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Class <scp>II</scp>‐specific histone deacetylase inhibitors <scp>MC</scp>1568 and <scp>MC</scp>1575 suppress <scp>IL</scp>‐8 expression in human melanoma cells
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2012
Year
ImmunologyDermatologyCancer BiologyTumor BiologyCancer Cell BiologyCancer ResearchMelanomaIl-8 PromoterIl-8 TranscriptionEpigenetic RegulationCell BiologyTumor MicroenvironmentChromatin FunctionChromatinChromatin StructureHuman MelanomaNatural SciencesHuman Melanoma CellsTumor SuppressorMedicine
Here, we explored the effects of the novel class II-specific histone deacetylase inhibitors (HDACis) MC1568 and MC1575 on interleukin-8 (IL-8) expression and cell proliferation in cutaneous melanoma cell line GR-M and uveal melanoma cell line OCM-3 upon stimulation with phorbol 12-myristate 13-acetate (PMA). We found that PMA upregulated IL-8 transcription via the AP-1 binding site and identified c-Jun as the transcription factor involved in this eventS. MC1568 and MC1575 inhibited IL-8 levels and cell proliferation in either unstimulated or PMA-stimulated melanoma cells. They acted by suppressing (i) c-Jun binding to the IL-8 promoter, (ii) recruitment of histones 3 and 4, RNA polymerase II and TFIIB to the c-Jun promoter, and (iii) c-Jun expression. Our findings provide new insights into mechanisms underlying anti-tumoral activities of class II-specific HDACis in human melanoma and suggest that they may constitute a novel therapeutic strategy for improving the treatment of this cancer.
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