Androgens and Bone

Vanderschueren, Dirk; Vandenput, Liesbeth; Boonen, Steven; Lindberg, Mattias F.; Bouillon, Roger; Ohlsson, Claes

doi:10.1210/er.2003-0003

Cited by 597 publications

(400 citation statements)

References 341 publications

Supporting

Mentioning

376

Contrasting

Unclassified

Order By: Relevance

“…Each of these factors may contribute to the increased fracture risk associated with male hypogonadism (1,30). Recent findings also highlight that a significant proportion of testosterone effects on bone depends upon aromatization to estradiol (31).…”

Section: Discussionmentioning

confidence: 98%

Adequacy of androgen replacement influences bone density response to testosterone in androgen-deficient men

Aminorroaya

Kelleher²,

Conway³

et al. 2005

eur j endocrinol

View full text Add to dashboard Cite

Objective: Androgen deficiency (AD) leads to bone loss and contributes to osteoporotic fractures in men. Although low bone mineral density (BMD) in AD men is improved by testosterone replacement, the responses vary between individuals but the determinants of this variability are not well defined. Design and methods: Retrospective review of dual energy X-ray absorptiometry (DEXA) of the lumbar spine and proximal femur in men with established AD requiring regular androgen replacement therapy (ART). After a DEXA scan all men were treated with testosterone implants (800 mg, , 6 month intervals). Patients were classified as having a congenital, childhood, or post-pubertal onset, as well as according to the adequacy of treatment prior to their first DEXA scan as untreated, partially treated or well treated. Results: Men with AD requiring regular ART (n ¼ 169, aged 46.3^1.1 years, range 22 -84 years) underwent a DEXA scan prior to being treated with testosterone implants (800 mg, ,6 month intervals). In cross-sectional analysis at the time of the first DEXA scan untreated men (n ¼ 24) had significantly reduced age-adjusted BMD at all four sites (L1 -L4, femoral neck, Ward's triangle and trochanter). Well-treated men (n ¼ 77) had significantly better age-adjusted BMD at all four sites compared with those who were partially treated (n ¼ 66) or untreated (n ¼ 24) with their ageadjusted BMD being normalized. In a longitudinal assessment of men (n ¼ 60) who had two or more serial DEXA scans, at the second DEXA scan after a median of 3 years, men who were previously partially treated (n ¼ 19) or untreated (n ¼ 11) had proportionately greater improvements in BMD, significantly for Ward's triangle (P ¼ 0.025) and the trochanter (P ¼ 0.044) compared with men (n ¼ 30) previously well treated. Conclusions: The present study demonstrates a positive relationship between adequacy of testosterone replacement and BMD in men with overt organic AD. Additionally, the BMD of well-treated AD men approximates that of age-matched non-AD controls. The greatest BMD gains are made by those who have been either untreated or partially treated, and optimal treatment over time (median 3 years) normalizes BMD to the level expected for healthy men of the same age.European Journal of Endocrinology 152 881-886

show abstract

Section: Discussionmentioning

confidence: 98%

Adequacy of androgen replacement influences bone density response to testosterone in androgen-deficient men

Aminorroaya

Kelleher²,

Conway³

et al. 2005

eur j endocrinol

View full text Add to dashboard Cite

show abstract

“…Thus DHT seems not to be necessary for the beneficial effects of testosterone on BMD in men and this evidence indirectly focuses on the positive effects on bone induced by the aromatization of androgens (74). A possible role of DHT on BMD was previously suggested on the basis of animal studies and in vitro research (29), but DHT was able to prevent bone loss in castrated rodents only when used at supraphysiological doses in vivo (75). Even though androgens seem to exert a direct action on bone cells (osteoblast, osteoclast, osteocytes), all these effects linked to the activation of androgen receptor (such as apoptosis, modulation and proliferation of osteoblasts and osteoclasts) have been proved only in vitro or in animal studies (29).…”

Section: Dhtmentioning

confidence: 99%

“…Nowadays it is known that bone tissue is able to produce sex steroids (i.e. estrogens and androgen metabolites) locally (28) and bone represents a target tissue for both locally produced and circulating sex steroids, since both androgen and estrogen receptors (a and b) as well as aromatase enzyme, are expressed in bone cells (29). Thus sex steroids may act on bone in an endocrine, paracrine and autocrine fashion.…”

Section: Aging Sex Steroids and Bone Loss In Menmentioning

confidence: 99%

“…Our understanding of the role of estrogen on human male bone physiology has certainly revisited and, in part, reduced the role of androgens on male bone physiology (29), but a direct action of androgens on bone cannot be ruled out even if its mechanism is now too complex to be characterized in vivo. Paradoxically, we know more about estrogens and less about androgens (Tables 2 and 4).…”

Section: Androgens and Age-related Male Osteoporosismentioning

confidence: 99%

See 1 more Smart Citation

Osteoporosis and male age-related hypogonadism: role of sex steroids on bone (patho)physiology

et al. 2006

View full text Add to dashboard Cite

Male age-related bone loss is caused, at least in part, by hypogonadism that occurs with advancing age. The study of the effects of sex steroids on bone physiology in men has recently highlighted the central role of estrogens on bone pathophysiology. This review focuses on particular aspects of bone physiology and pathophysiology in aging men, noting both the similarities to and the differences from female counterparts. In particular, the role of sex steroids on bone sexual dimorphism in health and disease has been analyzed.

show abstract

“…1,2 Reduction of serum androgen levels in aging men or in patients treated with anti-androgen therapy has been shown to be associated with the reduced bone mineral density (BMD) of the skeleton. 3 In mice, the androgen receptor (AR) is expressed in osteoblasts, osteocytes [4][5][6] and osteoclasts.…”

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

Androgens and Bone

Cited by 597 publications

References 341 publications

Adequacy of androgen replacement influences bone density response to testosterone in androgen-deficient men

Adequacy of androgen replacement influences bone density response to testosterone in androgen-deficient men

Osteoporosis and male age-related hypogonadism: role of sex steroids on bone (patho)physiology

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

Contact Info

Product

Resources

About