Relative Impact of Androgen and Estrogen Receptor Activation in the Effects of Androgens on Trabecular and Cortical Bone in Growing Male Mice: A Study in the Androgen Receptor Knockout Mouse Model

Venken, Katrien; Gendt, Karel De; Boonen, Steven; Ophoff, Jill; Bouillon, Roger; Swinnen, Johannes V.; Verhoeven, Guido; Vanderschueren, Dirk

doi:10.1359/jbmr.060103

Cited by 168 publications

(134 citation statements)

References 49 publications

Supporting

Mentioning

109

Contrasting

Unclassified

Order By: Relevance

“…Treatments with aromatizable as well as nonaromatizable androgens are able to prevent ORX-induced decrease of trabecular and cortical bone mass in ORX mice but not in ARKO male mice. (5) These observations provide further evidence for a major role for AR activation in normal trabecular bone development and periosteal bone growth in male mice. It is presently unclear, however, what the target cells are for ARmediated actions on bone.…”

Section: Introductionsupporting

confidence: 52%

“…(12,13) The absence of a major cortical phenotype across a number of similar mice models contrasts with the significant cortical phenotype characterized by reduction of periosteal expansion observed in the ubiquitous ARKO model. (5) Puberty appears to be a critical period for the development of skeletal sexual dimorphism as characterized by wider and longer bones in male. During puberty, androgens have been shown to enhance cortical bone development in male mice.…”

Section: Discussionmentioning

confidence: 99%

“…(27) The AR appears to be critically involved in this effect because both nonaromatizable androgens and aromatizable androgens enhance skeletal development in animals with a functional AR. (5) Although a functional AR in a number of nonosteocyte bone cells, such as immature periosteal bone cells or osteoclasts, may be partly responsible for AR-mediated androgen action during puberty, it should be noted that AR expression is much lower in these cells than in osteocytes. (28) Estrogen and estrogen receptor alpha activation after aromatization of androgens play a role in cortical bone development as well, as illustrated by the cortical phenotype in AR-ERa double-knockout mice.…”

Section: Discussionmentioning

confidence: 99%

See 2 more Smart Citations

Androgen receptor (AR) in osteocytes is important for the maintenance of male skeletal integrity: Evidence from targeted AR disruption in mouse osteocytes

Sinnesael

Claessens

Laurent

et al. 2012

Journal of Bone and Mineral Research

Self Cite

102

View full text Add to dashboard Cite

Androgens play a key role in the maintenance of male skeletal integrity. The regulation of this integrity by androgen receptor (AR) signaling has been mainly attributed to osteoblasts. Although osteocytes have emerged as key regulators of bone remodeling, the influence of sex steroids on these cells has been poorly studied. We aimed to investigate the role of AR signaling, specifically in osteocytes using the Cre/LoxP system in male mice (driven by dentin matrix protein 1 [ocy-ARKOs]). Osteocyte fractions of control (AR(ex2)/Y) and ocy-ARKO (ARflox(ex2)/Y; DMP1-cre) mice isolated through sequential collagenase digestion showed increasing AR expression toward the mature osteocyte fraction of control males compared with the more immature fractions, whereas this was reduced by >80% in ocy-ARKO osteocytes. The skeletal phenotype of mutant mice was further assessed by histomorphometry and quantitative micro-computed tomography at 12 and 32 weeks of age. Ocy-ARKOs had significantly lower trabecular bone volume and number in femora and tibias at 32 weeks as well as decreased trabecular number in the L 5 vertebra at 12 weeks. Biomechanical testing showed that ocy-ARKO femora were also stiffer and required a lower ultimate force to induce failure at 32 weeks. However, femoral cortical structure was not significantly different at any time point. The absence of AR in osteocyte also did not appear to affect trabecular bone formation nor its response to mechanical loading. In conclusion, selective inactivation of the AR in osteocytes of male mice accelerates age-related deterioration of skeletal integrity. These findings provide evidence for a direct role of androgens in the maintenance of trabecular bone through actions of the AR in osteocytes. ß

show abstract

Section: Introductionsupporting

confidence: 52%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Androgen receptor (AR) in osteocytes is important for the maintenance of male skeletal integrity: Evidence from targeted AR disruption in mouse osteocytes

