Salt-inducible kinases dictate parathyroid hormone 1 receptor action in bone development and remodeling
Shigeki Nishimori, … , Henry M. Kronenberg, Marc N. Wein
Shigeki Nishimori, … , Henry M. Kronenberg, Marc N. Wein
Published August 20, 2019
Citation Information: J Clin Invest. 2019;129(12):5187-5203. https://doi.org/10.1172/JCI130126.
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Research Article Bone biology Endocrinology

Salt-inducible kinases dictate parathyroid hormone 1 receptor action in bone development and remodeling

Abstract

The parathyroid hormone 1 receptor (PTH1R) mediates the biologic actions of parathyroid hormone (PTH) and parathyroid hormone–related protein (PTHrP). Here, we showed that salt-inducible kinases (SIKs) are key kinases that control the skeletal actions downstream of PTH1R and that this GPCR, when activated, inhibited cellular SIK activity. Sik gene deletion led to phenotypic changes that were remarkably similar to models of increased PTH1R signaling. In growth plate chondrocytes, PTHrP inhibited SIK3, and ablation of this kinase in proliferating chondrocytes rescued perinatal lethality of PTHrP-null mice. Combined deletion of Sik2 and Sik3 in osteoblasts and osteocytes led to a dramatic increase in bone mass that closely resembled the skeletal and molecular phenotypes observed when these bone cells express a constitutively active PTH1R that causes Jansen’s metaphyseal chondrodysplasia. Finally, genetic evidence demonstrated that class IIa histone deacetylases were key PTH1R-regulated SIK substrates in both chondrocytes and osteocytes. Taken together, our findings establish that SIK inhibition is central to PTH1R action in bone development and remodeling. Furthermore, this work highlights the key role of cAMP-regulated SIKs downstream of GPCR action.

Authors

Shigeki Nishimori, Maureen J. O’Meara, Christian D. Castro, Hiroshi Noda, Murat Cetinbas, Janaina da Silva Martins, Ugur Ayturk, Daniel J. Brooks, Michael Bruce, Mizuki Nagata, Wanida Ono, Christopher J. Janton, Mary L. Bouxsein, Marc Foretz, Rebecca Berdeaux, Ruslan I. Sadreyev, Thomas J. Gardella, Harald Jüppner, Henry M. Kronenberg, Marc N. Wein

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Figure 6

Class IIa HDACs are key downstream mediators of PTH1R/SIK action in the growth plate.

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Class IIa HDACs are key downstream mediators of PTH1R/SIK action in the ...
(A) H&E staining of the whole tibia at birth (original magnification, ×20) reveals that the expanded growth plate in the Sik3-cKO mouse is abrogated when the Hdac4 gene is simultaneously deleted. Each mouse genotype shown is defined as follows: Sik3fl/fl, Sik3-cKO (Sik3fl/fl Col2a1-Cre), Hdac4-cHET Sik3-cKO (Hdac4fl/+ Sik3fl/fl Col2a1-Cre), Hdac4-cKO Sik3-cKO (Hdac4fl/fl Sik3fl/fl Col2a1-Cre), Hdac4-cKO (Hdac4fl/fl Col2a1-Cre). (B) In situ hybridization for Col10a1 mRNA on the proximal tibial growth plate at birth (original magnification, ×40). Numbers represent the average length of the proliferating chondrocyte region (black lines) (mean ± SEM, n = 3, biological triplicates; we measured the average length using 6–9 sections for each mouse). *P < 0.001 by 1-way ANOVA followed by Dunnett’s test, when the Sik3-cKO measurement is control. P values less than 0.05 were considered significant. Scale bars (red lines): 500 µm.