The invasive phenotype of cancers critically depends on the expression of proteases such as the M-R 92,000 type IV collagenase (MMP-9). Several growth factors and oncogenes were found to increase promoter activity and as a consequence protease expression. This frequently requires the activation of the transcription factor AP-1 by signal transduction cascades such as the ERK and JNR pathways. We have previously demonstrated that the tumor promoter TPA can induce MMP-9 expression via a third signaling cascade, the p38 pathway. Considering that TPA is a potent activator of AP-1, we hypothesized that this transcription factor might also be required for p38 path way-dependent MMP-9 regulation. While dominant negative p38 and MKK-6 mutants reduced MMP-9 promoter activity in CAT assays, a construct encoding an activating mutation in the MKK-6 protein potently stimulated it. This was mediated via 144 bp of the 5'flanking region of the wild-type promoter, which contains an AP-1 site at -79. Both point mutations in this motif and the expression of a c-jun protein lacking its transactivation domain and therefore acting as a dominant negative AP-1 mutant abrogated MKK-6-dependent promoter stimulation. Finally SB 203580, a specific p38 pathway inhibitor, reduced MMP-9 expression/secretion and in vitro invasion of cancer cells. Thus, our results provide evidence that also the third SAPK/MAPK signaling cascade, the p38 signal transduction pathway, stimulates MMP-9 expression in an AP-1-dependent fashion. (C) 2001 Elsevier Science.
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Univ Monastir, Biochem Lab, Mol Mech & Dis Res Unit, Fac Med,UR12ES08, BP 5019, Monsatir 5000, TunisiaUniv Monastir, Biochem Lab, Mol Mech & Dis Res Unit, Fac Med,UR12ES08, BP 5019, Monsatir 5000, Tunisia
Aroui, Sonia
Najlaoui, Feten
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Univ Poitiers 7368, ERL CNRS, Georges Bonnet St 1,TSA 51106, F-86073 Poitiers 9, FranceUniv Monastir, Biochem Lab, Mol Mech & Dis Res Unit, Fac Med,UR12ES08, BP 5019, Monsatir 5000, Tunisia
Najlaoui, Feten
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Chtourou, Yassine
Meunier, Annie-Claire
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Univ Poitiers 7368, ERL CNRS, Georges Bonnet St 1,TSA 51106, F-86073 Poitiers 9, FranceUniv Monastir, Biochem Lab, Mol Mech & Dis Res Unit, Fac Med,UR12ES08, BP 5019, Monsatir 5000, Tunisia
Meunier, Annie-Claire
Laajimi, Amel
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Inst Pasteur Tunis, Lab Venins & Therapeut Biomol, LR11IPT08,13, Tunis 1002, TunisiaUniv Monastir, Biochem Lab, Mol Mech & Dis Res Unit, Fac Med,UR12ES08, BP 5019, Monsatir 5000, Tunisia
Laajimi, Amel
Kenani, Abderraouf
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Univ Monastir, Biochem Lab, Mol Mech & Dis Res Unit, Fac Med,UR12ES08, BP 5019, Monsatir 5000, TunisiaUniv Monastir, Biochem Lab, Mol Mech & Dis Res Unit, Fac Med,UR12ES08, BP 5019, Monsatir 5000, Tunisia
Kenani, Abderraouf
Fetoui, Hamadi
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Univ Sfax, Sci Fac Sfax, Lab Toxicol Microbiol & Environm Hlth, UR11ES70, BP1171, Sfax 3000, TunisiaUniv Monastir, Biochem Lab, Mol Mech & Dis Res Unit, Fac Med,UR12ES08, BP 5019, Monsatir 5000, Tunisia
机构:
Univ Lorraine, INSERM, UHP, Ex U961,UMR S U1116, Vandoeuvre Les Nancy, FranceUniv Lorraine, INSERM, UHP, Ex U961,UMR S U1116, Vandoeuvre Les Nancy, France
Gilet, Alexandre
Zou, Feng
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Jianghan Univ, Sch Med, Dept Pathol & Pathophysiol, Wuhan 430056, Hubei Province, Peoples R ChinaUniv Lorraine, INSERM, UHP, Ex U961,UMR S U1116, Vandoeuvre Les Nancy, France
Zou, Feng
Boumenir, Meriem
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Univ Lorraine, INSERM, UHP, Ex U961,UMR S U1116, Vandoeuvre Les Nancy, FranceUniv Lorraine, INSERM, UHP, Ex U961,UMR S U1116, Vandoeuvre Les Nancy, France
Boumenir, Meriem
Frippiat, Jean-Pol
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Lorraine Univ, EA7300, Stress Immun Pathogens Lab, Vandoeuvre Les Nancy, FranceUniv Lorraine, INSERM, UHP, Ex U961,UMR S U1116, Vandoeuvre Les Nancy, France
Frippiat, Jean-Pol
Thomton, Simon N.
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Univ Lorraine, INSERM, UHP, Ex U961,UMR S U1116, Vandoeuvre Les Nancy, FranceUniv Lorraine, INSERM, UHP, Ex U961,UMR S U1116, Vandoeuvre Les Nancy, France