Abstract

Glucocorticoids (GCs) are potent immunosuppressive and anti-inflammatory agents that are widely used in the treatment of autoimmune and inflammatory diseases, including rheumatoid arthritis (RA) and systemic lupus erythematosus (SLE). A well established mechanism of GC action is inhibition of AP-1 and NF-KappaB transcription factors that are activated by pathogenic cytokines such as IL-1 and TNF. We have explored the effects of GCs on the Jak-STAT pathway, the major signal transduction pathway utilized by a large number of cytokines important in rheumatic disease pathogenesis, including interferons (IFNs), interleukin-2 (IL-2), IL-6, IL-15, and GM-CSF. We found that GCs had minimal effects on basal Jak-STAT signaling. Instead, GCs strongly suppressed the sensitization and enhancement of Jak-STAT signaling that occurs during cell activation. Sensitization and enhancement of macrophage responses to cytokines and microbial products after previous exposure to IFNs was described in the 1970s and termed priming. More recently there has been increasing interest in a role for enhanced cellular responses to cytokines, microbial products, and environmental antigens in the pathogenesis of rheumatic diseases. Since priming is suppressed by GCs and relevant for rheumatic disease pathogenesis, we studied the molecular mechanisms of priming. Our long term goals are to increase our understanding of the molecular basis of priming, and subsequently to study how priming mechanisms are regulated by GCs. We have found that priming enhanced cytokine activation of Stat1, a pro-inflammatory transcription factor, by increasing Stat1 expression and coupling the Syk tyrosine kinase to the Jak-STAT signal transduction pathway. Priming also enhanced macrophage cytokine production by abrogating a feedback inhibition loop mediated by IL-10 and Stat3, an anti-inflammatory transcription factor in myeloid cells that mediates the suppressive effects of IL-10. Stat1 and StatS typically oppose each others' activity, and GCs suppressed Stat1 activation and promoted Stat3 activity. We hypothesize that altered Stat1 and Stat3 activation in primed relative to unprimed macrophages underlies the enhanced responses of primed macrophages to inflammatory factors and cytokines. In this application, we will delineate molecular mechanisms that regulate Stat1 and StatS activation and function in primed macrophages, and investigate the functional consequences of altered STAT activation in the context of rheumatic disease pathogenesis. We anticipate that these studies will provide insight into mechanisms that regulate cellular responsiveness to activating factors that are important in the pathogenesis of rheumatic diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI046712-06
Application #
6929597
Study Section
Special Emphasis Panel (ZRG1-ACTS (01))
Program Officer
Esch, Thomas R
Project Start
2000-03-01
Project End
2010-02-28
Budget Start
2005-03-01
Budget End
2006-02-28
Support Year
6
Fiscal Year
2005
Total Cost
$382,500
Indirect Cost

  Institution

Name
Hospital for Special Surgery
Department
Type
DUNS #
622146454
City
New York
State
NY
Country
United States
Zip Code
10021

  Publications

Sokhi, Upneet K; Liber, Mark P; Frye, Laura et al. (2018) Dissection and function of autoimmunity-associated TNFAIP3 (A20) gene enhancers in humanized mouse models. Nat Commun 9:658
Binder, Nikolaus; Miller, Christine; Yoshida, Masaki et al. (2017) Def6 Restrains Osteoclastogenesis and Inflammatory Bone Resorption. J Immunol 198:3436-3447
Park, Sung Ho; Kang, Kyuho; Giannopoulou, Eugenia et al. (2017) Type I interferons and the cytokine TNF cooperatively reprogram the macrophage epigenome to promote inflammatory activation. Nat Immunol 18:1104-1116
Kang, Kyuho; Park, Sung Ho; Chen, Janice et al. (2017) Interferon-? Represses M2 Gene Expression in Human Macrophages by Disassembling Enhancers Bound by the Transcription Factor MAF. Immunity 47:235-250.e4
Ivashkiv, Lionel B; Park, Sung Ho (2016) Epigenetic Regulation of Myeloid Cells. Microbiol Spectr 4:
Qiao, Yu; Kang, Kyuho; Giannopoulou, Eugenia et al. (2016) IFN-? Induces Histone 3 Lysine 27 Trimethylation in a Small Subset of Promoters to Stably Silence Gene Expression in Human Macrophages. Cell Rep 16:3121-3129
Lee, Min Joon; Lim, Elisha; Mun, Sehwan et al. (2016) Intravenous Immunoglobulin (IVIG) Attenuates TNF-Induced Pathologic Bone Resorption and Suppresses Osteoclastogenesis by Inducing A20 Expression. J Cell Physiol 231:449-458
Miller, Christine H; Smith, Sinead M; Elguindy, Mahmoud et al. (2016) RBP-J-Regulated miR-182 Promotes TNF-?-Induced Osteoclastogenesis. J Immunol 196:4977-86
Huynh, Linda; Kusnadi, Anthony; Park, Sung Ho et al. (2016) Opposing regulation of the late phase TNF response by mTORC1-IL-10 signaling and hypoxia in human macrophages. Sci Rep 6:31959
Kalliolias, George D; Ivashkiv, Lionel B (2016) TNF biology, pathogenic mechanisms and emerging therapeutic strategies. Nat Rev Rheumatol 12:49-62

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