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Journal of Pharmacology And Experimental Therapeutics Fast Forward
First published on May 9, 2008; DOI: 10.1124/jpet.107.133702

0022-3565/08/3262-514-522$20.00
JPET 326:514-522, 2008
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INFLAMMATION, IMMUNOPHARMACOLOGY, AND ASTHMA

Compounds That Increase or Mimic Cyclic Adenosine Monophosphate Enhance Tristetraprolin Degradation in Lipopolysaccharide-Treated Murine J774 Macrophages

Ulla Jalonen, Erja-Leena Paukkeri, and Eeva Moilanen

The Immunopharmacology Research Group, Medical School, University of Tampere and Research Unit, Tampere University Hospital, Tampere, Finland

Tristetraprolin (TTP) is a trans-acting factor that can regulate mRNA stability by binding to the cis-acting AU-rich element (ARE) in the 3'-untranslated region in mRNAs of certain transiently expressed genes. The best-studied target of TTP is tumor necrosis factor (TNF)-{alpha}. By binding to ARE, TTP increases the degradation of TNF-{alpha} mRNA, thereby reducing the expression of TNF-{alpha}. We examined the effects of cAMP analogs and the cAMP-elevating agents forskolin and β2-agonists on lipopolysaccharide (LPS)-induced TTP mRNA and protein expression by quantitative real-time reverse transcriptase-polymerase chain reaction and Western blotting in activated macrophages. All of these agents caused a slight increase in LPS-induced expression of TTP mRNA. However, TTP protein levels were significantly reduced when the cells were treated with the combination of LPS and cAMP-elevating agent compared with LPS alone. Proteasome inhibitors MG132 (N-[(phenylmethoxy)-carbonyl]-L-leucyl-N-[(1S)-1-formyl-3-methylbutyl]-L-leucinamide) and lactacystin increased TTP protein levels and abolished the effects of cAMP-enhancing compounds on TTP protein levels. The results suggest that mediators and drugs that enhance intracellular cAMP reduce TTP expression in macrophages exposed to inflammatory stimuli by increasing TTP degradation through the proteasome pathway.

Received November 6, 2007; accepted May 8, 2008.

Address correspondence to: Dr. Eeva Moilanen, Medical School, Immunopharmacology, FIN-33014 University of Tampere, Finland. E-mail: eeva.moilanen{at}uta.fi






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