Abstract

The long-term goal of this project is to understand the basic molecular mechanisms and signalling pathways underlying immune tolerance. The specific objectives are to determine whether the transcription factor NFAT plays a role in tolerance induction. The underlying hypothesis to be tested is that tolerance induction involves unbalanced activation of NFAT in the absence of its cooperating transcription factor AP-1 (Fos/Jun).
In Aim 1, the requirements for tolerance induction by NFAT will be defined. NFAT1-/- T cells, which we have shown are much less susceptible to the induction of anergy in a cell culture model than are T cells from normal mice, will be reconstituted with wildtype NFAT, an NFAT mutant incapable of interacting with AP-1, and a version of NFAT that is hypersensitive to calcineurin, and the ability of the reconstituted cells to be anergised in a cell culture model will be compared. A selective peptide inhibitor of NFAT (VIVIT) will be tested for whether it interferes with tolerance induction.
In Aim 2, the role of NFAT will be tested in physiological systems of tolerance induction, including the high dose antigen model of T cell tolerance and the HL model of B cell tolerance. The selective NFAT inhibitor VIVIT will be transiently expressed in T cells during the first stage of tolerance induction and tested for whether it abrogates tolerance induction in vivo.
In Aim 3, NFAT-dependent target genes that are induced in tolerant T cells will be identified using multiple approaches (DNA arrays, subtractive strategies, and genome-wide retroviral insertion). Selected genes will be tested for whether they fit criteria expected for genes involved in tolerance induction.
In Aim 4, the role of NFAT in anergy induced by altered peptide ligands will be tested using the approaches and reagents already used in Aim 1. The experiments will determine whether tolerance has a transcriptional basis and whether inhibitors of the NFAT-Fos-Jun interaction can be used in cell culture and in vivo to induce a tolerant state.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI048213-04
Application #
6632445
Study Section
Immunological Sciences Study Section (IMS)
Program Officer
Nabavi, Nasrin N
Project Start
2000-06-15
Project End
2005-05-31
Budget Start
2003-06-01
Budget End
2004-05-31
Support Year
4
Fiscal Year
2003
Total Cost
$468,540
Indirect Cost

  Institution

Name
Immune Disease Institute, Inc.
Department
Type
DUNS #
059709394
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Keller, Tracy L; Zocco, Davide; Sundrud, Mark S et al. (2012) Halofuginone and other febrifugine derivatives inhibit prolyl-tRNA synthetase. Nat Chem Biol 8:311-7
Bandukwala, Hozefa S; Wu, Yongqing; Feuerer, Markus et al. (2011) Structure of a domain-swapped FOXP3 dimer on DNA and its function in regulatory T cells. Immunity 34:479-91
Sundrud, Mark S; Koralov, Sergei B; Feuerer, Markus et al. (2009) Halofuginone inhibits TH17 cell differentiation by activating the amino acid starvation response. Science 324:1334-8
Oh-hora, Masatsugu; Rao, Anjana (2009) The calcium/NFAT pathway: role in development and function of regulatory T cells. Microbes Infect 11:612-9
Picard, Capucine; McCarl, Christie-Ann; Papolos, Alexander et al. (2009) STIM1 mutation associated with a syndrome of immunodeficiency and autoimmunity. N Engl J Med 360:1971-80
Koh, Kian Peng; Sundrud, Mark S; Rao, Anjana (2009) Domain requirements and sequence specificity of DNA binding for the forkhead transcription factor FOXP3. PLoS One 4:e8109
Soto-Nieves, Noemi; Puga, Irene; Abe, Brian T et al. (2009) Transcriptional complexes formed by NFAT dimers regulate the induction of T cell tolerance. J Exp Med 206:867-76
Oh-Hora, Masatsugu; Yamashita, Megumi; Hogan, Patrick G et al. (2008) Dual functions for the endoplasmic reticulum calcium sensors STIM1 and STIM2 in T cell activation and tolerance. Nat Immunol 9:432-43
Puga, Irene; Rao, Anjana; Macian, Fernando (2008) Targeted cleavage of signaling proteins by caspase 3 inhibits T cell receptor signaling in anergic T cells. Immunity 29:193-204
Sundrud, Mark S; Rao, Anjana (2007) New twists of T cell fate: control of T cell activation and tolerance by TGF-beta and NFAT. Curr Opin Immunol 19:287-93

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