RANKL coordinates multiple osteoclastogenic pathways by regulating expression of ubiquitin ligase RNF146
Yoshinori Matsumoto, … , Feng Cong, Robert Rottapel
Yoshinori Matsumoto, … , Feng Cong, Robert Rottapel
Published March 13, 2017
Citation Information: J Clin Invest. 2017;127(4):1303-1315. https://doi.org/10.1172/JCI90527.
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Research Article Bone biology Cell biology

RANKL coordinates multiple osteoclastogenic pathways by regulating expression of ubiquitin ligase RNF146

Abstract

Bone undergoes continuous remodeling due to balanced bone formation and resorption mediated by osteoblasts and osteoclasts, respectively. Osteoclasts arise from the macrophage lineage, and their differentiation is dependent on RANKL, a member of the TNF family of cytokines. Here, we have provided evidence that RANKL controls the expression of 3BP2, an adapter protein that is required for activation of SRC tyrosine kinase and simultaneously coordinates the attenuation of β-catenin, both of which are required to execute the osteoclast developmental program. We found that RANKL represses the transcription of the E3 ubiquitin ligase RNF146 through an NF-κB–related inhibitory element in the RNF146 promoter. RANKL-mediated suppression of RNF146 results in the stabilization of its substrates, 3BP2 and AXIN1, which consequently triggers the activation of SRC and attenuates the expression of β-catenin, respectively. Depletion of RNF146 caused hypersensitivity to LPS-induced TNF-α production in vivo. RNF146 thus acts as an inhibitory switch to control osteoclastogenesis and cytokine production and may be a control point underlying the pathogenesis of chronic inflammatory diseases.

Authors

Yoshinori Matsumoto, Jose Larose, Oliver A. Kent, Melissa Lim, Adele Changoor, Lucia Zhang, Yaryna Storozhuk, Xiaohong Mao, Marc D. Grynpas, Feng Cong, Robert Rottapel

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Figure 5

Stabilization of 3BP2 is required for activated osteoclasts and TNF-α production in Rnf146fl/fl LysM-Cre osteoclast progenitors.

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Stabilization of 3BP2 is required for activated osteoclasts and TNF-α pr...
(A) Whole cell lysates from primary murine osteoclast progenitors derived from WT and Rnf146fl/fl LysM-Cre (KO) mice were probed with the indicated antibodies for Western blot analysis. (B and C) TRAP staining (B) or resorption pit assay (C) of osteoclasts derived from WT, Rnf146fl/fl LysM-Cre (KO), and Rnf146fl/fl Sh3bp2fl/fl LysM-Cre (dKO) osteoclast progenitors cultured in the presence or absence of RANKL for 7 days. Original magnification, ×40. n = 3. (D) Whole cell lysates from cells in B were probed with the indicated antibodies for Western blot analysis. (EG) qPCR analysis of Ctsk (E), Calcr (F), and Acp5 (G) mRNA expression in primary murine osteoclast progenitors derived from WT, Rnf146fl/fl LysM-Cre (KO), and Rnf146fl/fl Sh3bp2fl/fl LysM-Cre (dKO) mice and cultured in the presence of RANKL for 0 to 3 days. The relative expression of each mRNA was normalized to that in WT cells at day 3. n = 3. (H) qPCR analysis of Tnfα mRNA expression in primary murine osteoclast progenitors derived from WT, Rnf146fl/fl LysM-Cre (KO), and Rnf146fl/fl Sh3bp2fl/fl LysM-Cre (dKO) mice and cultured in the presence of LPS (10 ng/ml) for 0 to 24 hours. n = 3. (I) WT, Rnf146fl/fl LysM-Cre (KO), and Rnf146fl/fl Sh3bp2fl/fl LysM-Cre (dKO) mice were injected i.p. with LPS, and TNF-α in the serum was measured by ELISA 4 hours later. n = 6. P values were determined by ANOVA with Tukey-Kramer’s post hoc test (BI) or unpaired t test (A). Data are presented as mean ± SEM. *P < 0.05.