The relevance of mouse models for investigating age-related bone loss in humans

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Jilka, Robert L.¹

The relevance of mouse models for investigating age-related bone loss in humans

J Gerontol A Biol Sci Med Sci. October 2013;68(10):1209-1217

Affiliations

¹Center for Osteoporosis and Metabolic Bone Diseases, University of Arkansas for Medical Sciences, Central Arkansas Veterans Healthcare System, Little Rock, Arkansas
Abstract and keywords

Mice are increasingly used for investigation of the pathophysiology of osteoporosis because their genome is easily manipulated, and their skeleton is similar to that of humans. Unlike the human skeleton, however, the murine skeleton continues to grow slowly after puberty and lacks osteonal remodeling of cortical bone. Yet, like humans, mice exhibit loss of cancellous bone, thinning of cortical bone, and increased cortical porosity with advancing age. Histologic evidence in mice and humans alike indicates that inadequate osteoblast-mediated refilling of resorption cavities created during bone remodeling is responsible. Mouse models of progeria also show bone loss and skeletal defects associated with senescence of early osteoblast progenitors. Additionally, mouse models of atherosclerosis, which often occurs in osteoporotic participants, also suffer bone loss, suggesting that common diseases of aging share pathophysiological pathways. Knowledge of the causes of skeletal fragility in mice should therefore be applicable to humans if inherent limitations are recognized.

Keywords: Bones; Aging; Osteoporosis
Links

DOI: 10.1093/gerona/glt046

PubMed: 23689830

WoS: 000324834600008
History

Received: 2013-01-15

Accepted: 2013-03-25

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