A functional androgen receptor is not sufficient to allow estradiol to protect bone after gonadectomy in estradiol receptor–deficient mice
Natalie A. Sims, Philippe Clément-Lacroix, Dominique Minet, Caroline Fraslon-Vanhulle, Martine Gaillard-Kelly, Michèle Resche-Rigon, Roland Baron
Natalie A. Sims, Philippe Clément-Lacroix, Dominique Minet, Caroline Fraslon-Vanhulle, Martine Gaillard-Kelly, Michèle Resche-Rigon, Roland Baron
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Article Bone biology

A functional androgen receptor is not sufficient to allow estradiol to protect bone after gonadectomy in estradiol receptor–deficient mice

Abstract

Although the role of estradiol in maintaining bone mass is well established, the relative contributions of the estradiol receptors ERα and ERβ and of the androgen receptor (AR) remain controversial. To determine the role of ERα-mediated, ERβ-mediated, and non–ER-mediated mechanisms in maintaining bone mass, gonadectomy and estradiol treatment were studied in ER-knockout mice. Estradiol treatment of ovariectomized ERαβ–/– mice failed to prevent bone loss, precluding significant effects of estradiol on bone through non–ER-signaling pathways. In contrast, estradiol prevented ovariectomy-induced bone loss in ERβ–/– mice, as in WT males and females, indicating that ERα is the major mediator of estradiol effects in bone. No response of bone to estradiol was detected in orchidectomized ERα–/– mice, suggesting estradiol cannot protect bone mass via the AR in vivo. In contrast to female ERαβ–/– and male ERα–/– mice, female ERα–/– mice were partially protected against ovariectomy-induced bone loss by estradiol, confirming that ERβ mediates estradiol effects in bone, but only in females and with a lower efficacy than ERα. We conclude that ERα is the main effector of estradiol’s protective function in bone in both male and female mice, and that, in its absence, AR is not sufficient to mediate this response.

Authors

Natalie A. Sims, Philippe Clément-Lacroix, Dominique Minet, Caroline Fraslon-Vanhulle, Martine Gaillard-Kelly, Michèle Resche-Rigon, Roland Baron

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Male ERα–/– mice do not respond to estradiol (E2) treatment. (a) Represe...
Male ERα–/– mice do not respond to estradiol (E2) treatment. (a) Representative von Kossa–stained sections of the proximal tibia from WT and ERα–/– males sham-operated, orchidectomized (Orx), or orchidectomized and treated with slow-release pellets delivering 50 μg/kg/d estradiol (Orx+E2). (b) BV/TV and Tb.BMD were increased after estradiol treatment in WT mice, but estradiol treatment did not alter BV/TV or Tb.BMD in ERα–/– males. (c) ObS/BS, bone formation rate expressed as a percentage of trabecular bone surface (BFR/BS), and OcS/BS were all elevated after orchidectomy in WT and ERα–/– males. This was prevented by estradiol treatment in WT but not in ERα–/– males. The increased ObS/BS and OcS/BS were prevented by estradiol treatment in WT males, but not in ERα–/– males. BFR/BS was further elevated in WT males treated with estradiol but remained unchanged in treated ERα–/– males. Values are mean ± SEM. *P < 0.05, **P < 0.01, ***P < 0.001 vs. sham-operated of the same genotype; ++P < 0.01, +++P < 0.001 vs. Orx of the same genotype.