Abstract

The human inducible nitric oxide synthase (hiNOS) gene is expressed in nearly every organ during sepsis and other inflammatory conditions. While NO synthesis has beneficial effects during acute inflammation, excessive NO production is harmful. Chronic hiNOS expression has been implicated in NO-mediated tissue damage leading to diabetes, neurodegenerative disorders, and certain cancers. Our laboratory has cloned the human iNOS gene from eytokine-stimulated hepatoeytes, and we have shown that cytokine-responsive DNA elements are located approximately 5 kb upstream in the promoter region. We found that TNFalpha and IL-1beta signal through NF-kappaB, while IFNgamma signals through Stat-1 by binding to cis-acting elements at -5.2 and -5.8 kb in the promoter, thereby providing a molecular basis for cytokine synergy. Further functional roles have been demonstrated for AP-1, C/EBPbeta (LAP), and KLF6. Importantly, we have identified mechanisms for hiNOS repression that involve NF-kappaB repressing factor (NRF), LIP, and p53 proteins. A subsequent chromatin structure analysis using DNAse I mapping and in vivo footprinting revealed that regulation of hiNOS transcription was even more complex than originally anticipated and exhibited tissue-specific control by both basal and inducible transcription factors. Most recently, we have identified a novel role for the Wnt beta-catenin/Tcf-4 signaling pathway in regulating hiNOS expression. Therefore, our hypothesis is that the regulation of hiNOS gene expression requires an orchestrated flow of positive and negative transcription factors binding to a cis-acting upstream enhancer region located between -5.0 and -7.0 kb in the hiNOS promoter. In addition, a crucial downstream promoter region has been identified at -0.2 kb that is permissive for cytokine-induced transcription. In this proposal, we will pursue two specific aims to further elucidate the molecular mechanisms involved:
AIM I : TO DEFINE THE TRANSCRIPTION FACTORS AND FUNCTIONAL PROMOTER ELEMENTS RESPONSIBLE FOR CYTOKINE INDUCTION OF THE HUMAN iNOS GENE. ChIP assay will be used to confirm in vivo protein-DNA interactions for NF-kappaB, Stat-1, and AP-1 in the upstream enhancer region. New roles for Ets-1 and Oct-1 will be tested by gel shift and promoter transfection studies. Protein-protein interactions between NRF and NF-kB will be pursued, as well as mechanisms of downstream control elicited by LAP/LIP, KLF6, and p53.
AIM II : TO DETERMINE THE ROLE OF THE WNT Beta-CATENIN/TCF-4 SIGNALING PATHWAY IN REGULATING HUMAN iNOS EXPRESSION. A functional role for Beta-catenin/Tcf-4 binding to two TBE sites will be determined, as well as possible interactions with other transcription factors governing hiNOS expression. The information gained will increase our understanding of the control of hiNOS transcription, describe novel mechanisms of cytokine-synergy in signal transduetion, and help in designing therapeutic strategies for pathophysiologic disease states where hiNOS expression is relevant.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM052021-10
Application #
6821384
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Somers, Scott D
Project Start
1995-06-01
Project End
2008-06-30
Budget Start
2004-07-08
Budget End
2005-06-30
Support Year
10
Fiscal Year
2004
Total Cost
$290,895
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Surgery
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Cardinal, J S; Reddy, S K; Tsung, A et al. (2013) Laparoscopic major hepatectomy: pure laparoscopic approach versus hand-assisted technique. J Hepatobiliary Pancreat Sci 20:114-9
Du, Qiang; Zhang, Xinglu; Liu, Quan et al. (2013) Nitric oxide production upregulates Wnt/?-catenin signaling by inhibiting Dickkopf-1. Cancer Res 73:6526-37
Klune, John R; Dhupar, Rajeev; Kimura, Shoko et al. (2012) Interferon regulatory factor-2 is protective against hepatic ischemia-reperfusion injury. Am J Physiol Gastrointest Liver Physiol 303:G666-73
Li, Peiyuan; Du, Qiang; Cao, Zongxian et al. (2012) Interferon-ýý induces autophagy with growth inhibition and cell death in human hepatocellular carcinoma (HCC) cells through interferon-regulatory factor-1 (IRF-1). Cancer Lett 314:213-22
Du, Qiang; Geller, David A (2010) Cross-Regulation Between Wnt and NF-?B Signaling Pathways. For Immunopathol Dis Therap 1:155-181
Cao, Zongxian; Dhupar, Rajeev; Cai, Changchun et al. (2010) A critical role for IFN regulatory factor 1 in NKT cell-mediated liver injury induced by alpha-galactosylceramide. J Immunol 185:2536-43
Ueki, Shinya; Dhupar, Rajeev; Cardinal, Jon et al. (2010) Critical role of interferon regulatory factor-1 in murine liver transplant ischemia reperfusion injury. Hepatology 51:1692-701
Du, Qiang; Zhang, Xinglu; Cardinal, Jon et al. (2009) Wnt/beta-catenin signaling regulates cytokine-induced human inducible nitric oxide synthase expression by inhibiting nuclear factor-kappaB activation in cancer cells. Cancer Res 69:3764-71
Kim, Kee-Hwan; Dhupar, Rajeev; Ueki, Shinya et al. (2009) Donor graft interferon regulatory factor-1 gene transfer worsens liver transplant ischemia/reperfusion injury. Surgery 146:181-9
Park, Kyung Soo; Guo, Zhong; Shao, Lifang et al. (2009) A far-upstream Oct-1 motif regulates cytokine-induced transcription of the human inducible nitric oxide synthase gene. J Mol Biol 390:595-603

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