Abstract

Hyaluronic acid (HA), the predominant glycosaminoglycan on malignant tumor cells, is bound to the cell surface by its receptor CD44. Levels of HA correlate with enhanced metastatic behavior, as do certain of the isoforms of CD44. Human breast cancer cell tumors grown in SCID mice decrease in size following i.v. hyaluronidase treatment, a 50% decrease occurring in four days. Brief exposure of cultured breast cancer cells in vitro to hyaluronidase eliminates not only the cell-associated HA, but also all of the malignant variants of CD44, leaving only two """"""""benign"""""""" forms, CD44S and CD44E. It is now proposed to develop an animal model of oral squamous cell carcinoma (OSCC) using human cell lines grown orthotopically in nude mice, and to determine whether hyaluronidase can also cause tumor regression in this model. Simultaneously, coordinated studies using immunohistochemistry, FACS analyses, and RT-PCR will be performed to document modulation of HA and CD44 isoforms with hyaluronidase. It is postulated that the enzyme is a previously unrecognized anticancer therapeutic, that HA stabilizes its own receptor, and that eradication of HA by hyaluronidase causes down regulation of CD44 metastatic variant isoforms, thereby causing tumor regression, and prevention of further cancer spread. Furthermore, it is suspect that saliva creates an HA-rich environment in the oral cavity, and underlies the particularly aggressive course of OSCC's. In conjunction with these studies, levels and localization of HA, hyaluronidase, CD44, and its isoforms will be documented in an array of cultured OSCC cells of increasing aggressiveness, as well as in human biopsy specimens obtained from the oral cancer tissue and histopathology core. OSCC, comprising the vast majority of oral cancers, metastasizes widely. The degree of aggressiveness, unlike other human cancers, does not correlate with the histological appearance. Nor can it be predicted which patients with dysplasia or leukoplakia will go on to develop OSCC. The contention of this proposal is that the metabolism of HA is fundamental to the process of malignant progression, and that among the parameters measured in this proposal will be those that can function as predictive and prognostic indicators. Such potential markers will be of enormous clinical value in identifying not only patients at increased risk for developing malignancy, but also those with existing lesions that have particularly aggressive potential.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Specialized Center (P50)
Project #
3P50DE011912-05S2
Application #
6500415
Study Section
Project Start
2001-08-01
Project End
2003-01-31
Budget Start
Budget End
Support Year
5
Fiscal Year
2001
Total Cost
$103,677
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Type
DUNS #
073133571
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Bortoluzzi, Marcelo C; Yurgel, Liliane S; Dekker, Nusi P et al. (2004) Assessment of p63 expression in oral squamous cell carcinomas and dysplasias. Oral Surg Oral Med Oral Pathol Oral Radiol Endod 98:698-704
Sethi, Neerja; Palefsky, Joel (2003) Treatment of human papillomavirus (HPV) type 16-infected cells using herpes simplex virus type 1 thymidine kinase-mediated gene therapy transcriptionally regulated by the HPV E2 protein. Hum Gene Ther 14:45-57
Stern, Robert; Shuster, Svetlana; Neudecker, Birgit A et al. (2002) Lactate stimulates fibroblast expression of hyaluronan and CD44: the Warburg effect revisited. Exp Cell Res 276:24-31
Mio, Kazuhiro; Stern, Robert (2002) Inhibitors of the hyaluronidases. Matrix Biol 21:31-7
Regezi, Joseph A; Ramos, Daniel M; Pytela, Robert et al. (2002) Tenascin and beta 6 integrin are overexpressed in floor of mouth in situ carcinomas and invasive squamous cell carcinomas. Oral Oncol 38:332-6
Nicoll, Steven B; Barak, Ory; Csoka, Antonei B et al. (2002) Hyaluronidases and CD44 undergo differential modulation during chondrogenesis. Biochem Biophys Res Commun 292:819-25
Shuster, Svetlana; Frost, Gregory I; Csoka, Antonei B et al. (2002) Hyaluronidase reduces human breast cancer xenografts in SCID mice. Int J Cancer 102:192-7
Csoka, A B; Frost, G I; Stern, R (2001) The six hyaluronidase-like genes in the human and mouse genomes. Matrix Biol 20:499-508
Mio, K; Csoka, A B; Nawy, S S et al. (2001) Detecting hyaluronidase and hyaluronidase inhibitors. Hyaluronan-substrate gel and -inverse substrate gel techniques. Methods Mol Biol 171:391-7
Lin, G; Stern, R (2001) Plasma hyaluronidase (Hyal-1) promotes tumor cell cycling. Cancer Lett 163:95-101

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