Abstract

The goals of this proposal are to test the hypothesis that (i) lack of recognition of squamous cell carcinoma of the head and neck (SCCHN) cells by HLA class I antigen restricted, tumor antigen (TA)-specific cytotoxic T lymphocytes (CTL), in spite of restricting HLA class I allele and TA expression, reflects defects in HLA class I antigen-TA peptide complex expression, (ii) these defects are caused by decreased expression and/or function of antigen processing machinery (ARM) components, which we are considering to include the ctglucosidases l/ll (Gl/ll) and (Hi) HLA class I -TA peptide complex expression and SCCHN cell recognition by HLA class I antigen restricted, TA peptide-specific CTL can be restored by correcting ARM component defects and (iv) these defects have clinical significance. These hypotheses stem from observations that ARM component downregulation (i) has been observed in SCCHN cells and is associated with lack of their recognition by HLA class I antigen restricted, TA-specific CTL, (ii) can be corrected in vitro by IFN-y resulting in recognition of SCCHN cells by can restore HLA class I-TA peptide complex expression as well as SCCHN cell recognition by HLA class I antigen restricted, TA-specific CTL and (iii) plays a role in the clinical course of the disease. To test our hypotheses, we will correlate levels of ARM components in SCCHN cells with those of HLA class I antigens and HLA class I-TA peptide complexes and recognition by HLA class I antigen restricted, TA peptide-specific CTL, as well as investigate the effect of ARM component modulation on HLA class I antigen-TA peptide complex expression by SCCHN cells and their recognition by CTL. To assess the clinical significance of our studies we will (i) correlate ARM component defects in SCCHN lesions with their histopathology and/or clinical course, and (ii) determine if intralesional administration of INF-y enhances ARM component and HLA class I-TA peptide complex expression SCCHN lesions. The proposed studies will utilize a unique panel of monoclonal antibody (mAb) which recognize all ARM components and methodology we have recently developed to quantitate the level of ARM component expression in cells and HLA-AHER2369- 377 and HLA-A2-MAGE-3/6271-279 peptide complexes. The results derived form the outlined studies will contribute to our understanding of the molecular mechanism(s) underlying the lack of recognition of SCCHN cells by HLA class I antigen restricted, TA peptide-specific CTL, assess the clinical relevance of ARM component and HLA class I-TA peptide complex defects, and may identify strategies to correct these abnormalities and impact on the clinical course of SCCHN.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA109688-04
Application #
7903456
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2009-08-01
Budget End
2010-07-31
Support Year
4
Fiscal Year
2009
Total Cost
$119,887
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Type
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Spitler, Lynn E; Cao, Huynh; Piironen, Timo et al. (2017) Biological Effects of Anti-Granulocyte-Macrophage Colony-Stimulating Factor (GM-CSF) Antibody Formation in Patients Treated With GM-CSF (Sargramostim) as Adjuvant Therapy of Melanoma. Am J Clin Oncol 40:207-213
Macatangay, Bernard J C; Riddler, Sharon A; Wheeler, Nicole D et al. (2016) Therapeutic Vaccination With Dendritic Cells Loaded With Autologous HIV Type 1-Infected Apoptotic Cells. J Infect Dis 213:1400-9
Szczepanski, Miroslaw J; Luczak, Michal; Olszewska, Ewa et al. (2015) Molecular signaling of the HMGB1/RAGE axis contributes to cholesteatoma pathogenesis. J Mol Med (Berl) 93:305-14
Whiteside, Theresa L (2015) Clinical Impact of Regulatory T cells (Treg) in Cancer and HIV. Cancer Microenviron 8:201-7
Schuler, P J; Saze, Z; Hong, C-S et al. (2014) Human CD4+ CD39+ regulatory T cells produce adenosine upon co-expression of surface CD73 or contact with CD73+ exosomes or CD73+ cells. Clin Exp Immunol 177:531-43
Schuler, Patrick J; Harasymczuk, Malgorzata; Visus, Carmen et al. (2014) Phase I dendritic cell p53 peptide vaccine for head and neck cancer. Clin Cancer Res 20:2433-44
Whiteside, Theresa L (2014) Regulatory T cell subsets in human cancer: are they regulating for or against tumor progression? Cancer Immunol Immunother 63:67-72
Whiteside, Theresa L (2013) Immune modulation of T-cell and NK (natural killer) cell activities by TEXs (tumour-derived exosomes). Biochem Soc Trans 41:245-51
Chi Sabins, Nina; Taylor, Jennifer L; Fabian, Kellsye P L et al. (2013) DLK1: a novel target for immunotherapeutic remodeling of the tumor blood vasculature. Mol Ther 21:1958-68
Jie, H-B; Gildener-Leapman, N; Li, J et al. (2013) Intratumoral regulatory T cells upregulate immunosuppressive molecules in head and neck cancer patients. Br J Cancer 109:2629-35

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