| Literature DB >> 27669656 |
Marc Baud'huin1, François Lamoureux2, Camille Jacques2, Lidia Rodriguez Calleja2, Thibaut Quillard2, Céline Charrier2, Jérome Amiaud2, Martine Berreur2, Bénédicte Brounais-LeRoyer2, Robert Owen3, Gwendolen C Reilly3, James E Bradner4, Dominique Heymann1, Benjamin Ory5.
Abstract
Histone modifications are important for maintaining the transcription program. BET proteins, an important class of "histone reading proteins", have recently been described as essential in bone biology. This study presents the therapeutic opportunity of BET protein inhibition in osteoporosis. We find that the pharmacological BET protein inhibitor JQ1 rescues pathologic bone loss in a post-ovariectomy osteoporosis model by increasing the trabecular bone volume and restoring mechanical properties. The BET protein inhibition suppresses osteoclast differentiation and activity as well as the osteoblastogenesis in vitro. Moreover, we show that treated non-resorbing osteoclasts could still activate osteoblast differentiation. In addition, specific inhibition of BRD4 using RNA interference inhibits osteoclast differentiation but strongly activates osteoblast mineralization activity. Mechanistically, JQ1 inhibits expression of the master osteoclast transcription factor NFATc1 and the transcription factor of osteoblast Runx2. These findings strongly support that targeting epigenetic chromatin regulators such as BET proteins may offer a promising alternative for the treatment of bone-related disorders such as osteoporosis. Copyright ÂEntities:
Keywords: Bromodomain; Epigenetic; Inhibitor; Osteoblast; Osteoclast; Osteoporosis
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Year: 2016 PMID: 27669656 DOI: 10.1016/j.bone.2016.09.020
Source DB: PubMed Journal: Bone ISSN: 1873-2763 Impact factor: 4.398