Estrogen receptor specificity in the regulation of the skeleton in female mice

Lindberg, Mattias F.; Alatalo, Sari L.; Halleen, Jussi M.; Mohan, Subburaman; Gustafsson, Jan‐Åke; Ohlsson, Claes

doi:10.1677/joe.0.1710229

Cited by 184 publications

(237 citation statements)

References 37 publications

(28 reference statements)

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“…In line with previous findings from our laboratory, our data shows that OVX rats display a stronger increase of body weight compared to E 2 and SHAM rats mainly due to an increase in the percentage of total body fat (Lindberg et al 2001a, Hertrampf et al 2007). In contrast to treatment with 8-VE2, application of 16-LE2 resulted in an antagonization of body weight increase after OVX (Fig.…”

Section: Discussionsupporting

confidence: 93%

“…These data are in agreement with studies performed in knockout mice: application of E 2 did not prevent the development of osteoporosis in ERKO female (Lindberg et al 2001a, Lindberg et al 2002a) and male mice (Lindberg et al 2002b), indicating that the bone-protective effects of E 2 are primarily mediated by ER. Further, ERα gene polymorphisms are associated with osteoporosis in human populations (Gómez et al 2007).…”

Section: Discussionsupporting

confidence: 84%

“…Opposing effects were observed for longitudinal bone growth after activation of ERα and ERβ (Windahl et al 1999, Lindberg et al 2001a, suggesting a repressive function for ERβ in the regulation of bone growth during adolescence.…”

Section: Discussionmentioning

confidence: 88%

“…This is in agreement with studies using male and female ER knockout mice (ERKO). In these animals A c c e p t e d M a n u s c r i p t of body weight and composition in wild type animals with natural ratios of both ER subtypes is also mainly mediated via ER (Fig.2 B) (Lindberg et al 2001a, Hertrampf et al 2007). …”

Section: Discussionmentioning

confidence: 93%

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Estrogen receptor subtype-specific effects on markers of bone homeostasis

Hertrampf

Schleipen

Velders

et al. 2008

Molecular and Cellular Endocrinology

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Please cite this article as: Hertrampf, T., Schleipen, B., Velders, M., Laudenbach, U., Fritzemeier, K.H., Diel, P., Estrogen receptor subtype-specific effects on markers of bone homeostasis, Molecular and Cellular Endocrinology (2007), doi:10.1016/j.mce.2008 This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. AbstractTo further elucidate the processes involved in the physiology of bone-protection by estrogens, ovariectomized (OVX) rats were treated subcutaneously with 17-estradiol, the ER-specific agonist (16-LE2) and the ER-specific agonist (8-VE2).OVX and intact animals served as controls. Biomarkers of bone-formation (osteocalcin (OC), osteopontin (OPN)) and bone-resorption (telopeptides of collagen type I (CTx), pyridinoline cross-links (Pyd)) were quantified. Bone mineral density was measured by computed tomography.OVX-induced bone loss could be antagonized by subcutaneous administration of 17-estradiol and 16-LE2. Serum levels of CTx, OC and OPN were significantly elevated in OVX compared to intact animals and reduced by 17-estradiol and 16-LE2. Treatment of OVX rats with 8-VE2 did not affect BMD or bone-marker serum levels.Taken together, the complex expression pattern of bone-markers in OVX rats following subcutaneous administration of ER subtype-specific agonists indicates that 17-estradiol exerts its bone-protective effects by modulating the activity of osteoclasts and osteoblasts via ERα.

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Section: Discussionsupporting

confidence: 93%

Section: Discussionsupporting

confidence: 84%

Section: Discussionmentioning

confidence: 88%

Section: Discussionmentioning

confidence: 93%

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Estrogen receptor subtype-specific effects on markers of bone homeostasis

Hertrampf

Schleipen

Velders

et al. 2008

Molecular and Cellular Endocrinology

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“…Several SERMs are well known to protect against bone loss related to the menopause-related deficit in estrogen, and a wide variety of studies in multiple species and conditions have demonstrated the efficacy of SERMs to reduce bone turnover, and to prevent bone or BMD loss. 31,32,45,46 The effect of estrogen on BMD is ERa-dependent, 21 and the ERa and ERb appear to exert opposing actions: 47 activation of the ERa promotes longitudinal bone growth, whereas that of the ERb represses it. In the present study, substantial changes in BMD over a 28-day period in 5-month-old mice were obviously not expected, but the data nevertheless point to interesting trends.…”

