Additive protective effects of estrogen and androgen treatment on trabecular bone in ovariectomized rats

Asa Tivesten; Sofia Movérare-Skrtic; Andrei Chagin; Katrien Venken; Phil Salmon; Dirk Vanderschueren; Lars Sävendahl; Agneta Holmäng; Claes Ohlsson

doi:10.1359/JBMR.040819

Additive protective effects of estrogen and androgen treatment on trabecular bone in ovariectomized rats

J Bone Miner Res. 2004 Nov;19(11):1833-9. doi: 10.1359/JBMR.040819. Epub 2004 Aug 23.

Authors

Asa Tivesten¹, Sofia Movérare-Skrtic, Andrei Chagin, Katrien Venken, Phil Salmon, Dirk Vanderschueren, Lars Sävendahl, Agneta Holmäng, Claes Ohlsson

Affiliation

¹ Wallenberg Laboratory for Cardiovascular Research, Cardiovascular Institute at the Sahlgrenska Academy, Sahlgrenska University Hospital, Göteborg, Sweden.

PMID: 15476584
DOI: 10.1359/JBMR.040819

Abstract

Both ER and AR activation regulates trabecular bone mass. We show that combined estrogen and androgen treatment results in additive protection of trabecular bone in OVX rats. This may in part be attributable to the effect of AR activation to attenuate the inhibitory effect of ER activation on bone formation.

Introduction: Sex steroids are important regulators of trabecular bone mass. Both estrogen receptor (ER) and androgen receptor (AR) activation results in increased trabecular bone mass. The aim of this study was to investigate if combined estrogen and androgen treatment might be beneficial in the treatment of trabecular bone loss.

Materials and methods: Twelve-week-old female rats were ovariectomized (OVX) and treated with vehicle (V), 17beta-estradiol (E2; ER activation), dihydrotestosterone (DHT; AR activation), or the combination (E2 + DHT) for 6 weeks. The skeletal phenotype was analyzed by pQCT, microCT, histomorphometry of growth plates, and serum levels of biochemical bone markers.

Results: Both E2 (+121% over V) and DHT (+34%) preserved the trabecular volumetric BMD (tvBMD) in OVX rats. The effect of E2 and DHT on tvBMD was additive, resulting in a 182% increase over V in the rats given E2 + DHT. MicroCT analyses of the trabecular bone microstructure revealed that the effect of E2 and DHT was additive on the number of trabeculae. E2 treatment reduced serum markers of both bone resorption (collagen C-terminal telopeptide) and bone formation (osteocalcin), indicating reduced bone turnover. Addition of DHT to E2 treatment did not modulate the effects of E2 on the marker of bone resorption, whereas it attenuated the inhibitory effect of E2 on the bone formation marker, which might explain the additive protective effect of E2 and DHT on trabecular bone mass. In contrast, DHT partially counteracted the suppressive effect of E2 on longitudinal bone growth and the E2-induced alterations in growth plate morphology.

Conclusions: These findings show that combined estrogen and androgen treatment results in additive protective effects on trabecular bone in OVX rats. Our data suggest that a combined treatment with selective ER and AR modulators might be beneficial in the treatment of osteoporosis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Androgens / metabolism*
Androgens / therapeutic use
Animals
Body Weight
Bone Density
Bone Development / drug effects*
Bone Diseases, Metabolic / drug therapy*
Bone and Bones
Cell Proliferation
Dihydrotestosterone / pharmacology
Drug Therapy, Combination
Estradiol / metabolism
Estrogens / metabolism*
Estrogens / therapeutic use
Female
Femur / pathology
Insulin-Like Growth Factor I / biosynthesis
Organ Size
Ovary / metabolism*
Rats
Rats, Sprague-Dawley
Tibia / pathology
Time Factors
Tomography, X-Ray Computed
Uterus / pathology

Substances

Androgens
Estrogens
Dihydrotestosterone
Estradiol
Insulin-Like Growth Factor I