Elevated levels of the cytokine interleukin-10 (IL-10) have been reported in patients with active systemic lupus erythematosus (SLE). Any role for IL-10 in the pathogenesis of SLE is likely to involve the activation of expression of specific genes within its target cells. We have previously reported elevated levels of the 90000 MW heat-shock protein (hsp 90) and autoantibodies to hsp 90 in patients with SLE. Recent studies have shown that the cytokine IL-6 activates hsp 90 gene expression via specific transcription factors that include STAT-3 (signal transducer and activator of transcription 3). In view of the known role of STAT proteins in IL-10 signalling pathways, we have investigated the effect of IL-10 on hsp 90 gene expression. Here we report that IL-10 enhances the expression of hsp 90 in both a human hepatoma cell line (HepG2) stably expressing the human IL-10 receptor and peripheral blood mononuclear cells (PBMC). In reporter gene assays IL-10 is able to activate both the hsp 90 alpha and hsp 90 beta promoters directly. Furthermore, a short region of the hsp 90 beta promoter which is activated in response to IL-10, contains a STAT-3 binding site. This element but not a mutant derivative unable to bind STAT-3, is able to confer a response to IL-10 on a heterologous promoter. These results may be understood in terms of the shared signalling mechanisms of IL-10 and IL-6 and provide evidence of a role for IL-10 in the overexpression of hsp 90 in SLE, with possible pathological consequences.
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UCL, Inst Child Hlth, Med Mol Biol Unit, 30 Guilford St, London WC1N 1EH, EnglandUCL, Inst Child Hlth, Med Mol Biol Unit, 30 Guilford St, London WC1N 1EH, England
Stephanou, Anastasis
Latchman, David S.
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UCL, Inst Child Hlth, Med Mol Biol Unit, 30 Guilford St, London WC1N 1EH, EnglandUCL, Inst Child Hlth, Med Mol Biol Unit, 30 Guilford St, London WC1N 1EH, England
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UNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCEUNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCE
COUMAILLEAU, P
BILLOUD, B
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UNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCEUNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCE
BILLOUD, B
SOURROUILLE, P
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UNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCEUNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCE
SOURROUILLE, P
MOREAU, N
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UNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCEUNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCE
MOREAU, N
ANGELIER, N
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UNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCEUNIV PARIS 06,DEPT MOLEC CELLULAR & DEV BIOL,GRP GENES & DEV,CNRS,UA 1135,F-75252 PARIS 05,FRANCE