Glucocorticoids suppress bone formation via the osteoclast
Hyun-Ju Kim, … , F. Patrick Ross, Steven L. Teitelbaum
Hyun-Ju Kim, … , F. Patrick Ross, Steven L. Teitelbaum
Published August 1, 2006
Citation Information: J Clin Invest. 2006;116(8):2152-2160. https://doi.org/10.1172/JCI28084.
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Glucocorticoids suppress bone formation via the osteoclast

Abstract

The pathogenesis of glucocorticoid-induced (GC-induced) bone loss is unclear. For example, osteoblast apoptosis is enhanced by GCs in vivo, but they stimulate bone formation in vitro. This conundrum suggests that an intermediary cell transmits a component of the bone-suppressive effects of GCs to osteoblasts in the intact animal. Bone remodeling is characterized by tethering of the activities of osteoclasts and osteoblasts. Hence, the osteoclast is a potential modulator of the effect of GCs on osteoblasts. To define the direct impact of GCs on bone-resorptive cells, we compared the effects of dexamethasone (DEX) on WT osteoclasts with those derived from mice with disruption of the GC receptor in osteoclast lineage cells (GRoc–/– mice). While the steroid prolonged longevity of osteoclasts, their bone-degrading capacity was suppressed. The inhibitory effect of DEX on bone resorption reflects failure of osteoclasts to organize their cytoskeleton in response to M-CSF. DEX specifically arrested M-CSF activation of RhoA, Rac, and Vav3, each of which regulate the osteoclast cytoskeleton. In all circumstances GRoc–/– mice were spared the impact of DEX on osteoclasts and their precursors. Consistent with osteoclasts modulating the osteoblast-suppressive effect of DEX, GRoc–/– mice are protected from the steroid’s inhibition of bone formation.

Authors

Hyun-Ju Kim, Haibo Zhao, Hideki Kitaura, Sandip Bhattacharyya, Judson A. Brewer, Louis J. Muglia, F. Patrick Ross, Steven L. Teitelbaum

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Figure 8

GRoc–/– mice are protected from DEX-suppressed bone formation.

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GRoc–/– mice are protected from DEX-suppressed bone f...
WT and GRoc–/– mice were injected with DEX (10 mg/kg) or vehicle daily for 14 days. Calcein was administered 8 and 2 days prior to sacrifice. (A) Fluorescent micrographs of representative calcein labels. Magnification, ×100. (B) Measured mineral apposition rate. (C) Measured bone formation rate. (D) Serum osteocalcin levels at sacrifice. (E) Serum alkaline phosphatase (ALP) levels at sacrifice. (F) Percentage of osteocytes in histological sections of bone undergoing apoptosis. *P < 0.05, **P < 0.005 versus control.