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W1895332014 abstract "The host response to pathogens through nuclear factor κB (NF-κB) is an essential defense mechanism for eukaryotic organisms. NF-κB-mediated host responses inhibit bone and other connective tissue synthesis and are thought to affect the transcription of matrix proteins through multiple indirect pathways. We demonstrate that inhibiting NF-κB in osteoblasts increases osteocalcin expression in vivo in mice with periodontal disease. Mutating NF-κB binding sites on osteocalcin (OC) or bone sialoprotein (Bsp) promoters rescues the negative impact of NF-κB on their transcription and that NF-κB can inhibit Wnt- and Bmp-induced OC and Bsp transcription, even when protein synthesis is inhibited, indicating a direct effect of NF-κB. This inhibition depends on p65-p50 NF-κB heterodimer formation and deacetylation by HDAC1 but is not affected by the noncanonical NF-κB pathway. Moreover, NF-κB reduces Runx2 and β-catenin binding to OC/Bsp promoters independently of their nuclear localization. Thus, inflammatory signals stimulate the direct interaction of NF-κB with response elements to inhibit binding of β-catenin and Runx2 binding to nearby consensus sites and reduce expression of matrix proteins. This direct mechanism provides a new explanation for the rapid decrease in new bone formation after inflammation-related NF-κB activation. © 2015 American Society for Bone and Mineral Research." @default.
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W1895332014 date "2015-08-06" @default.
W1895332014 modified "2023-09-25" @default.
W1895332014 title "NF-κB Has a Direct Role in Inhibiting Bmp- and Wnt-Induced Matrix Protein Expression" @default.
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W1895332014 doi "https://doi.org/10.1002/jbmr.2592" @default.
W1895332014 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4713353" @default.
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