Abstract

The CD94/NKG2 receptors expressed by subpopulations of NK cells and T cells have been implicated as receptors for a broad range of both classical and nonclassical HLA class I molecules. To examine the ligand specificity of CD94/NKG2 proteins, a soluble heterodimeric form of the receptor was produced and used in direct binding studies with cells expressing defined HLA class I/peptide complexes. We confirmed that CD94/NKG2A specifically interacts with HLA-E and demonstrated that this interaction is dependent on the association of HLA-E with peptide. Moreover, no interaction between CD94/NKG2A and classical HLA class I molecules were observed, as assayed by direct binding of the soluble receptor or by functionalassays using CD94/NKG2A+ NK cells. The role of the peptide associated with HLA-E in the interaction between HLA-E and CD94/NKG2A was also assessed. All class I leader sequence peptides tested bound to HLA-E and were recognized by CD94/NKG2A. However, amino acid variations in class I leader sequences affected the stability of HLA-E. Additionally, not all HLA-E/peptide complexes examined were recognized by CD94/NKG2A. Thus CD94/NKG2A recognition of HLA-E is controlled by peptide at two levels; first, peptide must stabilize HLA- E and promote cell surface expression and second, the HLA-E/peptide complex must form the ligand for CD94/NKG2A. The crystal structure of the intracellular domain of CD94 was determined revealing a unique C- type lectin fold. The crystal structure is likely a prototype for other NK cell receptors such as Ly-49, NKR-P1 and CD-69.In primary embryonal fibroblasts from transgenic mice expressing H-2(b) genes and a miniature swine class I transgene (PD1), transformation with adenovirus 12 results in suppression of assembly and cell surface expression of all class I complexes. Cell surface expression of PD1 can be recovered by transfecting the cells with peptide transporter genes. However, reconstitution of the H-2K(b) gene expression requires, in addition, a 2-fold increase in the steady state level of the H-2K(b) mRNA that can be attained by treatment of the cells with interferons or by transfecting them with the H-2K(b) gene. A detailed analyses of the biogenesis of class I molecules has revealed the steady state expression of free class I heavy chains that are not converted into conformed complexes even when peptide transporter genes are overexpressed. - Natural Killer (NK) cells, HLA class I receptors, HLA- E, CD94/NKG2, MHC class I complexes, peptide binding, cancer

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Intramural Research (Z01)
Project #
1Z01AI000543-12
Application #
6288873
Study Section
Special Emphasis Panel (LIG)
Project Start
Project End
Budget Start
Budget End
Support Year
12
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
National Institute of Allergy and Infectious Diseases
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Burgess, Steven J; Marusina, Alina I; Pathmanathan, Ishani et al. (2006) IL-21 down-regulates NKG2D/DAP10 expression on human NK and CD8+ T cells. J Immunol 176:1490-7
Lieto, L D; Maasho, K; West, D et al. (2006) The human CD94 gene encodes multiple, expressible transcripts including a new partner of NKG2A/B. Genes Immun 7:36-43
Marusina, Alina I; Kim, Dae-Ki; Lieto, Louis D et al. (2005) GATA-3 is an important transcription factor for regulating human NKG2A gene expression. J Immunol 174:2152-9
Borrego, Francisco; Masilamani, Madhan; Kabat, Juraj et al. (2005) The cell biology of the human natural killer cell CD94/NKG2A inhibitory receptor. Mol Immunol 42:485-8
Maasho, Kerima; Marusina, Alina; Reynolds, Nicole M et al. (2004) Efficient gene transfer into the human natural killer cell line, NKL, using the Amaxa nucleofection system. J Immunol Methods 284:133-40
Kim, Dae-Ki; Kabat, Juraj; Borrego, Francisco et al. (2004) Human NKG2F is expressed and can associate with DAP12. Mol Immunol 41:53-62
Sanni, Tolib B; Masilamani, Madhan; Kabat, Juraj et al. (2004) Exclusion of lipid rafts and decreased mobility of CD94/NKG2A receptors at the inhibitory NK cell synapse. Mol Biol Cell 15:3210-23
Lieto, Louis D; Borrego, Francisco; You, Chi-Hyun et al. (2003) Human CD94 gene expression: dual promoters differing in responsiveness to IL-2 or IL-15. J Immunol 171:5277-86
Borrego, Francisco; Kabat, Juraj; Sanni, Tolib B et al. (2002) NK cell CD94/NKG2A inhibitory receptors are internalized and recycle independently of inhibitory signaling processes. J Immunol 169:6102-11
Kabat, Juraj; Borrego, Francisco; Brooks, Andrew et al. (2002) Role that each NKG2A immunoreceptor tyrosine-based inhibitory motif plays in mediating the human CD94/NKG2A inhibitory signal. J Immunol 169:1948-58

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