Abstract

Background. Natural killer (NK) cells eliminate incipient cancers and hematogenous metastases. NK mediated killing is inhibited y target cell HLA class i molecules, possibly through diverse HLA receptors recognize related HLA class I alleles, probably by contracting relatively conserved alpha-helical sites. Each NK cell expresses several crossreactive HLA receptors and recognizes multiple host HLA molecules. Recognition of target cell HLA inhibits NK mediated killing, proliferations, and cytokine production. Preliminary Studies. HLA-B*0702 protects transfected target cells from peripheral blood mononuclear cell )PBMC) NK mediated killing. Significantly increased killing is allowed by mutations in the B*0702 peptide binding groove, including the B pocket, and in the solvent- accessible T cell receptor contact site. The same mutations affect killing mediated by cytolytic T lymphocytes. HPLC separated peptides eluted from B*0702+ cells inhibit NK mediated killing of B*0702+ peptide transport deficient T2 cells. Our preliminary studies suggest that NK cells contact HLA-bound peptides and nearby HLA alpha-helical residues. Experimental Plan. We will test additions B*0702 mutants with PBMC NK cells nd NK clones to further refine the NK MHC contact site. We will examine how PBMC NK cells bearing the NKB1 putative HLA-B receptor and NK clones distinguish HLA alleles in three model systems; B*5101-B*0702, B*2705-B*0702, and Cw*0301-Cw*0601. If different HLA molecules inhibit NK cells in a quantitatively similar fashion, then expression of one, two, or three HLA genes will have an additive effect on NK mediated killing. We have devised several experimental approaches to identify HLA-binding peptides that inhibit NK cells. Peptide deficient T2 or acid stripped target cells will be incubated with HLA-binding synthetic or cellular peptides and tested in NK mediated killing assays. Alternatively, T2 cells will be transfected with individual minigenes or minigene libraries encoding HLA-binding peptides. Once protective peptides are identified, alanine substituted synthetic peptides will be tested for HLA binding and inhibition of K cells, allowing us to deduce NK receptor contact sites. Furthermore, we will t est if NK mediated killing, proliferations, and interferon gamma production are coordinately regulated by HLA and peptide variants. Whenever feasible, we will use both lymphoid and transformed oral keratinocyte target cells. Significance to Oral Cancer. Due to """"""""field cancerization"""""""", oral cancer patients frequently suffer second malignancies and would benefit from enhanced NK surveillance. Identification of HLA structures that control NK mediated killing will help characterize newly described NK receptors. Identification of HLA or peptide variants that produce a 'split response"""""""" separating NK mediated killing, proliferation, and cytokine production, may suggest better ways to manipulate Nk attack on oral cancers. Protective HLA-binding peptides could inhibit NK attack of normal cells but not cancer cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Dental & Craniofacial Research (NIDCR)
Type
Research Project (R01)
Project #
5R01DE011139-03
Application #
2443683
Study Section
Oral Biology and Medicine Subcommittee 1 (OBM)
Project Start
1995-07-01
Project End
1999-06-30
Budget Start
1997-07-01
Budget End
1998-06-30
Support Year
3
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
University of Iowa
Department
Pathology
Type
Schools of Medicine
DUNS #
041294109
City
Iowa City
State
IA
Country
United States
Zip Code
52242

  Publications

Lam-ubol, Aroonwan; Hopkin, Dustin; Letuchy, Elena M et al. (2010) Squamous carcinoma cells influence monocyte phenotype and suppress lipopolysaccharide-induced TNF-alpha in monocytes. Inflammation 33:207-23
Butler, James E; Moore, Mikel B; Presnell, Steven R et al. (2009) Proteasome regulation of ULBP1 transcription. J Immunol 182:6600-9
Kurago, Zoya B; Lam-Ubol, Aroonwan; Stetsenko, Anton et al. (2008) Lipopolysaccharide-Squamous Cell Carcinoma-Monocyte Interactions Induce Cancer-Supporting Factors Leading to Rapid STAT3 Activation. Head Neck Pathol 2:1-12
Lutz, Charles T; Moore, Mikel B; Bradley, Sarah et al. (2005) Reciprocal age related change in natural killer cell receptors for MHC class I. Mech Ageing Dev 126:722-31
Rayhill, Stephen C; Kirby, Patricia A; Voigt, Michael D et al. (2005) Positive serum cryoglobulin is associated with worse outcome after liver transplantation for chronic hepatitis C. Transplantation 80:448-56
Lutgendorf, Susan K; Moore, Mikel B; Bradley, Sarah et al. (2005) Distress and expression of natural killer receptors on lymphocytes. Brain Behav Immun 19:185-94
Moore, Mikel B; Kurago, Zoya B; Fullenkamp, Colleen A et al. (2003) Squamous cell carcinoma cells differentially stimulate NK cell effector functions: the role of IL-18. Cancer Immunol Immunother 52:107-15
Reber, Adrian J; Turnquist, Heth R; Thomas, Heather J et al. (2002) Expression of invariant chain can cause an allele-dependent increase in the surface expression of MHC class I molecules. Immunogenetics 54:74-81
Shi, Yan; Lutz, Charles T (2002) Interferon--gamma control of EBV-transformed B cells: a role for CD8+ T cells that poorly kill EBV-infected cells. Viral Immunol 15:213-25
Turnquist, H R; Thomas, H J; Prilliman, K R et al. (2000) HLA-B polymorphism affects interactions with multiple endoplasmic reticulum proteins. Eur J Immunol 30:3021-8

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