Abstract

Early studies examining the pathways of class I and class II restricted antigen presentation suggested a clear demarcation between these two pathways in terms of their antigenic sources. Class II-restricted antigens were derived from exogenous proteins processed in the cytoplasm. The exclusion of exogenous antigens from the class I pathway made sense in that this pathway was considered to be for the sensitizing of viral-infected cells for lysis by CD8 cytotoxic T lymphocytes (CTL). Thus, only cells containing the viral proteins (and therefore the virus) could become targets for CTL destruction. Evidence for this model of class I-restricted presentation was obtained by examining the requirements for sensitizing target cells for killing by effector CTL. When the priming of naive CD8 T-cells was examined, quite a different conclusion emerged. Exogenous proteins were reported to prime various CD8 T-cell responses, including those to minor HAs, viral and tumor antigens - this was referred to as cross-priming, and the pathway as the cross-presentation pathway. These studies implied that under certain conditions exogenous antigens could enter the class I pathway of antigen presenting cells (APC), be processed into the class I pathway, and prime CD8 T-cells. Recently, using transgenic mice expressing neo-self antigens in tissues such as the pancreas, the investigators have begun to characterize this pathway. Self antigens were shown to be constitutively presented in a class I-restricted manner by a bone marrow-derived APC that resides in the lymph nodes. These data suggest that antigens expressed in tissues are captured by APC, transported to the draining lymph nodes, and presented to CD8 T-cells. They have shown that this provides a pathway for induction of peripheral tolerance, as well as immunity, and that several factors affect which of these outcomes emerges, including the availability of cognate CD4 T-cell """"""""help"""""""". The hypothesis is that the cross-presentation pathway plays an important role in the surveillance of tissues for viral and tumor antigens, and in the maintenance of self tolerance to peripheral antigens. This application plans to utilize the transgenic models to characterize both peripheral tolerance and immunity induced by the cross-presentation pathway. Specifically, the application will examine: (i) the nature of antigens that can be presented by this pathway; (ii) the mechanism by which this pathway induces tolerance to self antigens; and (iii) how CD4 T-cells provide help for generation of CTL immunity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI043347-03
Application #
6170522
Study Section
Immunobiology Study Section (IMB)
Program Officer
Wiesch, Denise
Project Start
1998-09-30
Project End
2001-08-31
Budget Start
2000-09-01
Budget End
2001-08-31
Support Year
3
Fiscal Year
2000
Total Cost
$108,203
Indirect Cost

  Institution

Name
Walter and Eliza Hall Institute Medical Research
Department
Type
DUNS #
753236256
City
Parkville
State
Country
Australia
Zip Code
VIC, -3052

  Publications

Johnson, Susan; Zhan, Yifan; Sutherland, Robyn M et al. (2009) Selected Toll-like receptor ligands and viruses promote helper-independent cytotoxic T cell priming by upregulating CD40L on dendritic cells. Immunity 30:218-27
Behrens, Georg M N; Li, Ming; Davey, Gayle M et al. (2004) Helper requirements for generation of effector CTL to islet beta cell antigens. J Immunol 172:5420-6
Mueller, Scott N; Jones, Claerwen M; Chen, Weisan et al. (2003) The early expression of glycoprotein B from herpes simplex virus can be detected by antigen-specific CD8+ T cells. J Virol 77:2445-51
Coles, Richard M; Mueller, Scott N; Heath, William R et al. (2002) Progression of armed CTL from draining lymph node to spleen shortly after localized infection with herpes simplex virus 1. J Immunol 168:834-8
Davey, Gayle M; Kurts, Christian; Miller, Jacques F A P et al. (2002) Peripheral deletion of autoreactive CD8 T cells by cross presentation of self-antigen occurs by a Bcl-2-inhibitable pathway mediated by Bim. J Exp Med 196:947-55
Mintern, Justine D; Sutherland, Robyn M; Lew, Andrew M et al. (2002) Constitutive, but not inflammatory, cross-presentation is disabled in the pancreas of young mice. Eur J Immunol 32:1044-51
Mintern, Justine D; Davey, Gayle M; Belz, Gabrielle T et al. (2002) Cutting edge: precursor frequency affects the helper dependence of cytotoxic T cells. J Immunol 168:977-80
Mueller, Scott N; Jones, Claerwen M; Smith, Chris M et al. (2002) Rapid cytotoxic T lymphocyte activation occurs in the draining lymph nodes after cutaneous herpes simplex virus infection as a result of early antigen presentation and not the presence of virus. J Exp Med 195:651-6
Mintern, Justine D; Belz, Gabrielle; Gerondakis, Steve et al. (2002) The cross-priming APC requires a Rel-dependent signal to induce CTL. J Immunol 168:3283-7
Li, M; Davey, G M; Sutherland, R M et al. (2001) Cell-associated ovalbumin is cross-presented much more efficiently than soluble ovalbumin in vivo. J Immunol 166:6099-103

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