Bone turnover across the menopause transition : The role of gonadal inhibins. Conference Paper uri icon

abstract

  • Accumulating evidence demonstrates increasing bone turnover and bone loss in women prior to menopause and decreases in serum estradiol levels. Increased follicle-stimulating hormone levels have been correlated with some of these peri-menopausal changes. However, decreases in gonadal inhibins of the transforming growth factor (TGF)-beta superfamily strongly correlate with increases in bone formation and resorption markers across the menopause transition and predict lumbar bone mass in peri-menopausal women, likely as a result of direct inhibin suppression of osteoblastogenesis and osteoclastogenesis. Inhibins bind specifically to cells during osteoblastogenesis and osteoclastogenesis. They can block bone morphogenetic protein (BMP)-stimulated osteoblast and osteoclast development as well as BMP-stimulated SMAD1 phosphorylation, likely via inhibin-beta-glycan sequestration of BMP Type II receptor (BMPRII). Interestingly, continuous in vivo exposure to inhibin A is anabolic and protective against gonadectomy-induced bone loss in mice, suggesting that inhibins contribute to the endocrine regulation of bone metabolism via a bimodal mechanism of action whereby cycling inhibin exposure suppresses bone turnover and continuous exposure to inhibins is anabolic.

published proceedings

  • Ann N Y Acad Sci

author list (cited authors)

  • Nicks, K. M., Fowler, T. W., Akel, N. S., Perrien, D. S., Suva, L. J., & Gaddy, D.

citation count

  • 39

complete list of authors

  • Nicks, Kristy M||Fowler, Tristan W||Akel, Nisreen S||Perrien, Daniel S||Suva, Larry J||Gaddy, Dana

publication date

  • March 2010

publisher