Abstract

The objective of this proposal is to understand what role inactivation of the TGF-beta receptor complex plays in the multi-stage development of oral cancers. As the functional unit which transduces the inhibitory signal directed by TGF-beta, this heteromeric receptor complex is composed to two serine/threonine kinases (TbetaR-II and TbetaR-I). Working in obligatory cooperation, TbetaR-II and TbetaR-I indirectly regulate the phosphorylation of the retinoblastoma tumor suppressor gene product (pRB) and subsequent progression of the cell cycle. Inactivation of either TbetaR-II or TbetaR-I gene may lead to the deregulation of cell cycle and ultimately uncontrolled proliferation. The studies described herein address the hypothesis that a subset of the genetic changes commonly present in end-stage oral squamous cell carcinomas (SCC) will have already occurred in premalignant (leukoplakia, erythroplakia and proliferative verrucous leukoplakia) lesions. We have previously shown the TbetaR-II gene to be mutated (21%) and down-regulated (87%) in end-stage SCC of the head and neck. However, other potential mechanisms of this down- regulation, as well as a detailed evaluation of the TbetaR-I gene component in premalignant and malignant oral lesions have yet to be explored. Our experimental approach involves a combination of genetic and biochemical methodologies. Studies in Specific Aim 1 are designed to determine the incidence and mechanism of TbetaR-II and TbetaR-I gene inactivation (including deletions, insertions, single nucleotide substitutions, and hypermethylation events) in premalignant and malignant oral lesions. Once identified, oral lesions exhibiting TbetaR-II or TbetaR-I mutations will be assessed at the level transcription and/or translation for altered expression compared to patient-matched normal tissues (Specific Aim 2). These expression studies will be performed as a means of determining a precise level of TGF-beta receptor complex deregulation. In addition, specific TbetaR-II and TbetaR-I mutant proteins will be evaluated in Specific Aim 3 for their degree of biologic activity compared to the wild-type proteins. Mutant proteins will be constructed by site-directed mutagenesis and evaluated for their ligand binding, phosphorylation and trans-binding abilities in vitro. Overall, it is anticipated that the results from these studies will not only broaden our understand of the molecular mechanisms of oral cancer development, but may also aid in the identification of specific causative agents, intermediate endpoint biomarkers, and the development of successful intervention strategies which target premalignant disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Program Projects (P01)
Project #
1P01DE012704-01
Application #
6104961
Study Section
Project Start
1998-09-15
Project End
1999-06-30
Budget Start
Budget End
Support Year
1
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Ohio State University
Department
Type
DUNS #
098987217
City
Columbus
State
OH
Country
United States
Zip Code
43210

  Publications

Giannini, Peter J; Morse, Mark A; Weghorst, Christopher M et al. (2008) Functional Activities and Immunohistochemical Cellular Distribution of Glutathione S-Transferases in Normal, Dysplastic, and Squamous Cell Carcinoma Human Oral Tissues. Clin Med Oncol 2:159-168
Wang, Dian; Grecula, John C; Gahbauer, Reinhard A et al. (2006) p16 gene alterations in locally advanced squamous cell carcinoma of the head and neck. Oncol Rep 15:661-5
Sedghizadeh, Parish P; Mallery, Susan R; Thompson, Sarah J et al. (2006) Expression of the serine protease DESC1 correlates directly with normal keratinocyte differentiation and inversely with head and neck squamous cell carcinoma progression. Head Neck 28:432-40
Han, ChunHua; Ding, Haiming; Casto, Bruce et al. (2005) Inhibition of the growth of premalignant and malignant human oral cell lines by extracts and components of black raspberries. Nutr Cancer 51:207-17
Pasche, Boris; Knobloch, Thomas J; Bian, Yansong et al. (2005) Somatic acquisition and signaling of TGFBR1*6A in cancer. JAMA 294:1634-46
Ding, Haiming; Han, Chunhua; Zhu, Jiuxiang et al. (2005) Celecoxib derivatives induce apoptosis via the disruption of mitochondrial membrane potential and activation of caspase 9. Int J Cancer 113:803-10
Ding, Haiming; Han, Chunhua; Gibson-D'Ambrosio, Ruth et al. (2003) Piroxicam selectively inhibits the growth of premalignant and malignant human oral cell lines by limiting their progression through the S phase and reducing the levels of cyclins and AP-1. Int J Cancer 107:830-6
Smiraglia, D J; Smith, L T; Lang, J C et al. (2003) Differential targets of CpG island hypermethylation in primary and metastatic head and neck squamous cell carcinoma (HNSCC). J Med Genet 40:25-33
Mallery, Susan R; Morse, Mark A; Wilson, Ralph F et al. (2003) AIDS-related Kaposi's sarcoma cells rapidly internalize endostatin, which co-localizes to tropomysin microfilaments and inhibits cytokine-mediated migration and invasion. J Cell Biochem 89:133-43
Wilson, Ralph F; Morse, Mark A; Pei, Ping et al. (2003) Endostatin inhibits migration and invasion of head and neck squamous cell carcinoma cells. Anticancer Res 23:1289-95

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