Sinnesael

Claessens

Laurent

et al. 2012

Journal of Bone and Mineral Research

Self Cite

102

View full text Add to dashboard Cite

show abstract

“…Although skeletal size and volume are similar in prepubertal girls and boys (Kelly et al 1990, Seeman 2001, Vanderschueren et al 2004, Kirmani et al 2009, Callewaert et al 2010a, the sexual dimorphism in bone growth becomes apparent during puberty, at which time men reach higher peak bone mass (Clarke & Khosla 2010). This skeletal sexual dimorphism is mainly due to a stimulatory androgen action on periosteal bone formation in men, whereas an inhibitory estrogen-related action occurs in women (Bertelloni et al 1995, Finkelstein et al 1996, Katznelson et al 1996, Seeman 2001, Venken et al 2006, Kirmani et al 2009). Since an excess of androgen in women is associated with higher bone mineral density, there is evidence that androgens also affect peak bone mass in women (Buchanan et al 1988, Zborowski et al 2000, Wei et al 2010.…”

Section: Sex Steroid Hormones Regulate Bone Growthmentioning

confidence: 99%

The mutual dependence between bone and gonads

Karsenty¹

2012

Journal of Endocrinology

View full text Add to dashboard Cite

It has long been known that sex steroid hormones regulate bone mass accrual. This observation raises the testable hypothesis that bone may in turn regulate the synthesis and secretion of sex steroid hormones in one or both genders. This hypothesis is comprised within a more general hypothesis that bone mass, energy metabolism, and reproduction are regulated coordinately. The identification of osteocalcin as an osteoblast-specific secreted molecule allows us to address this question in molecular terms. This review details how the regulation of male fertility by osteocalcin was unraveled, and how osteocalcin signaling in Leydig cells of the testis occurs. It also discusses the implication of this novel mode of regulation of testosterone synthesis observed in males but not in females.

show abstract

“…9,12 A full AR knockout has been shown to exhibit increased bone turnover and reduced trabecular and cortical bone volume in male mice. [13][14][15][16] Further elimination of estrogen receptor a (ERa) caused an additional reduction in cortical bone mass. 14 In another full AR knockout model, the bone growth and composition of knockout female mice were indistinguishable from those of wild-type (WT) mice at 8 weeks of age, 17 suggesting that the AR is not important during the early development or rapid growth phase of the female skeleton.…”

Section: Introductionmentioning

confidence: 99%

Inactivation of the androgen receptor in bone-forming cells leads to trabecular bone loss in adult female mice

et al. 2013

View full text Add to dashboard Cite

Removal of the androgen receptor (AR) from bone-forming cells has been shown to reduce trabecular bone volume in male mice. In female mice, the role of AR in the regulation of bone homeostasis has been poorly understood. We generated a mouse strain in which the AR is completely inactivated only in mineralizing osteoblasts and osteocytes by breeding mice carrying osteocalcin promoter-regulated Cre-recombinase with mice possessing loxP recombination sites flanking exon 2 of the AR gene (AR DOB/DOB mice). In female AR DOB/DOB mice, the trabecular bone volume was reduced owing to a smaller number of trabeculae at 6 months of age compared with the control AR fl/fl animals. In male AR DOB/DOB mice, an increase in trabecular bone separation could already be detected at 3.5 months of age, and at 6 months, the trabecular bone volume was significantly reduced compared with that of male AR fl/fl mice. No AR-dependent changes were observed in the cortical bone of either sex. On the basis of micro-computed tomography and histomorphometry, we conclude that in male mice, the AR is involved in the regulation of osteoclast number by osteoblasts, whereas in female mice, the lack of the AR in the bone-forming cells leads to a decreased number of trabeculae upon aging.

show abstract

Relative Impact of Androgen and Estrogen Receptor Activation in the Effects of Androgens on Trabecular and Cortical Bone in Growing Male Mice: A Study in the Androgen Receptor Knockout Mouse Model

Cited by 168 publications

References 49 publications

Androgen receptor (AR) in osteocytes is important for the maintenance of male skeletal integrity: Evidence from targeted AR disruption in mouse osteocytes

Androgen receptor (AR) in osteocytes is important for the maintenance of male skeletal integrity: Evidence from targeted AR disruption in mouse osteocytes

The mutual dependence between bone and gonads

Inactivation of the androgen receptor in bone-forming cells leads to trabecular bone loss in adult female mice

Contact Info

Product

Resources

About