This proposal is to continue the examination of the processing and presentation of protein antigens. The main goal is to obtain information on the biochemistry and cellular basis of protein processing by antigen presenting cells (APC) that results in the surface expression of a peptide associated with class II-MHC molecules (Ia). We focus here on the identification of subcellular pathways of antigen transport and on the biochemical analysis of protein antigens; in the identification of organelles where proteins are fragmented and where the fragments associated with Ia; and in the analysis of conditions that may modulate the primary interaction of Ia with peptides. We combine herewith techniques, many already developed, of cellular fractionation, peptide and protein biochemistry and cellular immunology. The goal of Project 1 is to identify, isolate and characterize intracellular organelles that bear Ia molecules. It includes ultrastructural analysis and biochemical attempts to isolate Ia-bearing vesicles. It also contains biochemical attempts to reproduce Ia-peptide interactions in cell-free systems using the contents of, or the conditions found in, endosomes. It has a section evaluating the role of Invariant chain. The goal of Project 2 is to identify biochemically the products of catabolism of the protein hen-egg white lysozyme relevant in antigen presentation. Included are several projects examining the intracellular site of catabolism of antigen and of coupling of peptide to Ia. A key goal is to identify the chemistry of natural peptides of lysozyme that associate with Ia molecules. The goal of Project 3 is to examine whether there are differences in antigen processing among APC that depend on cell types and/or their state of activation. It also includes studies examining how polysaccharides affect antigen processing. The information on the biochemical and cellular basis of antigen processing and presentation will allow us to understand many of the events, and regulation, of immune induction and some of the basis for self/non-self identification of proteins.

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI022033-08
Application #
3132638
Study Section
Allergy and Immunology Study Section (ALY)
Project Start
1985-04-01
Project End
1995-03-31
Budget Start
1992-04-01
Budget End
1993-03-31
Support Year
8
Fiscal Year
1992
Total Cost
Indirect Cost
Name
Washington University
Department
Type
Schools of Medicine
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130
Ireland, Jamie M; Unanue, Emil R (2012) Processing of proteins in autophagy vesicles of antigen-presenting cells generates citrullinated peptides recognized by the immune system. Autophagy 8:429-30
Strong, Beverly S I; Unanue, Emil R (2011) Presentation of type B peptide-MHC complexes from hen egg white lysozyme by TLR ligands and type I IFNs independent of H2-DM regulation. J Immunol 187:2193-201
Ireland, Jamie M; Unanue, Emil R (2011) Autophagy in antigen-presenting cells results in presentation of citrullinated peptides to CD4 T cells. J Exp Med 208:2625-32
Atibalentja, Danielle F; Murphy, Kenneth M; Unanue, Emil R (2011) Functional redundancy between thymic CD8?+ and Sirp?+ conventional dendritic cells in presentation of blood-derived lysozyme by MHC class II proteins. J Immunol 186:1421-31
Yang, Chiao-Wen; Strong, Beverly S I; Miller, Mark J et al. (2010) Neutrophils influence the level of antigen presentation during the immune response to protein antigens in adjuvants. J Immunol 185:2927-34
Belizaire, Roger; Unanue, Emil R (2009) Targeting proteins to distinct subcellular compartments reveals unique requirements for MHC class I and II presentation. Proc Natl Acad Sci U S A 106:17463-8
Atibalentja, Danielle F; Byersdorfer, Craig A; Unanue, Emil R (2009) Thymus-blood protein interactions are highly effective in negative selection and regulatory T cell induction. J Immunol 183:7909-18
Lovitch, Scott B; Petzold, Shirley J; Unanue, Emil R (2003) Cutting edge: H-2DM is responsible for the large differences in presentation among peptides selected by I-Ak during antigen processing. J Immunol 171:2183-6
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Williams, I R; Unanue, E R (1990) Costimulatory requirements of murine Th1 clones. The role of accessory cell-derived signals in responses to anti-CD3 antibody. J Immunol 145:85-93

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