching below the surface: wound healing and alanine mutagenesis provide unique insights into interactions between eristostatin, platelets and melanoma cells. Pathophysiol Haemost Thromb 34:164-8
Butera, Diego; Piazza, Roxane Maria Fontes; McLane, Mary Ann et al. (2005) Molecular engineering of an EGFP/disintegrin-based integrin marker. Toxicon 46:178-84