Abstract

We have recently demonstrated the expression of a gene, the ubiquitin E3 ligase, GRAIL, in CD4+ T cells during the induction and maintenance phases of anergy in vivo, following our original description of the ability of over expression of GRAIL in vitro to block activation induced IL-2 transcription in T cell hybridomas. Additionally, however, expression of GRAIL in naive CD4+ TCR transgenic T cells in vivo, following retroviral transduction of bone marrow cells and adoptive transfer into immuno-incompetent recipients, rendered resultant peripheral CD4+ T cells refractory to antigen stimulation, both for proliferation and IL-2 production, resembling the typical phenotype of anergic CD4+ T cells. The striking finding that expression of an enzymatically inactive version of the E3 ligase, H2N2 GRAIL, effectively prevented the establishment of the anergy phenotype in similar bone marrow transduced adoptively transferred peripheral CD4+ T cells, clearly establishes the importance of this new E3 ligase as a central player in the anergy phenotype. Studies in this competing renewal proposal will take advantage of these data to further explore the function and regulation of GRAIL in anergy, not only in models in vitro, but will also look into the potential role of GRAIL and its binding partners, DOG and SOG, in animal models of cancer and autoimmunity as well as an attempt to establish a role for these proteins (or their dysregulation) in human disease. These studies will be accomplished under two specific aims: (1) Molecular and biochemical characterization of the GRAIL pathway in anergic T cells; and (2) Analysis of GRAIL and GRAIL associated protein expression in animal models of cancer and autoimmunity and in human disease counterparts. Although many of the techniques that will be used in these studies are commonly practiced, innovative methods of screening for E3 ligase substrates, techniques to follow GRAIL expressing cells in vivo using knock-in technology, and the development of a novel lentiviral vector for bone marrow hematopoietic stem cell transduction and reconstitution of immuno-incompetent mice are novel techniques that have recently been or are being developed in the lab. Dysregulation of GRAIL and/or its binding partners, DOG or SOG, in human diseases of immune or cellular dysfunction, is suggested by preliminary data. If this proves correct, it will open studies of an exciting pathway of cellular signaling whose dysregulation has important implications in cancer and autoimmunity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA065237-16
Application #
6780200
Study Section
Allergy and Immunology Study Section (ALY)
Program Officer
Mccarthy, Susan A
Project Start
1989-04-01
Project End
2009-04-30
Budget Start
2004-05-01
Budget End
2005-04-30
Support Year
16
Fiscal Year
2004
Total Cost
$290,295
Indirect Cost

  Institution

Name
Stanford University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Levin, Aron M; Bates, Darren L; Ring, Aaron M et al. (2012) Exploiting a natural conformational switch to engineer an interleukin-2 'superkine'. Nature 484:529-33
Junttila, Ilkka S; Creusot, Remi J; Moraga, Ignacio et al. (2012) Redirecting cell-type specific cytokine responses with engineered interleukin-4 superkines. Nat Chem Biol 8:990-8
Lin, Jack T; Stein, Emily A; Wong, Michael T et al. (2012) Differential mTOR and ERK pathway utilization by effector CD4 T cells suggests combinatorial drug therapy of arthritis. Clin Immunol 142:127-38
Whiting, Chan C; Su, Leon L; Lin, Jack T et al. (2011) GRAIL: a unique mediator of CD4 T-lymphocyte unresponsiveness. FEBS J 278:47-58
Lin, Jack T; Lineberry, Neil B; Kattah, Michael G et al. (2009) Naive CD4 t cell proliferation is controlled by mammalian target of rapamycin regulation of GRAIL expression. J Immunol 182:5919-28
Lineberry, Neil B; Su, Leon L; Lin, Jack T et al. (2008) Cutting edge: The transmembrane E3 ligase GRAIL ubiquitinates the costimulatory molecule CD40 ligand during the induction of T cell anergy. J Immunol 181:1622-6
Lineberry, Neil; Su, Leon; Soares, Luis et al. (2008) The single subunit transmembrane E3 ligase gene related to anergy in lymphocytes (GRAIL) captures and then ubiquitinates transmembrane proteins across the cell membrane. J Biol Chem 283:28497-505
Fathman, C Garrison; Lineberry, Neil B (2007) Molecular mechanisms of CD4+ T-cell anergy. Nat Rev Immunol 7:599-609
Su, Leon; Lineberry, Neil; Huh, Yul et al. (2006) A novel E3 ubiquitin ligase substrate screen identifies Rho guanine dissociation inhibitor as a substrate of gene related to anergy in lymphocytes. J Immunol 177:7559-66
Ermann, Joerg; Hoffmann, Petra; Edinger, Matthias et al. (2005) Only the CD62L+ subpopulation of CD4+CD25+ regulatory T cells protects from lethal acute GVHD. Blood 105:2220-6

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