JBMR Online - Journal of Bone and Mineral Research - 20(4):613

²Division of General Internal Medicine, Department of Medicine, University of California, San Francisco, California, USA;

³Departments of Medicine and Epidemiology, Minneapolis Veterans Affairs Medical Center and University of Minnesota, Minneapolis, Minnesota, USA.

A role for osteoblastic β-adrenoreceptors in bone regulation is suggested by the finding that β-blockers increase bone mass in mice. We studied the association of β-blocker use with BMD and fractures in the Study of Osteoporotic Fractures. β-blocker use and BMD are unrelated in this cohort, and associations with fracture risk are inconsistent.

Introduction: The central nervous system has been shown to regulate bone mass in mice, possibly by way of the β₂-adrenoreceptors on osteoblasts. β-blockers have been shown to increase bone mass in mice. Because these agents are widely used therapeutically, it is possible that they may influence fracture epidemiology in humans, and they are a potential therapy for osteoporosis.

Materials and Methods: We have studied the association of β-blocker use with BMD and fracture rates in the Study of Osteoporotic Fractures. β-blocker use was recorded at the fourth visit, in 8412 women, of whom 1099 were users, and these women were followed for 7 years.

Results: Users had significantly higher weight, more thiazide use, more estrogen use, less glucocorticoid use, more statin use, and more hypertension than nonusers, and they smoked less. Total hip BMD at the fourth visit was higher in the β-blocker users (0.746 versus 0.735 g/cm², p = 0.02), but adjustment for weight alone, or together with these other variables, eliminated this difference (p = 0.62). There was no effect of β-blocker use on loss of hip BMD over a mean follow-up of 4 years (p = 0.48). Os calcis BMD at visit 4 was also higher in those taking β-blockers (0.385 versus 0.375 g/cm², p = 0.005), but weight adjustment eliminated this difference (p = 0.14). The frequencies of hip or any fracture (since age 50) were similar in users and nonusers (p = 0.80 and p = 0.51, respectively). Over a mean follow-up of 7 years, there were 2167 total fractures, including 431 at the wrist and 585 at the hip. Among β-blocker users, hazards ratios were 0.92 (0.81, 1.05) for any fracture, 0.74 (0.54, 1.01) for wrist fracture, and 0.76 (0.58, 0.99) for hip fracture. Adjustment for weight and other factors previously shown to influence hip fracture incidence in this cohort made little difference to the outcome. When fracture data were analyzed for nonselective and β₁-selective agents separately, trends toward fewer fractures were confined to the users of selective β₁-blockers.

Conclusions: β-blocker use and BMD are unrelated in this cohort, and associations with fracture risk are inconsistent. Therefore, a history of use of these drugs is not useful in assessing fracture risk, nor do they have a role in osteoporosis management at this time. The relationship between β-blocker use and hip fracture deserves further study.

Cited by

Jane A Cauley, LieLing Wu, Nina S Wampler, Janice M Barnhart, Matthew Allison, Zhao Chen, Rebecca Jackson and John Robbins. (2007) Clinical Risk Factors for Fractures in Multi-Ethnic Women: The Women’s Health Initiative. Journal of Bone and Mineral Research 22:11, 1816-1826
Online publication date: 1-Nov-2007.
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Xin Chen, In-Hwan Song, James E Dennis and Edward M Greenfield. (2007) Endogenous PKIγ Limits the Duration of the Anti-Apoptotic Effects of PTH and β-Adrenergic Agonists in Osteoblasts. Journal of Bone and Mineral Research 22:5, 656-664
Online publication date: 1-May-2007.
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Roberto L de Souza, Andrew A Pitsillides, Lance E Lanyon, Timothy M Skerry and Chantal Chenu. (2005) Sympathetic Nervous System Does Not Mediate the Load-Induced Cortical New Bone Formation. Journal of Bone and Mineral Research 20:12, 2159-2168
Online publication date: 1-Dec-2005.
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