Abstract

The acute phase response, the systemic response to inflammatory stimuli, consists of a large number of early defensive and adaptive mechanisms which represent a phenomenon of great biologic importance. Our long term goals have been to delineate the mechanisms which mediate the acute phase response, with particular emphasis on C-reactive protein (CRP) induction in hepatocytes. Optimal induction of CRP in the human hepatoma cell line Hep 3B can be accomplished by the combination of IL-6 and IL-1. IL-6 induces transcription of CRP, while IL-1beta, which alone has no effect, significantly enhances the transcriptional effect of IL-6. Our recent studies indicate that a) the transcription factor STAT3 plays an important role in CRP induction by IL-6, an observation which led us to identify a STAT response element in the CRP promoter, b) expression of chimeric constructs of the CRP promoter and a reporter gene (CRP-CAT) are influenced by NFkappaB family members: p50 enhances expression, while p65 blocks this effect, and c) the effect of p50 requires a region in the promoter which contains both STAT and C/EBP response elements but contains no apparent kappaB binding site. These observations give rise to our working hypothesis, that synergistic effects of [IL-6 + IL-1beta] on CRP transcription are mediated by functional interactions between transcription factors activated by IL-1 (most likely NFkappaB family members) and IL-6- responsive STAT or C/EBP family members.
Our specific aims, which are designed to define the precise molecular mechanisms which mediate transcription factor interaction in CRP induction, are: I. To define the role of STAT family members in IL-6 induced transcriptional activation of CRP. II. To determine which transcription factors activated by IL-1beta lead to enhanced CRP gene expression in the presence of IL-6 and to define their response elements III. To elucidate the molecular mechanisms by which interaction between these cytokine-activated transcription factors leads to increased CRP transcription, with particular emphasis on a) requirements for orientation, phase and optimal distance between cis elements, b) the possibility that one transcription factor may enhance binding of another factor to cis elements and c) possible physical contact between factors. These studies will cast light on the molecular mechanisms regulating hepatocyte expression of genes whose products are important to the body's defense mechanisms against infection and tissue injury. They are especially relevant to the elderly, who are particularly vulnerable to these processes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG002467-18
Application #
2882050
Study Section
Medical Biochemistry Study Section (MEDB)
Program Officer
Sierra, Felipe
Project Start
1985-02-01
Project End
2000-07-31
Budget Start
1999-04-01
Budget End
2000-07-31
Support Year
18
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Young, Duprane Pedaci; Kushner, Irving; Samols, David (2008) Binding of C/EBPbeta to the C-reactive protein (CRP) promoter in Hep3B cells is associated with transcription of CRP mRNA. J Immunol 181:2420-7
Chakravarty, Kaushik; Hanson, Richard W (2007) Insulin regulation of phosphoenolpyruvate carboxykinase-c gene transcription: the role of sterol regulatory element-binding protein 1c. Nutr Rev 65:S47-56
Cha-Molstad, Hyunjoo; Young, Duprane Pedaci; Kushner, Irving et al. (2007) The interaction of C-Rel with C/EBPbeta enhances C/EBPbeta binding to the C-reactive protein gene promoter. Mol Immunol 44:2933-42
Schwartz, Randall; Osborne-Lawrence, Sherri; Hahner, Lisa et al. (2007) C-reactive protein downregulates endothelial NO synthase and attenuates reendothelialization in vivo in mice. Circ Res 100:1452-9
Vongpatanasin, Wanpen; Thomas, Gail D; Schwartz, Randall et al. (2007) C-reactive protein causes downregulation of vascular angiotensin subtype 2 receptors and systolic hypertension in mice. Circulation 115:1020-8
Jiang, S; Xia, D; Samols, D (2006) Expression of rabbit C-reactive protein in transgenic mice inhibits development of antigen-induced arthritis. Scand J Rheumatol 35:351-5
Kushner, Irving; Rzewnicki, Debra; Samols, David (2006) What does minor elevation of C-reactive protein signify? Am J Med 119:166.e17-28
Mineo, Chieko; Gormley, Andrew K; Yuhanna, Ivan S et al. (2005) FcgammaRIIB mediates C-reactive protein inhibition of endothelial NO synthase. Circ Res 97:1124-31
Chakravarty, Kaushik; Wu, Shwu-Yuan; Chiang, Cheng-Ming et al. (2004) SREBP-1c and Sp1 interact to regulate transcription of the gene for phosphoenolpyruvate carboxykinase (GTP) in the liver. J Biol Chem 279:15385-95
Black, Steven; Agrawal, Alok; Samols, David (2003) The phosphocholine and the polycation-binding sites on rabbit C-reactive protein are structurally and functionally distinct. Mol Immunol 39:1045-54

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