期刊
JOURNAL OF CLINICAL INVESTIGATION
卷 119, 期 10, 页码 3024-3034出版社
AMER SOC CLINICAL INVESTIGATION INC
DOI: 10.1172/JCI38716
关键词
-
资金
- NIH [AR43S 10, AR48697]
TNF and RANKL mediate bone destruction in common bone diseases, including osteoarthritis and RA. They activate NF-kappa B canonical signaling directly in osteoclast precursors (OCPs) to induce osteoclast formation in vitro. However, unlike RANKL, TNF does not activate the alternative NF-kappa B pathway efficiently to process the I kappa B protein NF-kappa B p100 to NF-kappa B p52, nor does it appear to induce osteoclast formation in vivo in the absence of RANKL. Here, we show that TNF limits RANKL- and TNF-induced osteoclast formation in vitro and in vivo by increasing NF-kappa B p100 protein accumulation in OCPs. In contrast, TNF induced robust osteoclast formation in vivo in mice lacking RANKL or RANK when the mice also lacked NF-kappa B p100, and TNF-Tg mice lacking NF-kappa B p100 had more severe joint erosion and inflammation than did TNF-Tg littermates. TNF, but not RANKL, increased OCP expression of TNF receptor-associated factor 3 (TRAF3), an adapter protein that regulates NF-kappa B p100 levels in B cells. TRAF3 siRNA prevented TNF-induced NF-kappa B p100 accumulation and inhibition of osteoclastogenesis. These findings suggest that upregulation of TRAF3 or NF-kappa B p100 expression or inhibition of NF-kappa B P100 degradation in OCPs could limit bone destruction and inflammation-induced bone loss in common bone diseases.
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