Section: Discussionmentioning

confidence: 99%

Estrogen receptor α-mediated adiposity-lowering and hypocholesterolemic actions of the selective estrogen receptor modulator acolbifene

et al. 2005

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OBJECTIVE:The selective estrogen receptor (ER) modulator (SERM) acolbifene (ACOL), a potent and pure antiestrogen in the mammary gland and uterus, exerts beneficial pro-estrogenic actions on energy balance, insulin sensitivity and lipid metabolism. ACOL binds ERs a and b, both of which have been involved in the metabolic actions of estrogen. This study aimed at determining the identity of the ER involved in the beneficial metabolic actions of ACOL. DESIGN AND MEASUREMENTS: ACOL was administered for 4 weeks to male and female wild-type and ERa knockout (KO) mice, and indices of energy balance as well as plasma and liver lipid concentrations were determined. RESULTS: ERa KO mice were heavier, gained more fat mass and had larger adipose depots than their wild-type counterparts. In both genders, ACOL decreased fat gain (50%) and white adipose tissue mass in male and female wild-type, but not in ERa KO mice. ACOL reduced plasma cholesterol in female wild-type mice (À27%), whereas the compound remained ineffective in their ERa KO counterparts. Plasma triglycerides were unaffected by ACOL. Finally, ACOL decreased liver cholesterol and triglyceride concentrations only in wild-type female animals. CONCLUSION: The beneficial metabolic actions of the SERM ACOL on adiposity and on plasma and liver lipids are entirely due to its interaction with the ERa.

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17β‐Estradiol Exposure Accelerates Skeletal Development in Xenopus laevis Tadpoles

Bauer-Dantoin

Meinhardt

2010

The Anatomical Record

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Although it is well established that estrogen regulates skeletal growth and ossification in mammals, the effects of estrogen on skeletal development in amphibians are relatively uncharacterized. This study was conducted to characterize the impact of 17b-estradiol exposure on skeletal development in Xenopus laevis tadpoles. On day 48 postfertilization, tadpoles were placed in tanks containing 50% Holtfreter's Solution AE17b-estradiol at one of four concentrations (10 À11 , 10 À10 , 10 À9 , and 10 À8 M). At 7-11 day intervals until day 91, 7-10 tadpoles per group were killed, fixed, measured, and staged. Specimens were then cleared and double-stained for cartilage and bone, and 34 skeletal elements were analyzed for ossification. Results from the study indicate that both low (10 À11 M) and high (10 À8 M) concentrations of 17b-estradiol have a significant stimulatory effect on tadpole development. Both the larval stage and ossification index of tadpoles exposed to 10 À11 or 10 À8 M 17b-estradiol were significantly greater than those observed in control animals by day 91 postfertilization. These results are consistent with the hypothesis that endogenous and exogenous estrogen could play a role in the regulation of bone ossification in amphibians. Anat Rec, 293:1880Rec, 293: -1886Rec, 293: , 2010. V V C 2010 Wiley-Liss, Inc.Key words: estradiol; skeleton; bone; Xenopus laevis; metamorphosis; ossification; development Numerous studies have demonstrated that the female sex hormone estrogen has profound effects on the development and maintenance of the mammalian skeleton. These effects include the induction of sexually dimorphic characteristics through actions exerted during the prenatal, postnatal, and pubertal periods (reviewed in Turner et al., 1994); regulation of linear skeletal growth in both sexes, especially during puberty (reviewed in Nilsson et al., 2005); and reduction in the rate of bone remodeling and thus protection against bone loss after sexual maturation (reviewed in Manolagas et al., 2002).Perhaps the most significant of the skeletal effects of estrogen during development are its actions on longitudinal bone growth. In mammals as well as in other vertebrates, longitudinal bone growth occurs through a process known as endochondral ossification, during which chondrogenesis (cartilage formation), followed by remodeling of cartilage into bone (ossification), takes place in the growth plates at the ends of long bones (Nilsson et al., 2005). Mammalian studies investigating the influence of estrogen on this process have demonstrated that the sex steroid can have profound stimulatory and/or inhibitory effects on endochondral ossification in both males and females, depending on the species, dose, and developmental stage of exposure.

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Estrogen receptor specificity in the regulation of the skeleton in female mice

Cited by 184 publications

References 37 publications

Estrogen receptor subtype-specific effects on markers of bone homeostasis

Estrogen receptor subtype-specific effects on markers of bone homeostasis

Estrogen receptor α-mediated adiposity-lowering and hypocholesterolemic actions of the selective estrogen receptor modulator acolbifene

17β‐Estradiol Exposure Accelerates Skeletal Development in Xenopus laevis Tadpoles

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