Abstract

The present grant proposes to use lymphoblastoid cell line (LCL) variants that have lost expression of different portions of the HLA-D region (of one or both D haplotypes) to permit both genetic mapping of HLA-D encoded determinants and studies of genetic complementation. Preliminary investigations have demonstrated the feasibility of creating loss variants of varying lengths of the HLA-D region (including DNA loss variants) and mapping of determinants within this region, using cloned primed lymphocyte typing (PLT) reagents. Such reagents are of key import both because they offer a highly productive approach for the definition of multiple determinants associated with single D haplotypes, and because they can be readily prepared against normal cells (or LCLs) in any given combination. We shall focus first on DR2+ and DR4+ haplotypes, since these antigens are found in association with a large number of different """"""""Dw antigenic clusters"""""""", defined with homozygous typing cells and PLT reagents. DNA probes will be used to determine the nature of the mutation underlying loss of antigen expression and to aid in construction of a genetic map of the D region, as well as to further our understanding of the genetic basis for the relationship between serologically and cellularly detected determinants of D region encoded molecules. Attempts will be made to generate serological reagents, including monoclonal antibodies against D region products. Molecules expressing DR determinants (and later other D region encoded molecules expressing serologically detected determinants) will be isolated and studied by peptide mapping to investigate whether some peptides are associated with the serologically detectable determinant and others with the cellularly defined determinant(s) within a single molecular entity. Finally, we shall perform studies on a molecule, B7/21, which is encoded by genes linked to HLA-DR but which is different from the presently defined D region encoded molecules. We expect that these various approaches will contribute to the generation of a coherent picture of the genetic structure of, and molecules encoded in, the D region and thus enhance continued progress in matching for transplantation and understanding of disease associations.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI019007-03
Application #
3128421
Study Section
Experimental Immunology Study Section (EI)
Project Start
1983-05-01
Project End
1988-04-30
Budget Start
1985-05-01
Budget End
1986-04-30
Support Year
3
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
University of Minnesota Twin Cities
Department
Type
Schools of Medicine
DUNS #
168559177
City
Minneapolis
State
MN
Country
United States
Zip Code
55455

  Publications

von Albertini, M A; Goodman, D J; Bach, F H (1996) Direct cell contact is required to induce expression of E-selectin and IL-8 secretion in pig endothelial cells by human natural killer cells. Transplant Proc 28:608
Goodman, D J; Von Albertini, M; Willson, A et al. (1996) Direct activation of porcine endothelial cells by human natural killer cells. Transplantation 61:763-71
Goodman, D J; von Albertini, M; Bach, F H (1996) Human natural killer cells induce expression of E-selectin and interleukin-8 mRNA in porcine endothelial cells. Transplant Proc 28:609
Adamkiewicz, T V; McSherry, C; Bach, F H et al. (1994) Natural killer lectin-like receptors have divergent carboxy-termini, distinct from C-type lectins. Immunogenetics 39:218
Turman, M A; Yabe, T; McSherry, C et al. (1993) Characterization of a novel gene (NKG7) on human chromosome 19 that is expressed in natural killer cells and T cells. Hum Immunol 36:34-40
Yabe, T; McSherry, C; Bach, F H et al. (1993) A multigene family on human chromosome 12 encodes natural killer-cell lectins. Immunogenetics 37:455-60
Houchins, J P; Kricek, F; Chujor, C S et al. (1993) Genomic structure of NKG5, a human NK and T cell-specific activation gene. Immunogenetics 37:102-7
Nelson, P J; Geller, R L; Podack, E et al. (1992) Molecular events in late stages of T-cell functional maturation. Scand J Immunol 35:311-20
Nelson, P J; Geller, R L; Bach, F H (1992) Gene expression in CD8 and CD4 T-cell populations following activation with the calcium ionophore A23187. Scand J Immunol 35:611-9
Houchins, J P; Yabe, T; McSherry, C et al. (1991) DNA sequence analysis of NKG2, a family of related cDNA clones encoding type II integral membrane proteins on human natural killer cells. J Exp Med 173:1017-20

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