Abstract

The long term goal is to identify molecular targets that can be used for prognosis and therapy of HNSCC. Head &neck squamous cell carcinomas (HNSCC) represent the 6th most common cancer type in western countries. The major HNSCC etiological factors are environmental carcinogens, e.g., tobacco and alcohol, which cause genetic alterations and chronic inflammation in head &neck (H&N) tissues. In this application, we will use an inducible H&N-specific gene targeting system to introduce several genetic alterations in the TGF? signaling pathway, which are common in human HNSCC, into mouse H&N tissues, and assess the mechanisms by which these alterations promote HNSCC development.
Aim 1 will examine molecular mechanisms of Smad4 loss-mediated HNSCC development. We will assess if any Fanc/Brca members are direct Smad4 transcriptional targets, and if VEGF overexpression in Smad4-/- HNSCCs is the result of Smad3 activation and contributes to Smad4 loss-mediated HNSCC carcinogenesis. Genome-wide analyses will be performed to identify additional alterations caused by Smad4 loss, which contribute to oncogenic effects on H&N epithelia and stroma.
Aim 2 will assess the role of Smad2 loss in HNSCC promotion. We will determine if Smad2 loss promotes HNSCC formation and progression in the presence of a Kras mutation. We will analyze if increased HGF signaling found in Smad2-/- tissues contributes to Smad2 loss-associated oncogenic effects and study the mechanisms of HGF upregulation in Smad2-/- cells. Genome-wide screens will also be performed to identify molecular alterations caused by Smad2 loss in H&N tissues.
Aim 3 will assess the role of stromal TGF?RII loss in HNSCC development. We will induce TGF?RII deletion in oral fibroblasts to ascertain if this will induce or promote HNSCC formation in the presence of either a chemical carcinogen-induced H-ras mutation or TGF?RII deletion in H&N epithelia. Pathological and molecular alterations caused by oral fibroblast TGF?RII deletion will be analyzed. These studies will not only improve our understanding of HNSCC biology, but will also directly test therapeutic approaches in HSNCC with specific TGF? signaling defects.

Public Health Relevance

The application will use state-of-the-art experimental models and approaches to identify molecular mechanisms that cause head &neck cancer formation and progression. The proposed studies will lead to the identification of biomarkers that can be used to improve cancer prognosis and therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
5R01DE015953-10
Application #
8403387
Study Section
Tumor Microenvironment Study Section (TME)
Program Officer
Venkatachalam, Sundaresan
Project Start
2004-03-01
Project End
2015-01-31
Budget Start
2013-02-01
Budget End
2014-01-31
Support Year
10
Fiscal Year
2013
Total Cost
$381,161
Indirect Cost
$119,007

  Institution

Name
University of Colorado Denver
Department
Pathology
Type
Schools of Medicine
DUNS #
041096314
City
Aurora
State
CO
Country
United States
Zip Code
80045

  Publications

Luo, Jingjing; Bian, Li; Blevins, Melanie A et al. (2018) Smad7 Promotes Healing of Radiotherapy-Induced Oral Mucositis without Compromising Oral Cancer Therapy in a Xenograft Mouse Model. Clin Cancer Res :
Dionne, Lai Kuan; Peterman, Eric; Schiel, John et al. (2017) FYCO1 regulates accumulation of post-mitotic midbodies by mediating LC3-dependent midbody degradation. J Cell Sci 130:4051-4062
Jian, Zhe; Strait, Alexander; Jimeno, Antonio et al. (2017) Cancer Stem Cells in Squamous Cell Carcinoma. J Invest Dermatol 137:31-37
Haeger, Sarah M; Thompson, Joshua J; Kalra, Sean et al. (2016) Smad4 loss promotes lung cancer formation but increases sensitivity to DNA topoisomerase inhibitors. Oncogene 35:577-586
Morton, J J; Bird, G; Keysar, S B et al. (2016) XactMice: humanizing mouse bone marrow enables microenvironment reconstitution in a patient-derived xenograft model of head and neck cancer. Oncogene 35:290-300
Mishra, Ameet K; Kadoishi, Tanya; Wang, Xiaoguang et al. (2016) Squamous cell carcinomas escape immune surveillance via inducing chronic activation and exhaustion of CD8+ T Cells co-expressing PD-1 and LAG-3 inhibitory receptors. Oncotarget 7:81341-81356
Dionne, Lai Kuan; Wang, Xiao-Jing; Prekeris, Rytis (2015) Midbody: from cellular junk to regulator of cell polarity and cell fate. Curr Opin Cell Biol 35:51-8
Dionne, L K; Driver, E R; Wang, X J (2015) Head and Neck Cancer Stem Cells: From Identification to Tumor Immune Network. J Dent Res 94:1524-31
Malkoski, Stephen P; Cleaver, Timothy G; Thompson, Joshua J et al. (2014) Role of PTEN in basal cell derived lung carcinogenesis. Mol Carcinog 53:841-6
Han, Gangwen; Bian, Li; Li, Fulun et al. (2013) Preventive and therapeutic effects of Smad7 on radiation-induced oral mucositis. Nat Med 19:421-8

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