Abstract

The IFN consensus sequence binding protein (ICSBP/IRF-8), which belongs to the interferon? regulatory factor family of transcription factors, is essential for a Thl immune response.? ICSBP plays an important role in the host defense against microbial pathogens, but the exact? roles of ICSBP in inflammation and chronic inflammatory diseases are still not clear. IL-10-/-? mice, which develop colitis characterized by increased Thl cytokines, mimic many aspects of? human Crohn's disease (CD). The importance of ICSBP in the development of colitis is shown? by the lack of disease in ICSBP and IL-10 double knockout mice. In addition, ICSBP mRNA? and protein are highly expressed in the colons of IL-10-/- mice with colitis, while expression? of IL-12 and iNOS is significantly compromised in ICSBP/IL-10 double KO mice. In agreement? with these results, patients with CD have significantly higher ICSBP expression than normal? individuals. ICSBP is active in several loci. ICSBP interacts with TRAF6 in the TLR4 pathway,? and binds to ISRE sites in the iNOS and IL-12 p40 promoters, activating the expression of? these genes. In addition, we find that ICSBP is ubiquitinated by the E3 ligase Cbl, resulting in? its degradation by the proteasome. To expore ICSBP as a suitable target for therapy in CD,? this proposal is structured around three aims: 1) We will analyze the regulation of ICSBP? expression in macrophages and dendritic cells activated with various TLR and NOD2 ligands.? In addition, we will define the role of ICSBP in the generation of regulatory T cells. 2) We will? define the function of Cbl in the control of Thl immune immune response and analyze the? role of Cbl in the development of colitis. 3) We will define the therapeutic effects of TLR4 and? ICSBP inhibition by cell-permeable peptide reagent in vivo in murine colitis models. These? studies will advance our understanding the role of ICSBP in the mucosal immune response,? and may identify ICSBP as a new target for therapy in CD.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK072201-03
Application #
7683157
Study Section
Special Emphasis Panel (ZDK1)
Project Start
Project End
Budget Start
2008-09-01
Budget End
2009-08-31
Support Year
3
Fiscal Year
2008
Total Cost
$202,134
Indirect Cost

  Institution

Name
Icahn School of Medicine at Mount Sinai
Department
Type
DUNS #
078861598
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Meisel, Marlies; Hinterleitner, Reinhard; Pacis, Alain et al. (2018) Microbial signals drive pre-leukaemic myeloproliferation in a Tet2-deficient host. Nature 557:580-584
Blander, J Magarian (2018) Regulation of the Cell Biology of Antigen Cross-Presentation. Annu Rev Immunol 36:717-753
Blander, J Magarian; Barbet, Gaetan (2018) Exploiting vita-PAMPs in vaccines. Curr Opin Pharmacol 41:128-136
Barbet, Gaetan; Sander, Leif E; Geswell, Matthew et al. (2018) Sensing Microbial Viability through Bacterial RNA Augments T Follicular Helper Cell and Antibody Responses. Immunity 48:584-598.e5
Moretti, Julien; Roy, Soumit; Bozec, Dominique et al. (2017) STING Senses Microbial Viability to Orchestrate Stress-Mediated Autophagy of the Endoplasmic Reticulum. Cell 171:809-823.e13
Moretti, Julien; Blander, J Magarian (2017) Cell-autonomous stress responses in innate immunity. J Leukoc Biol 101:77-86
Blander, J Magarian; Longman, Randy S; Iliev, Iliyan D et al. (2017) Regulation of inflammation by microbiota interactions with the host. Nat Immunol 18:851-860
Blander, J Magarian (2017) The many ways tissue phagocytes respond to dying cells. Immunol Rev 277:158-173
Tang, Mei San; Bowcutt, Rowann; Leung, Jacqueline M et al. (2017) Integrated Analysis of Biopsies from Inflammatory Bowel Disease Patients Identifies SAA1 as a Link Between Mucosal Microbes with TH17 and TH22 Cells. Inflamm Bowel Dis 23:1544-1554
Roulis, M; Bongers, G; Armaka, M et al. (2016) Host and microbiota interactions are critical for development of murine Crohn's-like ileitis. Mucosal Immunol 9:787-97

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