NLRC3 attenuates osteoclastogenesis by limiting TNF α+ Th17 cell response in osteoporosis

In this study, we transferred the wild-type and NLRC3−/− CD4+ cells into Rag1−/− mice. Consequently, we evidenced the effects of NLRC3 in CD4+ T cells on inhibiting the accumulation of TNF α + Th17 cells, thus restricting bone loss in the OVX mice. Simultaneously, NLRC3−/− CD4+ T cells promoted the recruitment of osteoclast precursors and inflammatory monocytes into the OVX mouse bone marrow. Mechanism-wise, NLRC3 reduced the secretion of TNF α + Th17 cells of RANKL, MIP1α, and MCP1, depending on the T cells. In addition, NLRC3 negatively regulated the Th17 osteoclastogenesis promoting functions via limiting the NF-κB activation. Collectively, this study appreciated the effect of NLRC3 on modulating bone mass via adaptive immunity depending on CD4+ cells. According to findings of this study, NLRC3 may be the candidate anti-OP therapeutic target.Key messagesNLRC3 negatively regulated the Th17 osteoclastogenesis promoting functions via limiting the NF- κB activation.NLRC3 may be the candidate anti-OP therapeutic target.
Source: Journal of Molecular Medicine - Category: Molecular Biology Source Type: research