Sex steroids and bone: current perspectives

doi:10.1093/humupd/dmg017

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Human Reproduction Update, Vol.9, No.3 pp.207-222, 2003
© European Society of Human Reproduction and Embryology 2003; all rights reserved

Sex steroids and bone: current perspectives

Juan Balasch¹

¹ Institut Clínic of Gynecology, Obstetrics and Neonatology, Faculty of Medicine-University of Barcelona, Hospital Clínic-Institut d’Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), Barcelona, Spain

To whom correspondence should be addressed at: Juan Balasch, Institut Clínic of Gynecology and Obstetrics, Hospital Clínic, C/Casanova 143, 08036-Barcelona, Spain. e-mail: jbalasch{at}medicina.ub.es

Abstract

Although the process of bone remodelling or its control hasnot yet been fully elucidated there is, at present, sufficientinformation available to conclude that ovarian steroids (estrogens,androgens, progesterone) play an essential role in skeletalhomeostasis. The mechanism of action of sex steroids on theskeleton is still not entirely clear, but it has traditionallyincluded indirect effects on systemic hormones that regulatecalcium balance and a direct receptor-mediated action. Morerecently, changes in cytokine production within the bone marrow,as well as pro-apoptotic and anti-apoptotic effects in the osteoblasticcells, have been proposed as new perspectives on the cellularand molecular mechanisms by which sex steroids influence adultbone homeostasis. Mechanical loading, when combined with estrogensor androgens, results in a greater osteogenic response thaneither condition separately. Women are especially at risk forosteoporosis if they have had a premature or surgical menopauseand have not received hormone replacement therapy (HRT). Otherreproductive factors that can help to identify women with osteopeniaand emphasize the role of sex steroids in preserving bone massin premenopausal women include: age at menarche, menstrual historyand irregularities (including those associated with excessiveexercise), age at menopause, previous hysterectomy, hyperprolactinaemia,anorexia nervosa, scoliosis, ovarian dysgenesis, pregnancy andlactation, and pharmacological ovarian suppression. The preventionof osteoporosis starts with the onset of the menarche. A combinationof exercise, appropriate nutrition and a healthy lifestyle allmaximize bone mineral accrual and result in optimal peak bonemass; normal ovarian function is essential to this process.Unfortunately, many women actually become aware of the needfor osteoporosis prevention much later in life, usually afterthey have already become menopausal. HRT, however, has importantlimitations for prevention of fractures in post-menopausal women.Future perspectives for treatment of osteoporosis include androgentherapy and anabolic agents. Specifically, synthetic ligandsof the estrogen receptor that can evoke the non-genotrophicbut not the genotrophic signal of the receptor may be bone anabolicagents, as opposed to natural estrogens or selective estrogenreceptor modulators that are anti-resorptive agents. The sameligands may circumvent the side effects associated with conventionalHRT.

Key words: bone homeostasis / bone remodelling / cytokines / hormone replacement therapy / osteoporosis / ovarian steroids

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