Abstract

Hyaluronate has been found to influence various aspects of cell behavior, including adhesion, phagocytosis and migration. These effects are probably mediated by a cellsurface receptor for hyaluronate which has been identified as an 85,000 Mr glycoprotein. Recent experiments have shown that the hyaluronate receptor is associated with actin filaments. Thus, the receptor may be responsible for a transmembrane interaction between extracellular hyaluronate and the intracellular actin filaments, which may in turn be important in regulating cell behavior. The goals of the present application are to further examine the hyaluronate receptor with respect to 1) its association with other proteins, 2) its distribution on the cell surface under different conditions, and 3) its role in regulating cell adhesion and migration. The first series of studies will examine the interaction of the receptor with other proteins. Preliminary experiments have shown that when cells are extracted with detergents under mild conditions, the receptor is present in a large complex. This complex will be isolated by molecularsieve chromatography and ratezonal centrifugation and the proteins which are present will be analyzed by SDSPAGE. In addition, proteins which interact with the receptor will be identified by binding experiments using an istopically labeled preparation of the receptor. The results of this study should reveal how the receptor interacts with Factin and other proteins. The next series of studies will examine the distribution of receptors on the surfaces of cells subjected to different conditions. First, to determine if Factin and/or hyaluronate controls the distribution of receptors, cells will be treated with drugs which alter these macromolecules, and the effect on the receptor distribution will be investigated. Secondly, the effects of viraltransformation on the distribution of receptors will be examined. And thirdly, migrating cells will be tested to determine if the receptors are distributed in a characteristic pattern. In each case, the receptors, will be visualized by immunofluorescent staining with a monoclonal antibody (K-3), specific for the receptor. The final series of experiments will examine the role of the receptor in mediating cell behavior. For this we will investigate the effects of the K3 monoclonal antibody and other substances which specifically interact with the receptor on 1) the heterotypic adhesion between tumor cells and endothelial cells, and 2) the rate of cell migration. The results of this study should answer a number of questions concerning the mechanism by which hyaluronate regulates cell behavior. This in turn may be of importance to several aspects of oncogensis, including tumor cell invasiveness, metastasis and angiogensis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA035592-06
Application #
3173188
Study Section
Cellular Biology and Physiology Subcommittee 1 (CBY)
Project Start
1984-07-01
Project End
1991-06-30
Budget Start
1989-07-01
Budget End
1991-06-30
Support Year
6
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Georgetown University
Department
Type
Schools of Medicine
DUNS #
049515844
City
Washington
State
DC
Country
United States
Zip Code
20057

  Publications

Zhang, L; Underhill, C B; Chen, L (1995) Hyaluronan on the surface of tumor cells is correlated with metastatic behavior. Cancer Res 55:428-33
Culty, M; Shizari, M; Thompson, E W et al. (1994) Binding and degradation of hyaluronan by human breast cancer cell lines expressing different forms of CD44: correlation with invasive potential. J Cell Physiol 160:275-86
Culty, M; Miyake, K; Kincade, P W et al. (1990) The hyaluronate receptor is a member of the CD44 (H-CAM) family of cell surface glycoproteins. J Cell Biol 111:2765-74
Aruffo, A; Stamenkovic, I; Melnick, M et al. (1990) CD44 is the principal cell surface receptor for hyaluronate. Cell 61:1303-13
Alho, A M; Underhill, C B (1989) The hyaluronate receptor is preferentially expressed on proliferating epithelial cells. J Cell Biol 108:1557-65
Underhill, C B (1989) The interaction of hyaluronate with the cell surface: the hyaluronate receptor and the core protein. Ciba Found Symp 143:87-99;discussion 100-6, 281-5
Green, S J; Tarone, G; Underhill, C B (1988) Distribution of hyaluronate and hyaluronate receptors in the adult lung. J Cell Sci 90 ( Pt 1):145-56
Green, S J; Underhill, C B (1988) Hyaluronate appears to be covalently linked to the cell surface. J Cell Physiol 134:376-86
Green, S J; Tarone, G; Underhill, C B (1988) Aggregation of macrophages and fibroblasts is inhibited by a monoclonal antibody to the hyaluronate receptor. Exp Cell Res 178:224-32
Underhill, C B; Green, S J; Comoglio, P M et al. (1987) The hyaluronate receptor is identical to a glycoprotein of Mr 85,000 (gp85) as shown by a monoclonal antibody that interferes with binding activity. J Biol Chem 262:13142-6

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