Abstract

Cancer appears to be, in many ways, a disease of the cell cycle. The molecular components of the cellular machinery that drives the cell cycle are being uncovered in rapid succession. Whether a cell enters the cycle and proceeds to cell division depends largely on the input it receives from growth factors and growth inhibitors in the extracellular milieu. The secreted polypeptide, Transforming Growth Factor-beta (TGF-beta), is the most potent known inhibitor of cell division of normal epithelial cell and induces the accumulation of extracellular matrix. These dual biological effects of TGFbeta1 are mediated by a complex of two interacting and interdependent receptor serin/threonine kinases, type I (TbetaR-I) and type II (TbetaR-II). In spite of the voluminous literature that supports the notion that escape from TGFbeta-mediated growth control plays and important part in malignant transformation, there is virtually no information on the molecular status of TGFbeta receptors in cancer in general and of squamous cell carcinomas of the upper aero-digestive tract (i.e. head-&- neck, esophagus and lung) in particular. The central hypothesis is that genetic alterations in this TGFbeta receptor system play an important role in squamous epithelial cell transformation by fundamentally altering the ways cells respond to TGFbeta1's signals. Dr. Reiss has identified several different SqCC cell lines in which the TbetaR-II gene carries point mutations, which result in amino acid substitution at highly conserved sites within the cytoplasmic domain of the protein. These mutations appear to alter the secondary structure, kinase activity and interactions of the type II receptor with TbetaR-I. This the first clear evidence that TbetaR mutants occur naturally in human cancer cells and provides strong support for my hypothesis. These observations raise the questions (1) how these mutation affect the biochemical, functional and biological properties of the TGFbeta receptor system; (2) what role they play in tumor development; (3) at which stage of tumor development these mutations are acquired in vivo and whether or not they carry any prognostic significance. These are the questions we plan to address during the next five years. In the longer term, these studies should lead to the development of molecular and/or pharmacological tools to correct the dysfunction of the TGFbeta receptor system in human cancers. As the TGFbeta system appears to play an important role in many different types of cancer, the significance of our findings is likely to extend far beyond that of aero-digestive tract cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
3R01CA041556-11S1
Application #
6012884
Study Section
Pathology B Study Section (PTHB)
Program Officer
Freeman, Colette S
Project Start
1986-07-01
Project End
1999-08-31
Budget Start
1999-01-11
Budget End
1999-08-31
Support Year
11
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Yale University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
082359691
City
New Haven
State
CT
Country
United States
Zip Code
06520

  Publications

Xie, Wen; Aisner, Seena; Baredes, Soly et al. (2013) Alterations of Smad expression and activation in defining 2 subtypes of human head and neck squamous cell carcinoma. Head Neck 35:76-85
Cohen-Solal, Karine A; Merrigan, Kim T; Chan, Joseph L-K et al. (2011) Constitutive Smad linker phosphorylation in melanoma: a mechanism of resistance to transforming growth factor-?-mediated growth inhibition. Pigment Cell Melanoma Res 24:512-24
Tan, Antoinette R; Alexe, Gabriela; Reiss, Michael (2009) Transforming growth factor-beta signaling: emerging stem cell target in metastatic breast cancer? Breast Cancer Res Treat 115:453-95
Bharathy, Savita; Xie, Wen; Yingling, Jonathan M et al. (2008) Cancer-associated transforming growth factor beta type II receptor gene mutant causes activation of bone morphogenic protein-Smads and invasive phenotype. Cancer Res 68:1656-66
Padgett, Richard W; Reiss, Michael (2007) TGFbeta superfamily signaling: notes from the desert. Development 134:3565-9
Ge, Rongrong; Rajeev, Vaishali; Ray, Partha et al. (2006) Inhibition of growth and metastasis of mouse mammary carcinoma by selective inhibitor of transforming growth factor-beta type I receptor kinase in vivo. Clin Cancer Res 12:4315-30
Subramanian, Gayathri; Schwarz, Roderich E; Higgins, Linda et al. (2004) Targeting endogenous transforming growth factor beta receptor signaling in SMAD4-deficient human pancreatic carcinoma cells inhibits their invasive phenotype1. Cancer Res 64:5200-11
Xie, Wen; Bharathy, Savita; Kim, David et al. (2003) Frequent alterations of Smad signaling in human head and neck squamous cell carcinomas: a tissue microarray analysis. Oncol Res 14:61-73
Liu, Chenghai; Gaca, Marianna D A; Swenson, E Scott et al. (2003) Smads 2 and 3 are differentially activated by transforming growth factor-beta (TGF-beta ) in quiescent and activated hepatic stellate cells. Constitutive nuclear localization of Smads in activated cells is TGF-beta-independent. J Biol Chem 278:11721-8
Xie, Wen; Mertens, Joachim C; Reiss, Daniel J et al. (2002) Alterations of Smad signaling in human breast carcinoma are associated with poor outcome: a tissue microarray study. Cancer Res 62:497-505

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