Odile Rimet scite author profile

We showed previously that microtubule disassembly by vinblastine induces the proto-oncogene c-myc in epithelial mammary HBL100 cells. In this study, we demonstrate that vinblastine treatment in these cells, in contrast to what was observed with the colon adenocarcinoma cell line HT29-D4, activated the transcription factor NFkappaB, which has been involved in c-myc regulation. The microtubule disassembly also induced IkappaB degradation. Using transient transfection analysis, we show that the trans-activation of c-myc by vinblastine was decreased when NFkappaB binding sites on c-myc promoter were mutated. Additionally, we demonstrate that microtubule dissolution trans-activated a thymidine kinase-CAT construct containing an NFkappaB binding site at -1180 to -1080 bp relative to the P1 promoter. Thus, vinblastine up-regulates the enhancer activity of the NFkappaB binding site. These results suggest that microtubule disassembly induced by vinblastine can trans-activate the c-myc oncogene through NFkappaB. Taking into consideration the paradoxical roles of both c-myc and NFkappaB in proliferation or apoptosis, this data reveals the complex action mechanism of this microtubule interfering agent.

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Thermodynamic study of dihydrofolate reductase inhibitor selectivity

Sasso

Gilli

Sari

et al. 1994

Biochimica et Biophysica Acta (BBA) - Protein Structure and Mol

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Retinoids repress Ah receptor CYP1A1 induction pathway through the SMRT corepressor

Fallone

Villard

Sérée

et al. 2004

Biochemical and Biophysical Research Communications

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CYP1A1 isoform is mainly regulated by the transcription factor AhR and to a lesser extent by the nuclear receptor RAR. The effect of a coexposure with 3MC, a AhR ligand, and RA, a RAR ligand, which are, respectively, strong and weak CYP1A1 inducers, is poorly known. We showed in Caco-2 cells that addition of RA significantly decreased 3MC-induced CYP1A1 expression by -55% for mRNA level and -30% for promoter and enzymatic activities. We further showed that RA decreased AhR protein level. Moreover, a physical interaction between AhR and the RAR-corepressor SMRT has been described in vitro. Using the corepressor inhibitor TSA, transfected-cells with SMRT cDNA, and coimmunoprecipitation experiments, we demonstrated that RA addition repressed AhR function through a marked AhR/SMRT physical interaction. This interaction explains the decrease of 3MC-induced CYP1A1 expression. This new mechanism involving the repression of AhR-induced CYP1A1 expression by retinoids allows better knowledge of the CYP1A1 regulation.

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Opposite effects of antimicrotubule agents on c-myc oncogene expression depending on the cell lines used

Bourgarel-Rey

Khyari

Rimet

et al. 2000

European Journal of Cancer

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Odile Rimet

Involvement of Nuclear Factor κB in c-Myc Induction by Tubulin Polymerization Inhibitors

Thermodynamic study of dihydrofolate reductase inhibitor selectivity

Retinoids repress Ah receptor CYP1A1 induction pathway through the SMRT corepressor

Opposite effects of antimicrotubule agents on c-myc oncogene expression depending on the cell lines used

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