RANK ligand converts the NCoR/HDAC3 co-repressor to a PGC1ß- and RNA-dependent co-activator of osteoclast gene expression [ChIP-seq]

To investigate the genomic localization of NCoR/HDAC3/PGC1ß complex and the enhancer/promoter activity in the regulation of osteoclast differentiation, we used NCoR KO or PGC1ß KO bone marrow cells, non-coding RNA Dancr/Rnu12 siRNA knockdown bone marrow cells and FLAG-tagged PGC1ß RNA recognition motif deletion mutant expressed RAW 264.7 cells. We then performed chromatin immunoprecipitation DNA-sequencing (ChIP-seq) for H3K27ac, NCoR, HDAC3, PGC1ß, p65, Fosl2, PU.1 and FLAG-tag. Overall design: Genomic localization of NCoR/HDAC3/PGC1ß and transcription factors with H3K27 acetylation depending on RANK signal