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Repression of Osteoblast Maturation by ERRα Accounts for Bone Loss Induced by Estrogen Deficiency
Author(s) -
Marlène Gallet,
Soraya Saïdi,
Eric Haÿ,
Johann Photsavang,
Caroline Marty,
Juliette Sailland,
Julie Carnesecchi,
Violaine Tribollet,
Bruno Barenton,
Christelle Forcet,
MarieChristine Birling,
Tania Sorg,
Olivier Chassande,
Martine CohenSolal,
Jean-Marc Vanacker
Publication year - 2013
Publication title -
plos one
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.99
H-Index - 332
ISSN - 1932-6203
DOI - 10.1371/journal.pone.0054837
Subject(s) - osteoblast , endocrinology , medicine , estrogen , estrogen receptor , in vivo , chemistry , biology , microbiology and biotechnology , in vitro , genetics , biochemistry , cancer , breast cancer
ERRα is an orphan member of the nuclear receptor family, the complete inactivation of which confers resistance to bone loss induced by ageing and estrogen withdrawal to female mice in correlation with increased bone formation in vivo . Furthermore ERRα negatively regulates the commitment of mesenchymal cells to the osteoblast lineage ex vivo as well as later steps of osteoblast maturation. We searched to determine whether the activities of ERRα on osteoblast maturation are responsible for one or both types of in vivo induced bone loss. To this end we have generated conditional knock out mice in which the receptor is normally present during early osteoblast differentiation but inactivated upon osteoblast maturation. Bone ageing in these animals was similar to that observed for control animals. In contrast conditional ERRαKO mice were completely resistant to bone loss induced by ovariectomy. We conclude that the late (maturation), but not early (commitment), negative effects of ERRα on the osteoblast lineage contribute to the reduced bone mineral density observed upon estrogen deficiency.

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