Abstract

The primary purpose of this proposal is to examine the role of class II MHC antigen and its associated molecules (H-2M and Ii) in allogeneic and/or xenogeneic transplantation involving keratinocytes and islet cells. These studies stem from the applicants' observation that keratinocytes isolated from class II MHC defective mice failed to prime for an allogeneic response from the host. These studies have motivated an examination of the role of other proteins in allogeneic transplant rejection or acceptance. Specifically, the investigators wish to test three mice strains: mice defective in the IA(b)[beta]gene, the H-2M molecule (which is necessary for peptide loading onto class II MHC proteins) and CIITA, a master transcriptional regulator essential for trans-activation of class II MHC genes, Ii chain, and the H-2M genes. Using keratinocytes and islet cells derived from these three mice, the applicants wish to test their acceptance as allografts. In addition, they wish to test if pre- transplantation with keratinocytes that are defective in class II MHC antigens can result in tolerance induction which can enhance the successful implant of allogeneic islet cells. Accordingly, the following aims will be pursued. First, immunologic priming by IA(b)[beta](-/-), H-2M(-/-), and CIITA(-/-) keratinocytes will be compared. The capacity of cells isolated from these animals to prime an allo- and xenoresponse will be assessed. Secondly, the acceptance of islet allografts from IA(b)[beta](-/-), H-2M(-/-), and CIITA(-/-) animals will be compared to grafts from wild type controls. The capacity to restore normal glycemia will be examined. Finally, the failure of keratinocytes from IA(b)[beta](-/-) allografts suggests that these cells may have caused immunologic tolerance. Direct studies to examine if this is the case are planned. An extension of these experiments will be to determine if mice transplanted with IA(b)[beta](-/-) keratinocytes are more tolerant of I(A(b)[beta](-/-) allogeneic islet cells. Similarly, if the experiments with H-2M(-/-) or CIITA(-/-) are encouraging, they also will be tested to determine if they can induce prolonged acceptance of islet cells. Together these experiments should shed light on the biological function of class II antigens as well as molecules involved in class II presentation in transplants that are relevant to a large proportion of patients with severe unhealed wounds, burns, or diabetes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI041580-04
Application #
6338617
Study Section
Project Start
2000-08-01
Project End
2002-07-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
4
Fiscal Year
2000
Total Cost
$189,927
Indirect Cost

  Institution

Name
University of North Carolina Chapel Hill
Department
Type
DUNS #
078861598
City
Chapel Hill
State
NC
Country
United States
Zip Code
27599

  Publications

Felix, Nathan J; de Serres, Suzan; Meyer, Anthony A et al. (2002) Comparison of Abeta(b-/-), H2-DM(-), and CIITA(-/-) in second-set skin allograft rejection. J Surg Res 102:185-92
van Deventer, Hendrik W; Serody, Jonathon S; McKinnon, Karen P et al. (2002) Transfection of macrophage inflammatory protein 1 alpha into B16 F10 melanoma cells inhibits growth of pulmonary metastases but not subcutaneous tumors. J Immunol 169:1634-9
June Brickey, W; Felix, Nathan J; Griffiths, Robert et al. (2002) Prolonged survival of class II transactivator-deficient cardiac allografts. Transplantation 74:1341-8
Tisch, R; Wang, B; Weaver, D J et al. (2001) Antigen-specific mediated suppression of beta cell autoimmunity by plasmid DNA vaccination. J Immunol 166:2122-32
Taxman, D J; Ting, J P (2001) Identification of novel Mycoplasma hyorhinis gene fragments by differential display analysis of co-cultures. J Microbiol Methods 44:217-23
Weaver Jr, D J; Liu, B; Tisch, R (2001) Plasmid DNAs encoding insulin and glutamic acid decarboxylase 65 have distinct effects on the progression of autoimmune diabetes in nonobese diabetic mice. J Immunol 167:586-92
Maile, R; Wang, B; Schooler, W et al. (2001) Antigen-specific modulation of an immune response by in vivo administration of soluble MHC class I tetramers. J Immunol 167:3708-14
Taxman, D J; Cressman, D E; Ting, J P (2000) Identification of class II transcriptional activator-induced genes by representational difference analysis: discoordinate regulation of the DN alpha/DO beta heterodimer. J Immunol 165:1410-6
Wang, B; Maile, R; Greenwood, R et al. (2000) Naive CD8+ T cells do not require costimulation for proliferation and differentiation into cytotoxic effector cells. J Immunol 164:1216-22
White 2nd, G C; Greenwood, R; Escobar, M et al. (2000) Hemophilia factor VIII therapy. Immunological tolerance. A clinical perspective. Haematologica 85:113-6

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