Abstract

How is tolerance induced to self-antigens that arise late in development or are inaccessible to the thymus and environmental antigens in the flora of the gut and airways? How are autoreactive T cells that escape negative selection, deleted or anergized in the periphery? This Program Project will address the central hypothesis that the immature DC functions to maintain peripheral tolerance, while the mature DC induces immunity. Four Projects will explore the mechanisms that underlie this ability of DCs to discriminate among infectious and self-antigens, potential defects in autoimmune states, and ways to manipulate these mechanisms to induce tolerance. In Project 1, Dr. Ralph Steinman will focus on the mechanisms by which DCs can induce tolerance to pancreatic islets. He will investigate maturation stimuli to selectively activate DCs in vivo and utilize this knowledge to induce peripheral tolerance to a surrogate beta cell antigen. Insulinoma cells will be studied to establish conditions for tolerizing the immune system to beta cell autoantigens, using the ability of DCs to cross-present islet cell autoantigens. In Project 2, Dr. Jeffrey Ravetch will focus on the specific role of immunoreceptors ITAM (an activation immunoreceptor) and ITIM (an inhibitory immunoreceptor) and signaling in DCs to induce maturation or maintain tolerance. The Fcgamma receptor (FcgammaR) system and its ligand, the immune complex, will be exploited to investigate how the balance between activation and inhibitory signaling can determine the in vivo outcome of antigens targeted to DCs. Through the use of novel genetically targeted animals, the role of the FcgammaR system in susceptibility to autoimmunity will be determined and manipulated to re-establish tolerance. In Project 3, Dr. Alexander Tarakhovsky will study the oncogene Src-family kinases in DC maturation and antigen presentation. Through the use of conditional disruptions in the negative regulators Csk and Cbp, he will determine the role of these pathways in DC function. To further define the signals involved in DC maturation, he proposes to study a novel toll-like receptor protein, RP105, expressed on DCs. In Project 4, Dr. Michel Nussenzweig will specifically target antigens to DCs in vivo to define their role in maintaining tolerance. Inducing DC maturation after targeting will be investigated as a way to convert a tolerogenic signal to an immunogenic signal. These approaches will be used in the experimental autoimmune encephalomyelitis (EAE) model to determine if targeting myelin oligodendrocyte glycoprotein (MOG) to DCs in various states of maturation can either induce tolerance or disease. Mice will be genetically engineered to express DCs arrested at the immature or mature state to test the hypothesis that the state of DC activation will determine if an antigenic stimulus is tolerogenic or immunogenic.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
1P01AI051573-01
Application #
6466183
Study Section
Special Emphasis Panel (ZAI1-NN-I (J1))
Program Officer
Rothermel, Annette L
Project Start
2002-09-10
Project End
2007-06-30
Budget Start
2002-09-10
Budget End
2003-06-30
Support Year
1
Fiscal Year
2002
Total Cost
$1,550,959
Indirect Cost

  Institution

Name
Rockefeller University
Department
Genetics
Type
Other Domestic Higher Education
DUNS #
071037113
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Sela, Uri; Park, Chae Gyu; Park, Andrew et al. (2016) Dendritic Cells Induce a Subpopulation of IL-12R?2-Expressing Treg that Specifically Consumes IL-12 to Control Th1 Responses. PLoS One 11:e0146412
Guermonprez, Pierre; Helft, Julie; Claser, Carla et al. (2013) Inflammatory Flt3l is essential to mobilize dendritic cells and for T cell responses during Plasmodium infection. Nat Med 19:730-8
Schreiber, Heidi A; Loschko, Jakob; Karssemeijer, Roos A et al. (2013) Intestinal monocytes and macrophages are required for T cell polarization in response to Citrobacter rodentium. J Exp Med 210:2025-39
Bozzacco, Leonia; Yu, Haiqiang (2013) Identification and quantitation of MHC class II-bound peptides from mouse spleen dendritic cells by immunoprecipitation and mass spectrometry analysis. Methods Mol Biol 1061:231-43
Bozzacco, Leonia; Yu, Haiqiang; Dengjel, Jorn et al. (2012) Strategy for identifying dendritic cell-processed CD4+ T cell epitopes from the HIV gag p24 protein. PLoS One 7:e41897
Meredith, Matthew M; Liu, Kang; Kamphorst, Alice O et al. (2012) Zinc finger transcription factor zDC is a negative regulator required to prevent activation of classical dendritic cells in the steady state. J Exp Med 209:1583-93
Meredith, Matthew M; Liu, Kang; Darrasse-Jeze, Guillaume et al. (2012) Expression of the zinc finger transcription factor zDC (Zbtb46, Btbd4) defines the classical dendritic cell lineage. J Exp Med 209:1153-65
Wang, Bei; Zaidi, Neeha; He, Li-Zhen et al. (2012) Targeting of the non-mutated tumor antigen HER2/neu to mature dendritic cells induces an integrated immune response that protects against breast cancer in mice. Breast Cancer Res 14:R39
Bozzacco, Leonia; Yu, Haiqiang; Zebroski, Henry A et al. (2011) Mass spectrometry analysis and quantitation of peptides presented on the MHC II molecules of mouse spleen dendritic cells. J Proteome Res 10:5016-30
Li, Fubin; Ravetch, Jeffrey V (2011) Inhibitory Fc? receptor engagement drives adjuvant and anti-tumor activities of agonistic CD40 antibodies. Science 333:1030-4

Showing the most recent 10 out of 40 publications