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Publication : Canonical Notch activation in osteocytes causes osteopetrosis.

First Author  Canalis E Year  2016
Journal  Am J Physiol Endocrinol Metab Volume  310
Issue  2 Pages  E171-82
PubMed ID  26578715 Mgi Jnum  J:235906
Mgi Id  MGI:5803931 Doi  10.1152/ajpendo.00395.2015
Citation  Canalis E, et al. (2016) Canonical Notch activation in osteocytes causes osteopetrosis. Am J Physiol Endocrinol Metab 310(2):E171-82
abstractText  Activation of Notch1 in cells of the osteoblastic lineage inhibits osteoblast differentiation/function and causes osteopenia, whereas its activation in osteocytes causes a distinct osteopetrotic phenotype. To explore mechanisms responsible, we established the contributions of canonical Notch signaling (Rbpjkappa dependent) to osteocyte function. Transgenics expressing Cre recombinase under the control of the dentin matrix protein-1 (Dmp1) promoter were crossed with Rbpjkappa conditional mice to generate Dmp1-Cre(+/-);Rbpjkappa(Delta/Delta) mice. These mice did not have a skeletal phenotype, indicating that Rbpjkappa is dispensable for osteocyte function. To study the Rbpjkappa contribution to Notch activation, Rosa(Notch) mice, where a loxP-flanked STOP cassette is placed between the Rosa26 promoter and the NICD coding sequence, were crossed with Dmp1-Cre transgenic mice and studied in the context (Dmp1-Cre(+/-);Rosa(Notch);Rbpjkappa(Delta/Delta)) or not (Dmp1-Cre(+/-);Rosa(Notch)) of Rbpjkappa inactivation. Dmp1-Cre(+/-);Rosa(Notch) mice exhibited increased femoral trabecular bone volume and decreased osteoclasts and bone resorption. The phenotype was reversed in the context of the Rbpjkappa inactivation, demonstrating that Notch canonical signaling was accountable for the phenotype. Notch activation downregulated Sost and Dkk1 and upregulated Axin2, Tnfrsf11b, and Tnfsf11 mRNA expression, and these effects were not observed in the context of the Rbpjkappa inactivation. In conclusion, Notch activation in osteocytes suppresses bone resorption and increases bone volume by utilization of canonical signals that also result in the inhibition of Sost and Dkk1 and upregulation of Wnt signaling.
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